Alzheimers PDF

PR A C T I CE G UI D E L INE FOR T H E
Treatment of Patients With

Alzheimers Disease and
Other Dementias
Second Edition
WORK GROUP ON ALZHEIMERS DISEASE AND OTHER DEMENTIAS

Peter V. Rabins, M.D., M.P.H., Chair
Deborah Blacker, M.D., Sc.D.
Barry W. Rovner, M.D.
Teresa Rummans, M.D.
Lon S. Schneider, M.D.
Pierre N. Tariot, M.D.
David M. Blass, M.D., Consultant
STEERING COMMITTEE ON PRACTICE GUIDELINES

John S. McIntyre, M.D., Chair
Sara C. Charles, M.D., Vice-Chair
Daniel J. Anzia, M.D.
Ian A. Cook, M.D.
Molly T. Finnerty, M.D.
Bradley R. Johnson, M.D.
James E. Nininger, M.D.
Barbara Schneidman, M.D.
Paul Summergrad, M.D.
Sherwyn M. Woods, M.D., Ph.D.
AREA AND COMPONENT LIAISONS

Joseph Berger, M.D. (Area I)
C. Deborah Cross, M.D. (Area II)
Harry A. Brandt, M.D. (Area III)
Philip M. Margolis, M.D. (Area IV)
John P. D. Shemo, M.D. (Area V)
Barton J. Blinder, M.D. (Area VI)
David L. Duncan, M.D. (Area VII)
Mary Ann Barnovitz, M.D.
Anthony J. Carino, M.D.
Zachary Z. Freyberg, M.D., Ph.D.
Sheila Hafter Gray, M.D.
Tina Tonnu, M.D.
Copyright 2010, American Psychiatric Association. APA makes this practice guideline freely available to promote its dissemination and use; however, copyright protections are enforced in full. No part of this guideline may
be reproduced except as permitted under Sections 107 and 108 of U.S. Copyright Act. For permission for reuse, visit APPI Permissions & Licensing Center at http://www.appi.org/CustomerService/Pages/Permissions.aspx.
STAFF
Robert Kunkle, M.A., Senior Program Manager
Amy B. Albert, B.A., Project Manager
Thomas J. Craig, M.D., M.P.H., Director, Dept. of Quality Improvement and Psychiatric Services
Darrel A. Regier, M.D., M.P.H., Director, Division of Research
MEDICAL EDITOR
Laura J. Fochtmann, M.D.
This practice guideline was approved in July 2007 and published in October 2007.
A guideline watch, summarizing signicant developments in the scientic literature since publication of this guideline,
may be available in the Psychiatric Practice section of the APA Web site at www.psych.org.
The Work Group on Alzheimers Disease and Other Dementias reports the following potentially competing interests
for the period January 2003 to December 2006: Dr. Rabins has received speaking fees from Pzer, AstraZeneca, Janssen,
Eli Lilly and Company, Forest Pharmaceuticals, Inc., and Wyeth Pharmaceuticals. Dr. Blacker reports no competing
interests. Dr. Rovner has served on speakers bureaus for Pzer and Forest Pharmaceuticals, Inc. Dr. Rummans has
received a research grant from the Linse Bock Foundation. Dr. Schneider has received research or other grants from
Abbott Laboratories, AstraZeneca, Forest Pharmaceuticals, Inc., Johnson & Johnson, Eli Lilly and Company, Novartis,
Pzer, and Myriad. Dr. Schneider has served on speakers bureaus or performed other work relating to continuing medical
education for Abbott Laboratories, AstraZeneca, Forest Pharmaceuticals, Eli Lilly and Company, Solvay, Bristol-Myers
Squibb, and Lundbeck. Dr. Schneider has served on advisory panels for Abbott Laboratories, AstraZeneca, Forest
Pharmaceuticals, Inc., Johnson & Johnson, Eli Lilly and Company, and Novartis. Dr. Tariot has received consulting fees
from Memory Pharmaceuticals Corp. and Novartis; consulting fees and research support from Abbott Laboratories,
Bristol-Myers Squibb, Eisai Inc., GlaxoSmithKline, Janssen, Eli Lilly and Company, Merck and Company, Myriad,
Pzer, Sano-Synthlabo, Dr. Willmar Schwabe Pharmaceuticals, and Takeda Pharmaceuticals North America, Inc.;
educational fees from Lundbeck; consulting fees, research support, and educational fees from AstraZeneca, Eisai Inc.,
Forest Pharmaceuticals, Inc., and Pzer; and research support from Elan Corporation, Mitsubishi Pharma Corporation,
Neurochem, Inc., Ono Pharmaceuticals Co., Ltd., and Wyeth Pharmaceuticals. Dr. Tariot has received other research
support from the National Institute of Aging, the National Institute of Mental Health, the Alzheimers Association, the
Arizona Department of Health Services, and the Institute for Mental Health Research. Dr. Tariot has served on speakers
bureaus for AstraZeneca, Eisai Inc., Forest Pharmaceuticals, Inc., and Pzer, Inc. Dr. Blass reports no competing interests.
The Executive Committee on Practice Guidelines has reviewed this guideline and found no evidence of inuence
from these relationships.
CONTENTS
STATEMENT OF INTENT . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 7
OVERVIEW OF GUIDELINE DEVELOPMENT PROCESS. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 7
GUIDE TO USING THIS PRACTICE GUIDELINE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 8
INTRODUCTION . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 8
PART A: TREATMENT RECOMMENDATIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
I. EXECUTIVE SUMMARY . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
A. Coding System . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
B. General Treatment Principles and Alternatives. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
1. Psychiatric Management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
2. Specific Psychotherapies and Other Psychosocial Treatments. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11
3. Special Concerns Regarding Somatic Treatments for Elderly Patients and Patients With Dementia. . . . . . . . . . . . 12
4. Treatment of Cognitive Symptoms . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 12
5. Treatment of Psychosis and Agitation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 12
6. Treatment of Depression . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 13
7. Treatment of Sleep Disturbances . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 13
8. Special Issues for Long-Term Care. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
II. FORMULATION AND IMPLEMENTATION OF A TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14

A. Determining the Site of Treatment and Frequency of Visits . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14
B. Psychiatric Management . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
1. Establish and Maintain an Alliance With the Patient and the Family . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
2. Perform a Diagnostic Evaluation and Refer the Patient for Any Needed General Medical Care . . . . . . . . . . . . . . . 15
a. General Principles . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 15
b. Neuropsychological Testing . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
c. Neuroimaging . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
d. Biomarkers . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 16
e. Genetic Testing . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
3. Assess and Monitor Psychiatric Status . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 17
4. Monitor and Enhance the Safety of the Patient and Others . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
a. Suicidal Ideation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
b. Agitation and Aggression . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 18
c. Supervision . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 19
d. Falls . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 19
e. Abuse and Neglect . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
f. Wandering . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 20
5. Advise the Patient and Family Concerning Driving (and Other Activities That Put Other People at Risk) . . . . . . . . 20
6. Provide Education and Support to Patients and Families . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 22
a. Educate the Patient and Family About the Illness and Available Treatments . . . . . . . . . . . . . . . . . . . . . . 22
b. Refer the Family to Appropriate Sources of Care and Support . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 22
c. Watch for Signs of Caregiver Distress . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 23
d. Support Families During Decisions About Institutionalization . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 23
7. Advise the Family to Address Financial and Legal Issues . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 24
C. Development and Implementation of a Stage-Specific Treatment Plan . . . . . . . . . . . . . . . . . . . . . . . . . . . 24
1. Mildly Impaired Patients. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 25
2. Moderately Impaired Patients . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 25
3. Severely and Profoundly Impaired Patients . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 26
4. Implementation of Psychosocial Treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 26
5. Implementation of Pharmacological Treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 27
a. Treatments for Cognitive and Functional Losses . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 27
b. Treatments for Psychosis and Agitation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 30
c. Treatments for Depression and Related Symptoms . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 34
d. Treatments for Sleep Disturbance . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 36
III. SPECIFIC CLINICAL FEATURES INFLUENCING THE TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37

A. Demographic and Social Factors. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37
1. Age. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37
2. Gender . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37
3. Ethnic and Cultural Background . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
4. Other Demographic and Psychosocial Factors. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
B. Co-occurring Conditions and Other Dementias . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
1. General Medical Conditions. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
2. Delirium. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 38
3. Parkinsons Disease Spectrum Illnesses (Including Parkinsons Disease and Dementia With Lewy Bodies). . . . . . . 39
4. Cerebrovascular Disease . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
5. Frontotemporal Dementia Spectrum Disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 39
C. Site-Specific Issues . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
1. Home Care. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
2. Day Care . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
3. Long-Term Care. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 40
4. Inpatient General Medical or Surgical Services . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 41
5. General Psychiatric Inpatient Units . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
PART B: BACKGROUND INFORMATION AND REVIEW OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . 42
IV. DISEASE DEFINITION, NATURAL HISTORY, AND EPIDEMIOLOGY . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42

A. Definition of Dementia . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42
B. Associated Features . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
C. Differential Diagnosis. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 43
D. Prevalence and Course . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 44
E. Staging of Dementia . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 44
F. Specific Dementias . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 45
1. Dementia of the Alzheimers Type . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 45
2. Mild Cognitive Impairment . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 45
3. Vascular Dementia. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
4. Dementia of Parkinsons Disease and Dementia With Lewy Bodies . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 46
5. Dementia Due to Frontotemporal Dementia Spectrum Disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
6. Other Progressive Dementing Disorders . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
7. Dementia Due to Other Causes. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 47
V. REVIEW OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48

A. Specific Psychotherapies/Psychosocial Treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
1. Behavior-Oriented Approaches . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
2. Emotion-Oriented Approaches. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48
3. Cognition-Oriented Approaches . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 49
4. Stimulation-Oriented Approaches . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 49
B. Somatic Treatments . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
1. Treatments for Cognitive and Functional Losses . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
a. Cholinesterase Inhibitors . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 50
b. Memantine . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 52
c. Vitamin E . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 52
d. Other Agents . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 53
2. Treatments for Psychosis and Agitation . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 54
a. Antipsychotics . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 54
b. Benzodiazepines . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
c. Anticonvulsants . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
d. Other Agents . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 59
3. Treatments for Depression and Related Symptoms . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 60
a. Antidepressants . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 60
b. Electroconvulsive Therapy . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 60
4. Treatments for Sleep Disturbance . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 60
PART C: FUTURE RESEARCH NEEDS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61
INDIVIDUALS AND ORGANIZATIONS THAT SUBMITTED COMMENTS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 63
REFERENCES. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 64
Practice Guideline for the Treatment of Patients With Alzheimers Disease and Other Dementias 7
STATEMENT OF INTENT OVERVIEW OF GUIDELINE

DEVELOPMENT PROCESS
The APA Practice Guidelines are not intended to be con-
strued or to serve as a standard of medical care. Standards
This practice guideline was developed under the auspices
of medical care are determined on the basis of all clinical
of the APA Steering Committee on Practice Guidelines.
data available for an individual patient and are subject to
The development process is detailed in a document enti-
change as scientic knowledge and technology advance
tled APA Guideline Development Process, which is
and practice patterns evolve. These parameters of practice
available from the APA Department of Quality Improve-
should be considered guidelines only. Adherence to them
ment and Psychiatric Services. Key features of this pro-
will not ensure a successful outcome for every individual,
cess include the following:
nor should they be interpreted as including all proper
methods of care or excluding other acceptable methods of
A comprehensive literature review
care aimed at the same results. The ultimate judgment re-
Development of evidence tables
garding a particular clinical procedure or treatment plan
Initial drafting of the guideline by a work group that
must be made by the psychiatrist in light of the clinical
included psychiatrists with clinical and research exper-
data presented by the patient and the diagnostic and treat-
tise in dementia
ment options available.
Production of multiple revised drafts with widespread
This practice guideline has been developed by psychi-
review; 22 organizations and 64 individuals submitted
atrists who are in active clinical practice. In addition, some
signicant comments.
contributors are primarily involved in research or other
Approval by the APA Assembly and Board of Trustees
academic endeavors. It is possible that through such activ-
Planned revisions at regular intervals
ities some contributors, including work group members
and reviewers, have received income related to treatments Relevant literature was identied through a computer-
discussed in this guideline. A number of mechanisms are ized search of MEDLINE, using PubMed, for the period
in place to minimize the potential for producing biased from 1994 to 2004. By using the key words dementia, de-
recommendations due to conicts of interest. Work mentias, Alzheimer, Alzheimers, Pick disease, or
group members are selected on the basis of their expertise mild cognitive impairment, a total of 79,510 citations were
and integrity. Any work group member or reviewer who found. Limiting the search to clinical trials, practice guide-
has a potential conict of interest that may bias (or appear lines, and meta-analyses published in English that included
to bias) his or her work is asked to disclose this to the abstracts yielded 2,679 articles, which were screened by us-
Steering Committee on Practice Guidelines and the work ing title and abstract information. To locate citations relevant
group. Iterative guideline drafts are reviewed by the to Part B of the guideline, the above search terms were also
Steering Committee, other experts, allied organizations, used to identify review articles having medical subject head-
APA members, and the APA Assembly and Board of ing (MeSH) subheadings of classication, diagnosis, epide-
Trustees; substantial revisions address or integrate the miology, etiology, genetics, or mortality. This search yielded
comments of these multiple reviewers. The development 9,840 citations, of which 4,816 were published in English
of the APA Practice Guidelines is not nancially sup- with abstracts and were screened as described above. To lo-
ported by any commercial organization. cate other systematic reviews, a search of the Cochrane da-
More detail about mechanisms in place to minimize tabase was also conducted using the search term dementia.
bias is provided in a document entitled APA Guideline Additional, less formal literature searches were conducted by
Development Process, which is available from the APA APA staff and individual members of the Work Group on
Department of Quality Improvement and Psychiatric Alzheimers Disease and Other Dementias to identify refer-
Services. ences on related topics as well as articles published during the
This practice guideline was approved in July 2007 and guideline development process. Sources of funding were
published in October 2007. considered when the work group reviewed the literature but
are not identied in this document. When reading source ar-
ticles referenced in this guideline, readers are advised to con-
sider the sources of funding for the studies.
This document represents a synthesis of current scientic
knowledge and accepted clinical practice regarding the treat-
8 APA PRACTICE GUIDELINES
ment of patients with Alzheimers disease and other demen- previous sections and summarizes areas for which more re-
tias. It strives to be as free as possible of bias toward any search data are needed to guide clinical decisions.
theoretical approach to treatment. In order for the reader to To share feedback on this or other published APA prac-
appreciate the evidence base behind the guideline recom- tice guidelines, a form is available at http://www.psych.org/
mendations and the weight that should be given to each rec- psych_pract/pg/reviewform.cfm.
ommendation, the summary of treatment recommendations
is keyed according to the level of condence with which each
INTRODUCTION
recommendation is made. Each rating of clinical condence
considers the strength of the available evidence and is based
on the best available data. When evidence is limited, the level
of condence also incorporates clinical consensus with re- The purpose of this guideline is to assist the psychiatrist in
gard to a particular clinical decision. In the listing of cited caring for a patient with dementia. In particular, it seeks to
references, each reference is followed by a letter code in summarize data to inform the care of patients with demen-
brackets that indicates the nature of the supporting evidence. tia of the Alzheimers type (referred to here as Alzheimers
disease) and other dementias, including vascular dementia,
Parkinsons disease, dementia with Lewy bodies, and the fr-
GUIDE TO USING THIS ontotemporal dementia spectrum disorders. The guideline
PRACTICE GUIDELINE does not purport to review research or provide recommen-
dations for every dementia associated with general medical
conditions, such as human immunodeciency virus (HIV)
The Practice Guideline for the Treatment of Patients With infection, Huntingtons disease, head trauma, structural le-
Alzheimers Disease and Other Dementias consists of three sions, or endocrine and metabolic disturbances. Nonethe-
parts (Parts A, B, and C) and many sections, not all of less, many of the recommendations regarding the
which will be equally useful for all readers. The following management of cognitive and functional changes and neu-
guide is designed to help readers nd the sections that will ropsychiatric complications apply to dementia in general.
be most useful to them. Psychiatrists care for patients with dementia in many
Part A, Treatment Recommendations for Patients different settings and serve a variety of functions. For some
With Alzheimers Disease and Other Dementias, is pub- patients a psychiatrist will be the primary evaluating or
lished as a supplement to the American Journal of Psychiatry treating physician, for some the psychiatrist will serve as a
and contains general and specic treatment recommenda- consultant to another physician or other treating clinician
tions. Section I summarizes the key recommendations of regarding the care of psychiatric symptoms, and for other
the guideline and codes each recommendation according patients the psychiatrist will function as part of a multidis-
to the degree of clinical condence with which the recom- ciplinary team. In all settings, however, the care of every
mendation is made. Section II is a guide to the formula- patient with dementia must be individualized to meet the
tion and implementation of a treatment plan for the unique needs of that patient and his or her caregivers.
individual patient. Section III discusses a range of clinical The guideline begins at the point where the psychia-
considerations that could alter the general recommenda- trist or other medical professional has diagnosed a patient
tions discussed in Section II. with a dementing disorder according to the criteria in
Part B, Background Information and Review of Avail- DSM-IV-TR (see Table 1 for the criteria for dementia of
able Evidence, and Part C, Future Research Directions, the Alzheimers type) and has evaluated the patient for co-
are not included in the American Journal of Psychiatry sup- existing mental disorders, such as delirium, major depres-
plement but are provided with Part A in the complete sion, and substance use disorders. Making the initial
guideline, which is available online through the American diagnosis of dementia can be challenging, particularly
Psychiatric Association (http://www.psych.org) and in when the initial symptoms are not decits in memory but
print format in compendiums of APA practice guidelines are neuropsychiatric symptoms, personality changes, or
published by American Psychiatric Publishing, Inc. Part B decits in executive function. This guideline also assumes
provides an overview of Alzheimers disease and other de- that the psychiatrist, neurologist, or primary care physi-
mentias, including general information on natural history, cian has evaluated the patient for treatable factors that
course, and epidemiology. It also provides a structured re- may be causing or exacerbating the dementia and for gen-
view and synthesis of the evidence that underlies the rec- eral medical or other conditions that may affect its treat-
ommendations made in Part A. Part C draws from the ment and course.
TA BL E 1. DSM-IV-TR Diagnostic Criteria for 294.1x Dementia of the Alzheimers Type

A. The development of multiple cognitive decits manifested by both
(1) memory impairment (impaired ability to learn new information or to recall previously learned
information)
(2) one (or more) of the following cognitive disturbances:
(a) aphasia (language disturbance)
(b) apraxia (impaired ability to carry out motor activities despite intact motor function)
(c) agnosia (failure to recognize or identify objects despite intact sensory function)
(d) disturbance in executive functioning (i.e., planning, organizing, sequencing, abstracting)
B. The cognitive decits in Criteria A1 and A2 each cause signicant impairment in social or occupational
functioning and represent a signicant decline from a previous level of functioning.
C. The course is characterized by gradual onset and continuing cognitive decline.
D. The cognitive decits in Criteria A1 and A2 are not due to any of the following:
(1) other central nervous system conditions that cause progressive decits in memory and cognition (e.g.,
cerebrovascular disease, Parkinsons disease, Huntingtons disease, subdural hematoma, normal-pressure
hydrocephalus, brain tumor)
(2) systemic conditions that are known to cause dementia (e.g., hypothyroidism, vitamin B12 or folic acid
deciency, niacin deciency, hypercalcemia, neurosyphilis, HIV infection)
(3) substance-induced conditions
E. The decits do not occur exclusively during the course of a delirium.
F. The disturbance is not better accounted for by another Axis I disorder (e.g., Major Depressive Disorder,
Schizophrenia).
Code based on presence or absence of a clinically signicant behavioral disturbance:
294.10 Without Behavioral Disturbance: if the cognitive disturbance is not accompanied by any clinically
signicant behavioral disturbance.
294.11 With Behavioral Disturbance: if the cognitive disturbance is accompanied by a clinically
signicant behavioral disturbance (e.g., wandering, agitation).
Specify subtype:
With Early Onset: if onset is at age 65 years or below
With Late Onset: if onset is after age 65 years
Coding note: Also code 331.0 Alzheimers disease on Axis III. Indicate other prominent clinical features related
to the Alzheimers disease on Axis I (e.g., 293.83 Mood Disorder Due to Alzheimers Disease, With
Depressive Features, and 310.1 Personality Change Due to Alzheimers Disease, Aggressive Type).
Reprinted from the Diagnostic and Statistical Manual of Mental Disorders, 4th Edition, Text Revision. Washington, DC, Amer-
ican Psychiatric Association, 2000. Copyright 2000, American Psychiatric Association. Used with permission.
This guideline is intended to be inclusive and to cover ric symptoms that cannot be completely subsumed by one
the range of necessary treatments that might be used by a DSM-IV-TR diagnostic category; distinct treatment of
psychiatrist who provides or coordinates the overall care of these symptoms or disorders may also be needed. In terms
the patient with dementia. Much of the emphasis of this of the treatment of dementia, interventions to reduce or
practice guideline is on symptoms that are often referred to correct cognitive and functional decits are expected to
as neuropsychiatric or psychiatric and behavioral gain importance over time as new approaches are devel-
symptoms, terms that will be used interchangeably oped. Thus, the psychiatrist caring for a patient with de-
throughout this guideline. These symptoms are highly mentia should consider, but need not be limited to, the
prevalent, cause signicant morbidity, and can often be ef- treatments recommended in this practice guideline. Fi-
fectively treated; their evaluation and treatment usually rest nally, other key tasks include providing critical support for
upon knowledge acquired in general psychiatry training family members and other caregivers and making referrals
programs. Many patients also have co-occurring psychiat- to social, legal, and other community resources.
Part A
TREATMENT RECOMMENDATIONS
I. EXECUTIVE SUMMARY
A. CODING SYSTEM nitive psychiatric symptoms and their response to inter-
vention [I]. In order to offer prompt treatment, enhance
Each recommendation is identied as falling into one of safety, and provide timely advice to the patient and family,
three categories of endorsement, indicated by a bracketed it is generally necessary to see patients in routine follow-up
Roman numeral following the statement. The three cate- at least every 36 months [II]. More frequent visits (e.g., up
gories represent varying levels of clinical condence: to once or twice a week) or even psychiatric hospitalization
[I] Recommended with substantial clinical condence may be required for patients with acute, complex, or po-
[II] Recommended with moderate clinical condence tentially dangerous symptoms or for the administration of
[III] May be recommended on the basis of individual cir- specic therapies [I]. Recommended assessments include
cumstances evaluation of suicidality, dangerousness to self and others,
and the potential for aggression, as well as evaluation of
living conditions, safety of the environment, adequacy of
B. GENERAL TREATMENT PRINCIPLES
supervision, and evidence of neglect or abuse [I].
AND ALTERNATIVES All patients and families should be informed that even
Patients with dementia display a broad range of cognitive mild dementia increases the risk of vehicular accidents [I].
impairments and neuropsychiatric symptoms that can Mildly impaired patients should be advised to limit their
cause signicant distress to themselves and caregivers. As driving to safer situations or to stop driving [I], and mod-
a result, individualized and multimodal treatment plans erately impaired patients should be instructed not to drive
are required [I]. Dementia is usually progressive, and [I]. Advice about driving cessation should also be commu-
treatment must evolve with time in order to address newly nicated to family members, as the implementation of the
emerging issues [I]. At each stage the psychiatrist should recommendation often falls on them [I]. Relevant state
be vigilant for symptoms likely to be present, should iden- laws regarding notication should be followed [I].
tify and treat co-occurring psychiatric and medical condi- Important aspects of psychiatric management include
tions, and should help patients and families anticipate educating patients and families about the illness, its treat-
future symptoms and the care likely to be required [I]. ment, and sources of additional care and support (e.g.,
support groups, respite care, nursing homes, and other
1. Psychiatric Management long-term-care facilities) and advising patients and their
families of the need for nancial and legal planning due to
The treatment of patients with dementia should be based
the patients eventual incapacity (e.g., power of attorney
on a thorough psychiatric, neurological, and general med-
for medical and nancial decisions, an up-to-date will, and
ical evaluation of the nature and cause of the cognitive
the cost of long-term care) [I].
decits and associated noncognitive symptoms, in the
context of a solid alliance with the patient and family [I]. It
is particularly critical to identify and treat general medical 2. Specific Psychotherapies and Other
conditions, most notably delirium, that may be responsi- Psychosocial Treatments
ble for or contribute to the dementia or associated neuro- In addition to the general psychosocial interventions sub-
psychiatric symptoms [I]. sumed under psychiatric management, a number of spe-
Ongoing assessment includes periodic monitoring of cic interventions are appropriate for some patients. Few
the development and evolution of cognitive and noncog- of these treatments have been subjected to double-blind
11
randomized evaluation, but some research, along with Drug Administration (FDA) for treatment of mild to
clinical practice, supports their effectiveness. Behavior- moderate Alzheimers disease, and donepezil has been ap-
oriented treatments are used to identify the antecedents proved by the FDA for severe Alzheimers disease. These
and consequences of problem behaviors and attempt to re- medications have similar rates of adverse effects and have
duce the frequency of behaviors by directing changes in been shown to lead to modest benets in a substantial mi-
the environment that alter these antecedents and conse- nority of patients (i.e., 30%40% in clinical trials). These
quences. Behavioral approaches have not been subjected medications should be offered to patients with mild to
to large randomized clinical trials but are supported by moderate Alzheimers disease after a thorough discussion
small trials and case studies and are in widespread clinical of their potential risks and benets [I], and they may be
use [II]. Stimulation-oriented treatments, such as recre- helpful for patients with severe Alzheimers disease [II].
ational activity, art therapy, music therapy, and pet therapy, Cholinesterase inhibitors should be considered for pa-
along with other formal and informal means of maximiz- tients with mild to moderate dementia associated with
ing pleasurable activities for patients, have modest support Parkinsons disease [I]. Only rivastigmine has been ap-
from clinical trials for improving behavior, mood, and, to a proved by the FDA for this indication, but there is no rea-
lesser extent, function, and common sense supports their son to believe the benet is specic to this cholinesterase
use as part of the humane care of patients [II]. Among the inhibitor.
emotion-oriented treatments, supportive psychotherapy Cholinesterase inhibitors can be considered for pa-
can be employed to address issues of loss in the early stages tients with dementia with Lewy bodies [II].
of dementia [II]. Reminiscence therapy has some modest The constructs of mild cognitive impairment and vas-
research support for improvement of mood and behavior cular dementia are evolving and have ambiguous bound-
[III]; validation therapy and sensory integration have less aries with Alzheimers disease. The efcacy and safety of
research support [III]; none of these modalities has been cholinesterase inhibitors for patients with these disorders
subjected to rigorous testing. Cognition-oriented treat- are uncertain; therefore, no specic recommendation can
ments, such as reality orientation, cognitive retraining, be made at this time, although individual patients may
and skills training focused on specic cognitive decits, are benet from these agents [II].
unlikely to have a persistent benet and have been associ- Memantine, a noncompetitive N-methyl-D-aspartate
ated with frustration in some patients [III]. (NMDA) antagonist, which has been approved by the
FDA for use in patients with moderate and severe Alzhei-
3. Special Concerns Regarding Somatic Treatments for mers disease, may provide modest benets and has few
Elderly Patients and Patients With Dementia adverse effects; thus, it may be considered for such pa-
Medications are effective in the management of some symp- tients [I]. There is some evidence of its benet in mild
toms associated with dementia, but they must be used with Alzheimers disease [III] and very limited evidence of its
caution in this patient population [I]. Because age may alter benet in vascular dementia [I].
the absorption, distribution, metabolism, and elimination of Vitamin E (-tocopherol) is no longer recommended
many medications, elderly individuals may be more sensi- for the treatment of cognitive symptoms of dementia be-
tive to their effects. General medical conditions and use of cause of limited evidence for its efcacy as well as safety
more than one medication may further affect the pharma- concerns [II].
cokinetics of many medications. In addition, patients with Nonsteroidal anti-inammatory agents (NSAIDs),
dementia may be more likely to experience certain medica- statin medications, and estrogen supplementation (with
tion adverse effects, including anticholinergic effects, conjugated equine estrogens) have shown a lack of efcacy
orthostasis, sedation, and parkinsonism. Finally, symptoms and safety in placebo-controlled trials in patients with Alz-
of dementia may alter medication adherence in ways that heimers disease and therefore are not recommended [I].
are unsafe. Consequently, when using pharmacotherapy in
patients with dementia, low starting doses, small increases in 5. Treatment of Psychosis and Agitation
dose, and long intervals between dose increments may be Psychosis, aggression, and agitation are common in pa-
needed, in addition to ensuring that a system is in place that tients with dementia and may respond to similar thera-
can enhance proper medication adherence [I]. pies. When deciding if treatment is indicated, it is critical
to consider the safety of the patient and those around him
4. Treatment of Cognitive Symptoms or her [I]. A careful evaluation for general medical, psy-
Three cholinesterase inhibitorsdonepezil, rivastigmine, chiatric, environmental, or psychosocial problems that
and galantamineare approved by the U.S. Food and may underlie the disturbance should be undertaken [I]. If
possible and safe, such underlying causes should be sedation, worsening cognition, delirium, increased risk of
treated rst [I]. If this does not resolve the symptoms, and falls, and worsening of breathing disorders. Lorazepam
if they do not cause signicant danger or distress to the and oxazepam, which have no active metabolites, are pref-
patient or others, such symptoms are best treated with en- erable to agents with a longer half-life such as diazepam or
vironmental measures, including reassurance and redirec- clonazepam [III].
tion [I]. For agitation, some of the behavioral measures There is minimal evidence for the efcacy of anticon-
discussed in Section I.B.2 may also be helpful [II]. If these vulsants, lithium, and beta-blockers for the treatment of
measures are unsuccessful or the behaviors are particu- psychosis or agitation in dementia, and these medications
larly dangerous or distressing, then the symptoms may be have signicant adverse effects; therefore, they are gener-
treated judiciously with one of the agents discussed in the ally not recommended except for patients for whom other
following paragraphs [II]. The use of such agents should treatments have failed [III]. The antidepressant trazodone
be reevaluated and their benet documented on an ongo- and the selective serotonin reuptake inhibitors (SSRIs) are
ing basis [I]. also not well studied for symptoms other than depression
On the basis of good evidence, antipsychotic medica- but may be appropriate for nonpsychotic patients with ag-
tions are recommended for the treatment of psychosis in itation, especially for patients with mild agitation or prior
patients with dementia [II] and for the treatment of agita- sensitivity to antipsychotic medications [III].
tion [II]. These medications have also been shown to pro-
vide modest improvement in behavioral symptoms in 6. Treatment of Depression
general [I]. Evidence for the efcacy of these agents is Depression is common in patients with dementia. Pa-
based mostly on 612-week trials in nursing home resi- tients with depression should be evaluated for suicide risk
dents and outpatients. There is limited research on their [I]. Depressed mood may respond to improvements in the
use beyond 12 weeks, but considerable clinical experience patients living situation or to stimulation-oriented treat-
supports this practice [II]. Evidence for a difference in ef- ments [II]. Although evidence for antidepressant efcacy
cacy and safety among antipsychotic medications is lim- in patients with dementia and depression is mixed, clinical
ited. Antipsychotic medications as a group are associated consensus supports a trial of an antidepressant to treat
with a number of severe adverse events, including in- clinically signicant, persistent depressed mood [II]. The
creased risks for death, cerebrovascular accidents, tardive choice among agents is based on the side-effect prole of
dyskinesia, neuroleptic malignant syndrome, hyperlipid- specic medications and the characteristics of the individ-
emia, weight gain, diabetes mellitus, sedation, parkin- ual patient [I]. SSRIs may be preferred because they ap-
sonism, and worsening of cognition. Thus, they must be pear to be better tolerated than other antidepressants [II].
used with caution and at the lowest effective dosage [I], af- Bupropion, venlafaxine, and mirtazapine may also be ef-
ter considering the risks of not treating the psychiatric fective [II]. Agents with substantial anticholinergic effects
symptoms [I]. Patients and families should be advised (e.g., amitriptyline, imipramine) should be avoided [I].
about potential benets and risks of antipsychotic agents, Despite the lack of research data, clinical experience sug-
particularly the risk of mortality [I]. Second-generation gests that unilateral electroconvulsive therapy (ECT) may
(atypical) antipsychotics currently have a black box warn- be effective for patients who do not respond to pharma-
ing for increased risk of mortality in elderly patients; re- cological agents [II].
cent data suggest that rst-generation (typical) agents Treatments for apathy are not well supported, but psy-
carry at least a similar risk. High-potency agents tend to chostimulants, bupropion, bromocriptine, and amanta-
cause akathisia and parkinsonian symptoms; low-potency dine may be helpful [III]. Psychostimulants are also
agents tend to cause sedation, confusion, delirium, pos- sometimes useful in the treatment of depression in pa-
tural hypotension, and peripheral anticholinergic effects. tients with signicant general medical illness [III].
The decision of which antipsychotic to use is based on the
relationship between the side-effect prole and the char- 7. Treatment of Sleep Disturbances
acteristics of the individual patient [I]. Sleep disturbances are common in patients with demen-
Data demonstrating benet from benzodiazepines tia. Interventions include maintaining daytime activities
are modest, but benzodiazepines occasionally have a and giving careful attention to sleep hygiene [II]. Pharma-
role in treating patients with prominent anxiety [III] or cological intervention could be considered when other
on an as-needed basis for patients with infrequent epi- approaches have failed [II]. If a patient also requires med-
sodes of agitation or for those who require sedation for a ication for another psychiatric condition, an agent with
procedure such as a tooth extraction or a diagnostic ex- sedating properties, given at bedtime, could be selected
amination [II]. Adverse effects of benzodiazepines include [I]. For primarily treating the sleep disturbance, medica-
tions with possible effectiveness include trazodone, ate use of antipsychotic medications can relieve symptoms
zolpidem, or zaleplon [III], but there are few data on the and reduce distress and can increase safety for patients,
efcacy of specic agents. Benzodiazepines are not rec- other residents, and staff [I]. However, their use may be
ommended for other than brief use because of risks of associated with worsening cognitive impairment, overse-
daytime sedation, tolerance, rebound insomnia, wors- dation, falls, tardive dyskinesia, and neuroleptic malig-
ening cognition, falls, disinhibition, and delirium [II]. nant syndrome, as well as with hyperlipidemia, weight
Diphenhydramine is not recommended because of its an- gain, diabetes mellitus, cerebrovascular accidents, and
ticholinergic properties [II]. Antipsychotic medications death [I]. Thus, good clinical practice requires careful
should not be used solely for the purpose of treating sleep consideration and documentation of the indications and
disturbances [I]. available alternatives, both initially and on a regular on-
going basis [I]. A dose decrease or discontinuation should
8. Special Issues for Long-Term Care be considered periodically for all patients who receive
Many patients eventually require long-term-care place- antipsychotic medications [I]. A structured education pro-
ment; approximately two-thirds of nursing home patients gram for staff may help to both manage patients behavior
have dementia. Care should be organized to meet the and decrease the use of these medications in nursing
needs of patients, including those with behavioral prob- homes [II]. Physical restraints are rarely indicated and
lems [I]. Employing staff with knowledge and experience should be used only for patients who pose an imminent
concerning dementia and the management of difcult be- risk of physical harm to themselves or others [I]. Reasons
havior is important [II]. Special care units may offer more for the use of physical restraints should be carefully doc-
optimal care, although there is limited evidence that they umented [I]. The need for restraints can be decreased by
achieve better outcomes than traditional units [III]. environmental changes that decrease the risk of falls or
A particular concern is the use of physical restraints wandering and by careful assessment and treatment of
and medications to control disruptive behavior. Appropri- possible causes of agitation [II].
II. FORMULATION AND IMPLEMENTATION OF A

TREATMENT PLAN
The treatment of Alzheimers disease and related demen- agents or approaches are being used and problems persist
tias is inherently multidisciplinary and multimodal. It is (or new problems develop), it is advisable, if possible, to
guided by the stage of illness and is focused on the specic make one change at a time so that the effect of each
symptoms manifested by the patient. This discussion be- change can be assessed. The continuing utility of all inter-
gins with general principles of psychiatric management, ventions must be regularly reevaluated.
essential to the treatment of the patient with dementia, The site of treatment for an individual with dementia is
and then reviews specic treatments. These treatments determined by the need to provide safe and effective treat-
include the broad range of psychosocial interventions ment in the least restrictive setting. Approximately two-
used in dementia as well as the pharmacological options, thirds of patients with dementia live at home and receive
which are organized in the discussion by target symptom. care on an outpatient basis. The frequency of ofce or fa-
cility visits is determined by a number of factors, includ-
A. DETERMINING THE SITE OF TREATMENT AND ing the patients clinical status, the likely rate of change,
and the need for specic monitoring of treatment effects.
FREQUENCY OF VISITS Another factor is the reliability and skill of the patients
Choice of specic treatments for a patient with dementia caregivers, particularly regarding the likelihood of their
begins with the establishment of a specic diagnosis and notifying the clinician if a clinically important change oc-
an assessment of the symptoms being experienced by that curs. Most dementias are progressive, and symptoms
patient. A multimodal approach is often used, combining, change over time. Therefore, in order to offer prompt
for instance, behavioral and psychopharmacological in- treatment, enhance safety, and provide timely advice to
terventions as available and appropriate. When multiple the patient and family, it is generally necessary to see pa-
tients, usually together with their caregivers, at regular B. PSYCHIATRIC MANAGEMENT

follow-up visits. Patients who are clinically stable or are
taking stable doses of medications should generally be Successful management of patients with dementia re-
seen at a minimum of every 36 months. Patients who requires the concurrent implementation of a broad range of
quire active treatment of psychiatric complications should tasks, which are grouped under the term psychiatric
be seen regularly to adjust doses and monitor for changes management. These tasks help to maximize the patients
in target symptoms and side effects. Similarly, attempts to level of function and enhance the safety and comfort of
taper or discontinue psychotropic medications require patients and their families in the context of living with a
more frequent assessments than are required for routine difcult disease. In some settings, psychiatrists perform all
care. Weekly or monthly visits are likely to be required for or most of these tasks themselves. In others, they are part
patients with complex, distressing, or potentially danger- of multidisciplinary or interdisciplinary teams. In either
ous symptoms or during the administration of specic case, they must be aware of the full range of available
therapies. For example, outpatients with acute exacerba- treatments and take steps to ensure that any necessary
tions of depressive, psychotic, or behavioral symptoms treatments are administered. Good communication be-
may need to be seen as frequently as once or twice a week, tween the patients psychiatrist and primary care physician
sometimes in collaboration with other treating clinicians, ensures maximum coordination of care, may minimize
or be referred to intensive outpatient treatment or a par- polypharmacy, and may improve patient outcomes (4).
tial hospitalization program.
Individuals with dementia may need to be admitted to 1. Establish and Maintain an Alliance With the Patient and
an inpatient facility for the treatment of psychotic, affec- the Family
tive, or behavioral symptoms. In addition, they may need As with any psychiatric care, a solid therapeutic alliance is
to be admitted for treatment of general medical conditions critical to the treatment of a patient with dementia. The
co-occurring with psychiatric conditions. For patients care of a patient with dementia requires an alliance with
who are very frail or who have signicant general medical the patient, as well as with the family and other caregivers.
illnesses, a geriatric psychiatry or medical psychiatric unit Family members and other caregivers are a critical source
may be helpful when available (1). Indications for hospital- of information, as the patient is frequently unable to give
ization include symptom severity (e.g., signicant threats a reliable history, particularly as the disease progresses.
of harm to self or others, violent or uncontrollable behav- Because family members are often responsible for imple-
ior, inability to care for self or be cared for by others) and menting and monitoring treatment plans, their own atti-
intensity and availability of services needed (e.g., the need tudes and behaviors can have a profound effect on the
for continuous skilled observation, electroconvulsive ther- patient, and they often need the treating physicians com-
apy, or a medication or diagnostic test that cannot be per- passion and concern. For these reasons, treatment is di-
formed on an outpatient basis) (2, 3). The length of stay is rected to the patient-caregiver system. The needs of
similarly determined by the ability of the patient to safely caregivers will vary based on factors such as their relation-
receive the appropriate care in a less restrictive setting. ship to the patient, their long-standing role in the family,
Decisions regarding the need for temporary or perma- and their current customs. Clinical judgment is needed to
nent placement in a long-term-care facility often depend determine the circumstances in which it is appropriate or
on the degree to which the patients needs can be met in necessary to speak with caregivers without the patient
the community, either by relatives or other caregivers, ei- present, as well as how to proceed with clinical care when
ther in an assisted living facility or at home. The decision there are disputes among family members. A clear process
to remain at home should be reassessed regularly, with for medical decision making should be delineated for each
consideration of the patients clinical status and the con- patient, and a capacity assessment of the patient should be
tinued ability of the patients caregivers to care for the pa- performed when necessary.
tient, manage the burden of care, and utilize available
support services. The appropriate level of care may 2. Perform a Diagnostic Evaluation and Refer the Patient for
change over time, and patients often move from one level
Any Needed General Medical Care
of care to another during the course of dementia. If avail-
able, consultation with a social worker or geriatric case a. General Principles
manager may be benecial to assess the current support Patients with dementia should undergo a thorough diag-
system and facilitate referrals to additional services. At the nostic evaluation aimed at identifying the specic etiology
end of life, many patients with dementia are cared for in a of the dementia syndrome, because knowledge of the etiol-
hospice program. ogy may guide specic treatment decisions. In addition, the
evaluation should determine if any treatable psychiatric or tle or atypical symptoms actually has dementia as well as
general medical conditions (e.g., major depression, thyroid in more thoroughly characterizing an unusual symptom
disease, vitamin B12 deciency, hydrocephalus, structural picture. It is particularly useful in the evaluation of indi-
brain lesion) might be causing or exacerbating the demen- viduals who present with mild cognitive impairment (see
tia. The details of this evaluation are beyond the scope of Section IV.F.2), which requires evidence of memory
this guideline; the reader is referred to the American Acad- and/or other cognitive difculties in the presence of intact
emy of Neurology practice parameter on the diagnosis of functioning, and in the evaluation of individuals with the
dementia (5), the American Academy of Neurology prac- onset of dementia early in life. Testing may help to char-
tice parameter on early detection of dementia and mild acterize the extent of cognitive impairment, to distinguish
cognitive impairment (6), and the Agency for Health Care among the types of dementias, and to establish baseline
Policy and Research clinical practice guideline Recognition cognitive function. Neuropsychological testing may also
and Initial Assessment of Alzheimers Disease and Related De- help identify strengths and weaknesses that could guide
mentias (7) for more complete descriptions of the evalua- expectations for the patient, direct interventions to im-
tion of patients with dementia. A brief summary follows. prove overall function, assist with communication, and in-
The general principles of a complete psychiatric evalu- form capacity determinations.
ation are outlined in APAs Practice Guideline for the Psychi-
atric Evaluation of Adults (8). The evaluation of a patient c. Neuroimaging
with dementia frequently involves coordination with a The use of a structural neuroimaging study, such as com-
number of medical professionals, including the patients puterized tomography or magnetic resonance imaging
primary care physician (4). The physician with overall re- (MRI) scan, is generally recommended as part of an initial
sponsibility for the care of the patient oversees the evalu- evaluation, although clinical practice varies. Imaging is
ation, which should at a minimum include a clear history particularly important for those with a subacute onset
of the onset and progression of symptoms; a review of the (less than 1 year), symptom onset before age 65, vascular
patients medical problems and medications (including risk factors suggesting a higher likelihood of cerebrovas-
over-the-counter and herbal medications); assessment of cular involvement in their dementia, or a history or neu-
functional abilities; a complete physical examination and a rological examination ndings suggesting a possible focal
focused neurological examination; and a psychiatric exam- lesion. Nonetheless, clinically important lesions may be
ination, including a cognitive assessment that should in- found on neuroimaging in the absence of these indica-
clude at least a brief assessment of the cognitive domains of tions (11). The value of imaging in patients with late-stage
attention, memory, language, and visuospatial skills, ide- disease who have not been previously evaluated has not
ally used with age- and education-adjusted norms (9, 10). been established. Functional neuroimaging using brain
An assessment for past or current psychiatric illnesses that positron emission tomography (PET) scans may contrib-
might mimic or exacerbate dementia, such as schizophre- ute to diagnostic specicity in certain instances and has
nia or major depression, is also critical, as are laboratory been recently approved by Medicare for the indication of
studies, including a complete blood count (CBC), blood differentiating between Alzheimers disease and fronto-
chemistry battery (including glucose, electrolytes, cal- temporal dementia.
cium, and kidney and liver function tests), measurement of The development of additional imaging tools for im-
vitamin B12 level, and thyroid function tests. For some pa- proved diagnosis, early recognition, and more precise as-
tients, toxicology studies, syphilis serology, erythrocyte sessment of disease progression is a focus of current study.
sedimentation rate, HIV testing, serum homocysteine, a These additional tools include quantitative MRI, func-
lumbar puncture, or an electroencephalogram may also be tional MRI, use of investigational PET compounds, and
indicated. In general, many elements of the history will other methods aimed at imaging senile plaques in the
need to be obtained from the caregiver or the documented brain (12, 13).
medical record as well as from the patient. Often, it may be
necessary to conduct a portion of the interview with the d. Biomarkers
caregiver without the patient present, in order to allow for A wide variety of biomarkers are also under investigation
full disclosure of sensitive information. with the goal of enhancing diagnostic and prognostic
knowledge (14). Biomarkers of current interest include pro-
b. Neuropsychological Testing teins such as tau and amyloid beta protein in the cerebrospi-
Neuropsychological testing may be helpful in a number of nal uid (CSF) and plasma. Except in rare circumstances
ways. It may help in deciding whether a patient with sub- (notably the use of CSF-14-3-3 protein when Creutzfeldt-
Jakob disease is suspected and recent stroke or viral en- cic Alzheimers genetics resources are not available lo-
cephalitis can be excluded) (5, 15), these techniques re- cally, a referral to a professional genetic counselor or
main investigational, and there is insufcient evidence for clinical geneticist may help such families characterize
their utility in routine clinical practice. However, this area their risk and nd appropriate resources (27, 28).
is evolving rapidly, so recommendations may change with Genetic counseling and sometimes genetic testing may
new discoveries and the development of new markers also be appropriate for some patients with other dementias
and/or therapies. and a family history of similar syndromes. In particular, in-
dividuals with a clinical picture suggestive of frontotempo-
e. Genetic Testing ral dementia and a family history suggesting autosomal
Although genes involved in a variety of dementia syn- dominant inheritance can be tested for certain mutations
dromes have been identied (16), and family members of (29, 30). Likewise, individuals with a clinical picture sug-
patients with dementia are often concerned about their gestive of Huntingtons disease can be tested for the gene
risk of developing dementia, genetic testing is generally defect (31), and those suspected of having CADASIL (ce-
not part of the evaluation of patients with dementia except rebral autosomal dominant arteriopathy with subcortical
in very specic instances (5). In particular, testing for apo- infarcts and leukoencephalopathy) can be tested for asso-
lipoprotein E4 (APOE4) is not recommended for use in ciated Notch 3 gene polymorphisms (32).
diagnosis. Apolipoprotein E4 is one form of a gene on
chromosome 19 that is more common in individuals with
Alzheimers disease than in elderly individuals without de- 3. Assess and Monitor Psychiatric Status
mentia and is associated with late-onset Alzheimers dis- Ninety percent of patients with dementia develop a neu-
ease occurring with or without a family history (1719). ropsychiatric or behavioral symptom during the course of
However, it is also found in many elderly patients who do the disease (33). It is therefore important for the psychia-
not have dementia and is not found in many patients who trist to periodically assess the patient for the presence of
do have Alzheimers disease. Thus, the presence of an noncognitive psychiatric symptoms as well as for the pro-
APOE4 allele does not change the need for a thorough gression of cognitive symptoms.
workup and does not add substantially to diagnostic con- Both cognitive and noncognitive neuropsychiatric and
dence (5, 2022). behavioral symptoms of dementia tend to evolve over
First-degree relatives of patients with Alzheimers dis- time, so regular monitoring allows detection of new
ease have a risk of developing the disease that is two to symptoms and adaptation of treatment strategies to cur-
four times that of the general population. Three genes as- rent needs. For example, among the neuropsychiatric dis-
sociated with the disease have been identied in families turbances common in Alzheimers disease, depression is
with apparent autosomal dominant inheritance of early- reported more commonly early in the illness, whereas de-
onset Alzheimers disease. These genes include the amy- lusions and hallucinations are more common in the mid-
loid precursor protein (APP) gene on chromosome 21 dle and later stages, although any of these symptoms may
(23), presenilin 1 (PSEN1) on chromosome 14 (24), and occur at any stage of the disease (33, 34). It is particularly
presenilin 2 (PSEN2) on chromosome 1 (25). Genetic important to look for the emergence of such symptoms af-
testing is commercially available for PSEN1, which is ter a medication dose has been lowered or discontinued.
likely to be found in families with apparent autosomal Among the cognitive decits, memory loss is commonly
dominant inheritance and dementia developing before the earliest symptom, whereas language and spatial dys-
age 50 years. Testing for the other two genes is not com- function become more overt somewhat later.
mercially available but can sometimes be performed in the Among the neuropsychiatric symptoms that require
context of clinical genetics research. However, the role of ongoing assessment are depression (including major de-
such testing in clinical practice has not yet been estab- pression and other depressive syndromes), suicidal ide-
lished. Because no preventive treatments are currently ation or behavior, hallucinations, delusions, agitation,
available, testing should only be offered in the setting of aggressive behavior, disinhibition, sexually inappropriate
thorough pre- and posttest counseling (26). In addition, behavior, anxiety, apathy, and disturbances of appetite and
genetic testing is best done in conjunction with experts fa- sleep. Cognitive symptoms that almost always require as-
miliar with Alzheimers disease genetics, as test results re- sessment include impairments in memory, executive func-
quire careful interpretation. A referral to a local Alzheimers tion, language, judgment, and spatial abilities. It is often
Disease Research Center or the local chapter of the Alzhei- helpful to track cognitive status with a structured simple
mers Association may be helpful in locating someone who examination. If the same instrument is used repeatedly,
can provide the appropriate counseling and testing. If spe- the clinician should watch for practice effects. A detailed
assessment of functional status may also aid the clinician recommendations regarding adequate supervision, for
in documenting and tracking changes over time as well as example of medication administration, 4) make recom-
providing guidance to the patient and caregivers. Func- mendations regarding the prevention of falls and choking,
tional status is typically described in terms of the patients 5) address nutritional and hygiene issues, and 6) be vigi-
ability to perform instrumental activities of daily living lant regarding neglect or abuse. Patients who live alone
such as shopping, writing checks, basic housework, and require careful attention. Events that indicate that the pa-
activities of daily living such as dressing, bathing, feeding, tient can no longer live alone include several falls, re-
transferring, and maintaining continence. These regular peated hospitalization, dehydration, malnutrition,
assessments of recent cognitive and functional status pro- repeated errors in taking prescribed medications, dilapi-
vide a baseline for assessing the effect of any intervention, dated living conditions, or other signs of self-neglect.
and they improve the recognition and treatment of acute Other important safety issues in the management of pa-
problems, such as delirium. tients with dementia include interventions to decrease the
Whenever there is an acute worsening of cognition, hazards of wandering and recommendations concerning
functioning, behavior, mood, or psychosis, the clinician activities such as cooking, driving, hunting, and the oper-
should bear in mind that elderly persons in general and ation of hazardous equipment (see Section II.B.5). Care-
patients with dementia in particular are at high risk for givers should be referred to available books that provide
delirium associated with medications, general medical advice and guidance about maximizing the safety of the
problems, and surgery. Newly developing or acutely environment for patients with dementia (35).
worsening agitation in particular can be a sign of an occult
general medical condition (e.g., urinary tract infection, a. Suicidal Ideation
dehydration), untreated or undertreated pain, or physical All patients (and their caregivers) should be asked about
or emotional discomfort. Elderly patients may not mani- the presence of wishes for death, suicidal ideation, suicide
fest certain typical signs or symptoms such as fever in the plans, as well as a history of previous self-injurious behav-
face of infection or pain during a myocardial infarction. ior. If suicidal ideation occurs in patients with dementia, it
Thus, a thoughtful assessment of the patients overall sta- tends to be earlier in the disease, when insight is more
tus and a general medical evaluation must precede any in- likely to be preserved. It is a particular concern in patients
tervention with psychotropic medications or physical who are clinically depressed but can also occur in the ab-
restraint, except in an emergency. Assessments should also sence of major depression. Elderly persons in general and
include examination of the patients sensory function, elderly men in particular are at increased risk for suicide,
since sensory decits can precipitate or worsen psychiatric although the diagnosis of dementia is not known to confer
and cognitive symptoms and increase the risk that patients added risk. Interventions to address suicidal ideation are
will make medication errors. similar to those for patients without dementia and include
Before undertaking an intervention, the psychiatrist psychotherapy; pharmacotherapy; removal of potentially
should enlist the help of caregivers in carefully charac- dangerous items such as medications, guns, or vehicles;
terizing the target symptoms. Their nature, intensity, increased supervision; and hospitalization. Factors affect-
frequency, precipitants, and consequences should be re- ing the choice of intervention include the nature and in-
viewed and documented. This process is critical to reveal- tensity of the suicidal ideation or behavior and the
ing the cause of the symptoms, as well as monitoring the capacity and support system of the patient (36).
impact of any intervention. This approach also assists b. Agitation and Aggression
caregivers in beginning to achieve some mastery over the Agitation is an umbrella term that refers to a range of be-
problematic symptom. Before embarking on any inter- havioral disturbances, including physical aggression, com-
vention, it is also helpful if clinicians explicitly review bativeness, threatening behavior, persistent or intermittent
their own, the patients, and the caregivers expectations. psychomotor hyperactivity, and disinhibition. These be-
haviors pose a particular problem for patients cared for at
4. Monitor and Enhance the Safety of the Patient home, especially by frail spouses. Agitation is more likely to
and Others occur later in the course of dementia and often has multiple
It is important for the psychiatrist treating a patient with causes. New or worsened agitation can result from an oc-
dementia to regularly assess cognitive decits or behavioral cult general medical problem, medication side effects, un-
difculties that potentially pose a danger to the patient or treated or undertreated pain, constipation, depression,
others. The psychiatrist should 1) assess suicidality, 2) as- psychotic symptoms, or delirium. Thus, the rst priority is
sess the potential for aggression and agitation, 3) make a careful medical evaluation, because the agitation will of-
ten resolve with treatment of an underlying condition. The used to treat agitation or combativeness that puts the pa-
next step is an assessment of other features of the patients tient or others at risk. Nonetheless, principles of humane
overall situation. Hunger or sleep deprivation can provoke care as well as federal regulations support minimizing re-
agitation, as can interpersonal or emotional stressors such straint use as much as possible. In addition, some evidence
as undergoing a change in living situation, caregiver, or suggests that restraints may increase the risk of falls and
roommate or experiencing frustration, boredom, loneli- contribute to cognitive decline (42, 43) and that reducing
ness, or overstimulation. Consequently, attending to un- restraint use can decrease the rate of serious injuries
met needs, providing reassurance, redirecting activities, or among nursing home residents (44).
matching the level of stimulation to the patients current
level of activation may resolve the problem (37). c. Supervision
In designing an intervention to treat a problematic be- Decisions regarding supervision of the patient should take
havior, a structured approach should be taken to facilitate into consideration the patients cognitive decits, the home
selecting the optimal treatment and monitoring the effect environment, and the consequent risk of dangerous activi-
of that treatment (3840). The rst step is to carefully de- ties. For instance, a patient with signicant cognitive im-
scribe the target behavior, including where, when, and pairment may not be safe alone at home because he or she
how often it occurs. The next step is to assess the specic might improperly administer medications, be unable to
antecedents and consequences of each problem behavior, cope with a household emergency, or use the stove, power
which will often suggest specic strategies for interven- tools, or other equipment in a dangerous manner. Home
tion. Activities that consistently precede the problem be- occupational therapy functional and safety assessments, as
havior may be acting as precipitants and should be well as other community-based services, may be helpful in
avoided whenever possible. If the activity is a necessary determining whether increased supervision is needed.
one, for example, bathing, it may be helpful to decrease its
frequency or to alter the environment so that the negative d. Falls
consequences are minimized (e.g., switch bath time to al- Psychiatrists caring for patients with dementia should be
low a home health aid to supervise, or change the location aware that falls are a common and potentially serious
of baths to decrease the impact of aggressive outbursts on problem for all elderly individuals, especially those with
family members or other patients). When multistep activ- dementia. Falls can lead to hip fracture, head trauma, and
ities such as dressing and eating precipitate problem be- a variety of other injuries, including subdural hematomas,
haviors such as aggression, it often helps to simplify the which may further worsen cognitive function. A number
activities (e.g., using clothing with Velcro closures, serv- of interventions to prevent falls in elderly people have
ing several simple nutritious snacks instead of a large been shown to be effective (45). One of the most efca-
meal). Whatever the intervention, it is critical to match cious is withdrawing medications that are associated with
the level of demand on the patient with his or her current falls, central nervous system sedation, or cardiovascular
capacity, avoiding both infantilization and frustration. side effects (especially orthostatic hypotension), when ap-
Likewise, behavior may also improve by modifying the propriate. If gait disturbances are present, canes, walkers,
environment insofar as possible to compensate for the pa- or other supports may be helpful unless they are otherwise
tients decits and to capitalize on his or her strengths contraindicated (e.g., if their use poses a hazard to others).
(41). In assessing the effectiveness of interventions for Patients at high risk for falling may need to be closely su-
problematic behaviors, clinicians can recommend that pervised while walking.
caregivers maintain a log of specic behaviors as well as Environmental modications can also help reduce the
their intensity, frequency, precipitants, and consequences. risk of falls. The removal of loose rugs, low tables, and
If the agitation is deemed dangerous to the patient or other obstacles can diminish risk. The use of lower beds,
others, it is important to undertake further measures to night-lights, bedside commodes, and/or frequent toilet-
enhance safety. Such additional measures may include ing may help prevent falls at night. Although bed rails are
providing one-on-one care, instituting the behavioral thought to prevent patients from rolling out of bed, they
measures discussed in Section II.C.4, or initiating phar- may actually increase the risk of falls. Therefore, other
macological treatment as discussed in Section II.C.5. If environmental modications such as lowering the bed or
agitation and aggressive behavior cannot be brought un- placing a mattress on the oor are typically recom-
der control, hospitalization and/or nursing home place- mended. Bed and chair monitors have also been suggested
ment must be considered. as a way to alert caregivers or nursing staff when patients
Within hospital or nursing home settings, physical re- may be getting out of bed or leaving a chair. In addition,
straints (e.g., Posey restraints, geri-chairs) are sometimes programs for muscle strengthening and balance retraining
have been shown to be helpful in reducing falls in elderly grids/stripes of tape have been tried, there is no evidence
people (45). A physical therapy evaluation may be appro- that these subjective barriers prevent wandering in cogni-
priate for certain patients. For patients in acute inpatient tively impaired people (47). If patients are prevented from
or nursing home settings, restraints are occasionally used leaving on their own, adequate supervision must be pro-
on a temporary basis to reduce the likelihood of falling. vided to ensure emergency egress. Pharmacotherapy is
Under such circumstances, documentation should reect rarely effective in the treatment of wandering unless the
the rationale for the temporary use of restraints and wandering is due to an associated condition such as mania.
should include a discussion of the other measures that In addition, provision should be made for locating pa-
were tried and failed to bring the behavior under control. tients should wandering occur. Such measures include
sewing or pinning identifying information onto clothes,
e. Abuse and Neglect placing medical-alert bracelets on patients, and ling
The psychiatrist should be alert to the possibility of elder photographs with local police departments. Referrals to
abuse, nancial exploitation, and neglect. Individuals with the Safe Return Program of the Alzheimers Association
dementia are at particular risk for abuse because of their (1-888-572-8566; http://www.alz.org/safereturn) or sim-
limited ability to protest, their lack of comprehension, and ilar programs provided by local police departments or
the signicant demands and emotional strain on care- other organizations should be considered for patients at
givers. Patients whose caregivers appear angry or frus- risk of wandering.
trated may be at even higher risk. Any concern, especially
one raised by the patient, must be thoroughly evaluated.
Corroborating evidence (e.g., from physical examination)
5. Advise the Patient and Family Concerning Driving
should be sought in order to distinguish delusions, halluci- (and Other Activities That Put Other People at Risk)
nations, and misinterpretations from actual abuse. In many Most of the available evidence suggests that dementia,
states, when neglect or abuse is suspected, the psychiatrist even when mild, impairs driving performance to some ex-
is required to make a report to the appropriate local or state tent and that the risk of accidents increases with increas-
agency responsible for investigating elder abuse. ing severity of dementia (48). For example, compared to
age-matched controls, individuals with probable Alzhei-
f. Wandering mers disease had more difculties comprehending and
Families should be advised that patients with dementia operating a driving simulator, drove off the road more of-
may wander away from home and that wandering may be ten, spent more time driving considerably slower than the
dangerous to patients. Some patients are unable to nd posted speed limit, applied less brake pressure in stop
their way back, whereas others lack the judgment to rec- zones, spent more time negotiating left turns, and drove
ognize and deal with dangerous situations. Wandering has more poorly overall (49). Nonetheless, it is well docu-
been associated with more severe dementia and dementia mented that many individuals with dementia, even some
of longer duration. It has also been associated with de- with fairly serious impairment, continue to drive, raising
pression, delusions, hallucinations, sleep disorders, neu- signicant public health concerns (5054).
roleptic medication use, and male gender (46). Provision In an ofce or hospital setting, accurate assessment of
of adequate supervision is important to prevent patients functional abilities such as driving is not possible (55).
from wandering. However, since walking may be bene- Furthermore, the inuence of neuropsychiatric impair-
cial, both as stimulation and exercise, it should not be lim- ments or behavioral symptoms on driving performance is
ited unnecessarily. Providing access to a large, safe area neither clear-cut nor predictive (56, 57). However, risks of
for walking or opportunities for supervised walks is ideal. driving should be discussed with all patients with demen-
Environmental changes may also be necessary to prevent tia and their families, and these discussions should be
unsupervised departures. At home, the addition of a more carefully documented. Discussions should include an ex-
complex or less accessible door latch may be helpful. Elec- ploration of the patients current driving patterns, transpor-
tronic devices to reduce the risk of in-home wandering are tation needs, and potential alternatives. The psychiatrist
under development. If wandering occurs at night when should also ask the family about any history of getting lost,
caregivers are asleep, pharmacological intervention may trafc accidents, or near accidents. For patients with de-
be indicated. In institutional settings, electronic locks or mentia who continue to drive, the issue should be raised
electronic devices that trigger an alarm when the patient repeatedly and reassessed over time. This is especially
tries to leave may be used. true for patients with Alzheimers disease or other pro-
Although a number of interventions of visual and gressive dementias in which driving risk will predictably
other selective barriers such as mirrors, camouage, and worsen over time (58).
At this time, there is no clear consensus regarding the In individuals with moderate impairment (e.g., those
threshold level of dementia at which driving should be who cannot perform moderately complex tasks, such as
curtailed or discontinued (48, 5861). In mild dementia, preparing simple meals, household chores, yard work, or
the driving risk is greater than for age-matched individu- simple home repairs), there is some evidence and strong
als without dementia, although it is less than that for cog- clinical consensus that driving poses an unacceptable risk
nitively intact young drivers (e.g., younger than age 25 and patients should be instructed not to drive (48, 5961).
years) (48). Thus, some clinicians argue that in mild de- Those with severe impairment are generally unable to
mentia the benets to the patient of continued indepen- drive and certainly should not do so.
dence and access to needed services outweigh the risk of Advice about driving cessation should be communi-
an accident. Other clinicians argue that no patient with a cated to family members, as well as to the patient, because
diagnosis of dementia should drive, because the risk of an the burden of implementing the decision often falls on
accident is elevated even in patients with mild dementia, families. The psychiatrist can also lend moral authority
and it is impossible to say at what point this risk becomes and support to family members who wish to restrict driv-
unacceptable. In an evidence-based review of driving and ing but are reluctant to take responsibility for the decision
Alzheimers disease from the American Academy of Neu- (e.g., writing on a prescription pad, DO NOT DRIVE).
rology, it was found that driving was only mildly impaired Eventually, when the point is reached where the danger of
in drivers with a Clinical Dementia Rating (CDR) of 0.5 continued driving is undeniable, the psychiatrist can pro-
(mild cognitive impairment), but those with a CDR of 1 vide concrete advice regarding how best to accomplish
(mild or early stage dementia) were found to pose signif- cessation of driving (e.g., confrontation regarding risks to
icant risks from increased vehicular accidents and poorer grandchildren, discussion of the impact on insurance cov-
driving performance (48) (see Section I.V.E for informa- erage and rates, removing the car from view, hiding the
tion on the staging of dementia). keys, or removing ignition wires). The American Medical
Additional increases in risk may also be associated with Association publication, Physicians Guide to Counseling
a diagnosis of dementia with Lewy bodies. Concomitant and Assessing Older Drivers (http://www.ama-assn.
neurological symptoms such as motor decits (e.g., due org/ama/pub/category/10791.html) may be helpful to
to stroke or a parkinsonian syndrome, impairments in some clinicians (67). When making recommendations to
praxis), sensory decits (e.g., spatial neglect, visual loss, limit or stop driving, clinicians should be sensitive to the
deafness), or decits in judgment, coordination, process- signicant psychological meaning of giving up driving. In
ing speed, and reaction time are also thought to increase addition, patients and their families will need to make
risk, although this view has not been conrmed by re- plans for alternative modes of transportation (60, 61, 68).
search (56, 6264). Finally, general medical problems A social service referral may be helpful for some families to
(e.g., symptomatic cardiac arrhythmia, syncope, seizures, help with transportation arrangements and costs.
poorly controlled diabetes) or the use of sedating medi- Psychiatrists should familiarize themselves with state
cations may also impair driving ability. A history of at- motor vehicle regulations for reporting individuals with
fault trafc incidents may also signal increased risk (65). dementia. In some states, disclosure is forbidden. In oth-
Thus, in individuals with mild dementia and one or more ers, a diagnosis of dementia or Alzheimers disease must
of these additional factors, driving cessation may be par- be reported to the state department of motor vehicles, and
ticularly indicated. the patient and family should be so informed. In many
Patients with milder impairment may also need to con- states, the physician may breach condentiality to inform
sider giving up driving. For those who are unwilling to do the state motor vehicle department of a patient who is
so, it may be helpful to advise them to limit their driving judged to be a dangerous driver. This option is appropri-
to conditions likely to be less risky (e.g., familiar locations, ate for patients with signicant dementia who refuse to
modest speeds, good visibility, clear roads) (66). The pa- stop driving and whose families are unwilling or unable to
tients spouse or other individual may act as a navigator or stop them.
assessor of driving skill, but the utility of this strategy is Although the data and recommendations just de-
unproven, and passengers may be injured in the event of scribed refer to the operation of motor vehicles, similar
an accident (60, 61). Mildly impaired patients who wish to principles apply to the operation of other equipment that
have an independent assessment of their driving skills may puts the patient and others at risk. Thus, patients whose
be referred to an occupational therapist, rehabilitation leisure or work activities involve rearms, use of heavy
center, driving school, or local department of motor vehi- machinery, aircraft, lawn mowers, or other dangerous
cles, but the predictive value of these assessments for ac- equipment or material will need to have these activities
tual driving performance has not been established. limited and discontinued as the disease progresses.
6. Provide Education and Support to Patients and Families tients behavior (72). Section II.B.6.b includes suggestions
for reading materials that may be helpful in providing ed-
a. Educate the Patient and Family About the Illness and ucation to families and caregivers.
Available Treatments The family should be educated regarding basic princi-
An important task of the psychiatrist who cares for an in- ples of care, including 1) recognizing declines in capacity
dividual with dementia is providing or coordinating the and adjusting expectations appropriately, 2) bringing sud-
education of the patient and family regarding the illness den declines in function and the emergence of new symp-
and its natural history. Often the rst step is to communi- toms to professional attention, 3) keeping requests and
cate and explain the diagnosis of dementia, including the demands relatively simple, 4) deferring requests if the pa-
specic dementia etiology, if known. Terms should be tient becomes overly upset or angered, 5) avoiding overly
claried at the outset to facilitate communication. Pa- complex tasks that may lead to frustration, 6) not confront-
tients vary in their ability and desire to understand and ing patients about their decits, 7) remaining calm, rm,
discuss their diagnosis. Most mildly and some moderately and supportive and providing redirection if the patient be-
impaired individuals are able to discuss the matter at some comes upset, 8) being consistent and avoiding unnecessary
level, but the discussion must be adapted to the specic change, and 9) providing frequent reminders, explana-
concerns and abilities of the patient; it may be helpful to tions, and orientation cues. For example, when arriving
seek the familys input regarding the nature and timing of with visitors, families should say, This is your nephew,
any discussion with the patient (69). The issue of disclo- your sisters son rather than repeatedly testing a patients
sure of the diagnosis to the patient is complex because memory by saying Do you remember who this is? It is
many patients cannot recognize their decits. Decisions also important to individualize the approach to the pa-
about how to disclose should take into account factors tients needs, and, in this regard, psychiatrists and other
such as cultural issues that might modify the patients de- mental health care professionals can offer more specic
sire to receive such information (70). In most cases, the behavioral interventions that caregivers can use to avoid or
psychiatrist will have an explicit discussion with family deal with difcult behaviors. For additional details on such
members regarding the diagnosis, prognosis, and treat- interventions, see Sections II.B.4.b and II.C.4.
ment options, adapted to the unique concerns of the pa-
tient and family. This discussion will likely span a number b. Refer the Family to Appropriate Sources of Care and Support
of ofce visits. Certain specic symptoms (e.g., psychosis, Family members often feel overwhelmed by the combina-
extrapyramidal symptoms) are predictive of more rapid tion of hard work and personal loss associated with caring
decline and thus may be used in tandem with other fea- for an individual with dementia. The caring and prag-
tures to assess prognosis (71). matic attitude of the psychiatrist may provide critical sup-
It is important to educate the patient and family about port. This attitude may be expressed through thoughtful
the range of symptoms that could develop in the current inquiries about current needs and how they are being met,
stage of dementia or that may develop in the future. This advice about available sources of emotional and practical
education allows them to plan for the future and to recog- support, referrals to appropriate community resources,
nize emergent symptoms that should be brought to med- and supportive psychotherapy.
ical attention. Family members and other caregivers may Programs have been developed that reduce the burden
be particularly concerned about behavioral and neuropsy- and lessen the stress and depression associated with long-
chiatric symptoms, which they often associate with a loss term caregiving. These interventions include psychoedu-
of dignity, social stigma, and an increased caregiving bur- cational programs for coping with frustration or depres-
den. It may be helpful to reassure patients and their fam- sion; psychotherapy focused on alleviating depression and
ilies that these symptoms are part of the illness and are anxiety, and improving coping; exercise interventions for
direct consequences of the damage to the brain. More- caregivers; and workshops in stress management tech-
over, they may be relieved to know that although cogni- niques (7377). In addition, extensive clinical experience
tive losses are generally not reversible, neuropsychiatric and substantial scientic literature demonstrate that sup-
symptoms, especially the more disruptive ones, can often port groups, especially those combining education with
be improved or even eliminated with treatment, resulting support, improve caregiver well-being (7885). Support
in an overall increase in functional status and comfort. By groups conforming to this general pattern are available in
treating these symptoms, educating family caregivers, and many localities through local chapters of the Alzheimers
providing them with alternative strategies to deal with the Association and/or hospitals, community organizations,
patients disruptive behaviors, the psychiatrist can help to and religious groups. Support groups may vary widely in
minimize the caregivers negative reactions to the pa- their approaches as well as composition, and caregivers
may elect to try several before nding one that suits them. Thirty-Six Hour Day: A Family Guide to Caring for Persons
In addition to providing helpful information about the With Alzheimers Disease, Related Dementing Illness, and
disease, how to care for someone with the disease, and Memory Loss in Later Life (94); Mayo Clinic: Guide to Alz-
ways to decrease caregiver burden, these groups may en- heimers Disease: The Essential Resource for Treatment, Cop-
hance the quality of life of patients and spouses or other ing, and Caregiving (95); Practical Dementia Care (41); or
caregivers and may delay nursing home placement (79, The Complete Guide to Alzheimers-Proong Your Home (35)
8688). Internet message boards and chat rooms may also or view informational video media that may be available
be helpful for some caregivers. from the local Alzheimers Association chapter or public
In addition to providing families with information on library.
support groups, there are a number of benets of referral to
the local chapter or national ofce of the Alzheimers Asso- c. Watch for Signs of Caregiver Distress
ciation (1-800-272-3900; http://www.alz.org), the Alzhei- With or without support, caregivers frequently become
mers Disease Education and Referral Center (ADEAR) frustrated, overwhelmed, or clinically depressed (96).
(1-800-438-4380; http://www.nia.nih.gov/Alzheimers/), and Among the causes of demoralization are the progressive
other support organizations. Services offered by these or- nature of dementia and the patients lack of awareness of
ganizations include providing information about local re- the extent of support being provided. Psychiatrists caring
sources, operating hotlines staffed by well-informed for patients with dementia should be vigilant for these
volunteers, offering caregiver support services, and distrib- conditions in caregivers, because they increase the risk of
uting a wide array of educational material written for pa- substandard care, neglect, or abuse of patients and are a
tients, caregivers, and health professionals. sign that the caregivers themselves are in need of care.
Many other resources provide logistical support for Signs of caregiver distress include increased anger, social
caregivers who are trying to care for individuals with de- withdrawal, anxiety, depression, exhaustion, sleeplessness,
mentia at home. Respite care allows the caregiver periods irritability, poor concentration, increased health prob-
of relief from the responsibilities of dementia care. It pro- lems, and denial. When a caregiver is in signicant dis-
vides essential physical and emotional support, serving the tress, his or her need for greater psychosocial support
dual purposes of decreasing the burden of care and allow- should be evaluated. If treatment is indicated, it can be
ing caregivers to continue to work, participate in recre- provided (according to the preference of psychiatrist, pa-
ational activities, or fulll other responsibilities. Respite tient, and caregiver) by the patients psychiatrist or
care may last for hours to weeks and may be provided through a referral to another mental health professional.
through companions, home health aides, visiting nurses,
day care programs, and brief nursing home stays or other d. Support Families During Decisions About Institutionalization
temporary overnight care. Depending on the available lo- When family members feel that they are no longer able to
cal resources and individual circumstances, these types of care for the patient at home, they may need both logistical
care may be available from local senior services agencies, and emotional support in placing the patient in a long-
from the local chapter of the Alzheimers Association, re- term-care facility (i.e., continuing care retirement com-
ligious groups, U.S. Department of Veterans Affairs facil- munity, group home, assisted living facility, or nursing
ities, or other community organizations. Although respite home). Often, such transitions occur at times of crisis
care clearly provides benet for the caregiver, the evi- (e.g., medical hospitalizations or caregiver illness). The
dence is mixed as to whether these programs actually de- psychiatrist can be a valuable resource in informing fam-
lay institutionalization (8993). Clinical experience ilies about the available options and helping them evaluate
suggests that by decreasing caregiver burden these pro- and anticipate their needs in the context of their values,
grams may also improve the quality of life for patients priorities, and other responsibilities. The question of re-
and their families. Other resources that may be helpful ferral to a long-term-care facility should be raised well be-
include social service agencies, community-based social fore it becomes an immediate necessity so that families
workers, home health agencies, cleaning services, Meals who wish to pursue this option have time to select and ap-
on Wheels, transportation programs, geriatric law spe- ply for a suitable facility, plan for nancing long-term
cialists, and nancial planners. Useful information for care, and make needed emotional adjustments. A referral
caregivers from the Family Caregiver Alliance is avail- to a social service agency, social worker, or the local chap-
able at http://www.caregiver.org. ter of the Alzheimers Association may assist with this
Many clinicians also recommend that families read ar- transition. Some social service agencies provide compre-
ticles or books written specically for lay readers inter- hensive home service assessments that may help families
ested in understanding dementia and its care, such as The recognize and address their needs.
7. Advise the Family to Address Financial and Legal Issues decision maker does not exist, the closest relative is typi-
Patients with dementia usually lose the ability to make cally asked to provide consent. Nevertheless, the psychi-
medical, legal, and nancial decisions as the disorder atrist is encouraged to be familiar with local jurisdictional
progresses, and consequently these functions must be requirements, because procedures vary by state and some
taken over by others (97). Clinical evaluation, including states require judicial review.
cognitive testing when needed, can assist in determining Patients may also transfer authority for legal and -
whether a patient with Alzheimers disease has the capac- nancial decision making in the form of a durable power of
ity to make medical decisions (98100). attorney for nancial matters. At a minimum, it is recom-
If family members act while the patient is still able to mended to include a family member as a cosigner on any
participate, they can seek his or her guidance regarding bank accounts so that payment of expenses can proceed
long-term plans. This approach can help in incorporating smoothly even when the patient is no longer able to com-
the patients own wishes and values into the decision- plete the task him- or herself. In some instances, it may
making process, as well as in avoiding future conict. Al- be a good idea to warn families about the vulnerability of
though the specic laws vary from state to state, advance individuals with dementia to unscrupulous individuals
planning regarding health care and nances can help fam- seeking charitable contributions, selling inappropriate
ilies avoid the difculty and expense of petitioning the goods, or promoting sweepstakes. If needed, the family
courts for guardianship or conservatorship should such can ask the patient to give up charge cards, ATM cards,
arrangements become necessary later in the illness. Issues and checkbooks to prevent the loss of the patients re-
that might be raised related to health care in the later sources. Clinicians should remain vigilant for evidence of
stages of the illness include preferences about medical exploitation of patients.
treatment, the use of feeding tubes, the care desired for Patients should be advised to complete or update their
infections and other potentially life-threatening medical wills while they are able to make and express decisions
conditions, and articial life support. Medical decision (103). Patients and families should also be advised of the
making can be transferred in advance to a trusted family importance of nancial planning early in the illness. This
member (or friend) in the form of a durable power of at- advice may include a frank discussion regarding the nanc-
torney for health care or designation of a health care ing of home health care and/or institutional care. Unfor-
agent. For some patients, a living will or advance directive tunately, once the diagnosis of dementia is established, it is
may also be appropriate, but which document is used and often too late to purchase long-term-care insurance, but
its specic features depend on the prevailing state law. careful planning in the early stages may help to lessen the
Patients and family members should be offered the burden of nursing home care or home health services later
opportunity to discuss preferences about participation in in the disease course. A patient with more complex nan-
research studies early in the course of the illness, while cial issues should be referred to an attorney or nancial
the patient is still able to make his or her wishes known planner to establish appropriate trusts, plan for transfer of
(101). The Alzheimers Association has developed recom- assets, and make other nancial arrangements.
mendations for Institutional Review Boards and investi-
gators for obtaining research consent for cognitively C. DEVELOPMENT AND IMPLEMENTATION OF A
impaired adults (102).
STAGE-SPECIFIC TREATMENT PLAN
An individuals capacity to understand and give consent
to a particular intervention (including taking of medica- The treatment of dementia varies through the course of
tions, particularly those with potentially signicant side the illness, because symptoms evolve over time. Although
effects) will vary over time and with the nature and com- many symptoms can and do occur throughout the illness,
plexity of the intervention (99, 100). As individuals with certain symptoms are typical of the broad stages, as out-
dementia become more impaired, responsible family lined in Section IV.E. This outline of stages conforms
members are usually brought into the consent discussion. most to the typical course of Alzheimers disease, but it
When a patients capacity is diminished but still sufcient does not apply as well to other types of dementias, partic-
to give consent, consent or at least agreement is usually ularly the frontotemporal dementia spectrum disorders.
obtained from both patient and family member. Once a The following sections provide general recommenda-
patient no longer has adequate decisional capacity, con- tions for treating patients in three stages of illness (mild,
sent is obtained from either a health care proxy decision moderate, and severe) and specic recommendations for
maker designated in an advance directive or a guardian, if the implementation of select psychotherapeutic and phar-
either has been named. When such a legally designated macological treatments. The evidence supporting the ef-
cacy of these treatments is reviewed in Section V of this psychotherapeutic intervention, as described in Section
guideline. At each stage of the illness, the psychiatrist II.C.5.c. Patients with moderate to severe major depres-
should be vigilant for cognitive and noncognitive symp- sion who do not respond to or cannot tolerate antidepres-
toms likely to be present and should help the patient and sant medications should be considered for ECT. Mildly
family anticipate future symptoms. The family may also impaired patients should also be carefully assessed for sui-
benet from reminders to plan for the care likely to be cidality, even if they are not obviously depressed.
necessary at later stages.
2. Moderately Impaired Patients
1. Mildly Impaired Patients As patients become more impaired, they are likely to re-
At the early stages of a dementing illness, patients and quire more supervision to remain safe, and safety issues
their families are often dealing with acceptance of the ill- should be addressed as part of every evaluation (see Sec-
ness and recognition of associated limitations. They may tion II.B.4). Families should be advised about the possibil-
benet from pragmatic suggestions for how to cope with ity of accidents due to forgetfulness (e.g., res while
these limitations (e.g., making lists, using a calendar, cooking), of difculties coping with household emergen-
avoiding overwhelming situations such as certain child- cies, and of the possibility of wandering. Family members
care responsibilities). Patients may benet from referral should also be advised to determine whether the patient is
to health promotion activities and recreation clubs (104). handling nances appropriately and to consider taking
It may be helpful to identify specic impairments and over the paying of bills and other responsibilities. At this
highlight remaining abilities. Patients often experience a stage of the disease, nearly all patients should not drive.
sense of loss and perceived stigma associated with the ill- Families should be counseled to undertake measures to
ness. Consequently, psychotherapeutic interventions may prevent patients from driving, as many patients lack in-
be helpful for patients who are struggling with the diag- sight into the risk that their continued driving poses to
nosis and its implications. Features of treatment plan de- themselves or others (as described in Section II.B.5).
velopment for mildly impaired patients that have already As a patients dependency increases, caregivers may be-
been outlined in detail include addressing the issue of gin to feel more burdened. A referral for some form of re-
driving cessation (see Section II.B.5), assigning a durable spite care (e.g., home health aid, day care, brief assisted
power of attorney and addressing other legal and nancial living, or nursing home stay) may be helpful. At this stage,
matters (see Section II.B.7), and addressing caregiver families should begin to consider and plan for additional
well-being (see Section II.B.6.b). Support groups for pa- support at home as well as discuss the patients possible
tients and families with mild Alzheimers disease exist in transfer to a long-term-care facility. Family members may
many communities. differ in their opinion of the patients level of functioning
Patients with early Alzheimers disease should be of- and may have different psychological responses to the pa-
fered a trial of one of the three available cholinesterase in- tients impairments, generating family conict. It may be
hibitors approved and commonly used for the treatment benecial to meet with family members to openly discuss
of cognitive impairment (i.e., donepezil, rivastigmine, these issues.
galantamine), after a thorough discussion of their poten- Treatment for cognitive symptoms should also be con-
tial risks and benets. Given the possible risks of long- sidered. For patients with Alzheimers disease, currently
term high-dose vitamin E and selegiline and the minimal available data suggest that the combination of a cholines-
evidence for their benet, they are no longer recom- terase inhibitor plus memantine is more likely to delay
mended. Specic recommendations for implementing symptom progression than a cholinesterase inhibitor
these treatments are provided in Section II.C.5.a. Mildly alone during this stage of the illness. Specic implemen-
impaired patients may also be interested in referrals to lo- tation of these treatments is described in Section II.C.5.a.
cal research centers for participation in clinical trials of Delusions and hallucinations are prevalent in moder-
experimental agents for the treatment of early Alzheimers ately impaired patients, as are agitation and combative-
disease. Additional information regarding such trials may ness. The patient and family may be troubled and fearful
be obtained from a local or the national chapter of the about these symptoms, and it may be helpful to reassure
Alzheimers Association, from the National Institute on them that the symptoms are part of the illness and are of-
Aging, or at http://www.clinicaltrials.gov. ten treatable. Therapeutic approaches to these symptoms
Mildly impaired patients should be evaluated for neu- are described in Section II.C.5.b. For patients in whom
ropsychiatric symptoms, especially depressed mood or wandering is the only symptom, pharmacotherapy will
major depression, which may require pharmacological or rarely be indicated. Depression often remains part of the
picture at this stage and should be treated vigorously (105). In addition, some patients may benet from more specic
The pharmacotherapy of behavioral and neuropsychiatric psychosocial interventions. These more specic psychoso-
symptoms is described in Sections II.C.5.b, II.C.5.c, and cial treatments for dementia can be divided into four broad
II.C.5.d. groups: behavior oriented, emotion oriented, cognition
oriented, and stimulation oriented. Although these treat-
3. Severely and Profoundly Impaired Patients ment approaches differ in philosophy, focus, and methods,
At this stage of the illness, patients are severely incapaci- they share the broadly overlapping goals of improving
tated and are almost completely dependent on others for quality of life and maximizing function in the context of
help with basic functions, such as dressing, bathing, and existing decits (see references 112 and 113 for a compre-
feeding. Families are often struggling with a combined hensive review). Many of these therapies have the im-
sense of burden and loss and may benet from a frank ex- provement of cognitive skills, mood, or behavior as an
ploration of these feelings and any associated resentment additional goal. All of these approaches reect a person-
or feelings of guilt. They may also need encouragement to centered philosophy of care in which an understanding of
get additional help at home or to consider transient re- the individual is emphasized (114). For many individuals,
spite or relocation of the patient to a nursing home. several modalities will be selected at the same time. Be-
Of the cholinesterase inhibitors, only donepezil has thus cause these treatments generally do not provide lasting ef-
far been approved for use in late-stage disease, and some fects, those that can be offered regularly may be the most
studies show that other members of this class may also be practical and benecial. These treatments are generally
benecial (106, 107). Memantine, which has been ap- delivered daily or weekly. Beyond these considerations, the
proved for use in severe dementia, may provide modest choice of therapy is generally based on the patients char-
benets and has few adverse effects (108). If the benet of a acteristics and preference, availability of the therapy, and
medication is unclear, a brief medication-free trial may be cost. For instance, some approaches are available only in
used to assess whether continued treatment is worthwhile. institutional settings, such as nursing homes or day care
Depression may be less prevalent and more difcult to centers, whereas others can be used at home.
diagnose at this stage but, if present, should be treated Behavioral techniques and interventions are in wide
vigorously. Psychotic symptoms and agitation are often clinical use with patients who have difcult-to-manage
present and should be treated pharmacologically if they behavioral problems. There is some evidence for modest
cause distress to the patient or signicant danger or dis- benets of such therapies, particularly while the inter-
ruption to caregivers or to other residents of long-term- vention is ongoing (112, 115, 116), but additional well-
care facilities. designed clinical trials are needed. There also is some ev-
At this stage, it is important to ensure adequate nursing idence that behavioral interventions can reduce patients
care, including measures to prevent bedsores and contrac- depressive symptoms (117, 118).
tures. The treatment team should help the family prepare Stimulation-oriented treatments (e.g., recreational ac-
for the patients death. Ideally, discussions about feeding tivities or therapies, art therapies, exercise) are often in-
tube placement, treatment of infection, cardiopulmonary cluded in the care of patients with dementia as well. They
resuscitation, and intubation will have taken place when provide the kind of environmental stimulation that is rec-
the patient could participate, but if they have not, it is im- ognized as part of humane care, and modest efcacy data
portant to raise these issues with the family before a deci- exist that support their use for improving mood and re-
sion about one of these options is urgently required. ducing behavioral disturbances (117, 119121).
Hospice care is an underused resource for patients with Emotion-oriented treatments (e.g., reminiscence ther-
end-stage dementia (109, 110). Hospice provides physical apy, validation therapy, supportive psychotherapy, sensory
support for the patient (with an emphasis on attentive integration, simulated presence therapy) are often used in
nursing care and relief of discomfort rather than medical the treatment of patients with dementia to address issues
intervention) and emotional support for the family during of loss and to improve mood and behavior. Although there
the last months of life. A physician must certify that the is modest research support for the effectiveness of remi-
patient meets hospice criteria for admission for hospice niscence therapy for improvement of mood and behavior
benets to be available (111). (122124), none of these modalities has been subjected to
rigorous scientic testing. Cognition-oriented treatments
4. Implementation of Psychosocial Treatments (e.g., reality orientation, cognitive retraining, skills train-
The psychiatric care of patients with dementia involves a ing) may provide mild short-term improvements in se-
broad range of general psychosocial interventions for the lected domains of cognition, but such improvements,
patient and his or her family, as introduced in Section II.B. when achieved, are not lasting (125, 126).
Short-term adverse emotional consequences have some- cological approaches should be attempted rst to avoid
times been reported with psychosocial treatments. This is the very signicant morbidities associated with psycho-
especially true of the cognitively oriented treatments, tropic medication use in elderly patients. Nonetheless,
during which frustration, catastrophic reactions, agita- many elderly individuals with dementia manifest neuro-
tion, and depression have been reported (86, 127). Thus, psychiatric symptoms that do not respond to psychosocial
treatment regimens must be tailored to the cognitive abil- or environmental interventions but may respond to psy-
ities and frustration tolerance of each patient. chotropic medications individually or in combination.
The sections that follow describe somatic therapies
5. Implementation of Pharmacological Treatments used to treat the cognitive symptoms and functional losses
The following summarizes principles that underlie the associated with dementia, as well as the prevalent neuro-
pharmacological treatment of elderly patients and those psychiatric symptoms of psychosis, anxiety, agitation, de-
with dementia (128). First, elderly individuals have depression, apathy, and sleep disturbances. Although the
creased renal clearance and slowed hepatic metabolism, sections are organized by these specic target symptoms,
which alter the pharmacokinetics of many medications. many medications have broader impact in actual practice.
Moreover, because elderly individuals may have multiple
coexisting medical conditions and therefore may take a. Treatments for Cognitive and Functional Losses
multiple medications, it is important to consider how Because there is no cure for most cases of dementia, the
these general medical conditions and associated medica- primary goal of medication treatment for cognitive symp-
tions may interact to further alter the absorption, serum toms in dementia is to delay the progression of symptoms,
protein binding, metabolism, and excretion of the medi- with the hope that this delay will translate into a preser-
cation (129). Therefore, low starting doses, small dose in- vation of functional ability, maintaining the patient for as
creases, and long intervals between dose increases are long as possible at a particular level of symptom severity.
necessary. This is true even in the inpatient setting, where However, no medication treatment has been shown to de-
utilization review pressures may encourage physicians to lay the progression of neurodegeneration.
employ rapid titration schedules. However, some patients A number of psychoactive medications are used to
may ultimately need doses as high as would be appropriate achieve these goals. The only FDA-approved medica-
for younger patients. tions for dementia or cognitive impairment are the cho-
Pharmacodynamics may also be altered in elderly pa- linesterase inhibitors (tacrine, donepezil, rivastigmine,
tients and those with dementia. As a result, certain medi- and galantamine), memantine, and the combination of
cation side effects pose particular problems for elderly ergoloid mesylates (approved for nonspecic cognitive
patients and those with dementia; medications with these decline). In addition, other drugs, including vitamin E,
side effects must therefore be used judiciously. Anticholin- ginkgo biloba, and selegiline (approved by the FDA for
ergic side effects may be more burdensome for elderly pa- treatment of Parkinsons disease and in patch form for the
tients owing to coexisting cardiovascular disease, prostate treatment of depression), are occasionally used for this
or bladder disease, or other general medical conditions. purpose in selected patients, although they are not gen-
These medications may also lead to worsening cognitive erally recommended, because their efcacy and safety are
impairment, confusion, or even delirium (130). Orthosta- uncertain.
sis is common in elderly patients because of decreased vas- Several other medications that had been proposed for
cular tone and medication side effects. As a result, elderly the treatment or prevention of cognitive decline, includ-
patients, especially those with dementia, are more prone to ing NSAIDs, statin medications, and estrogen supple-
falls and associated injuries. Medications associated with mentation (with conjugated equine estrogens), have
central nervous system sedation may worsen cognition, in- shown a lack of efcacy and safety in placebo-controlled
crease the risk of falls, and put patients with sleep apnea at trials in patients with Alzheimers disease and therefore
risk for additional respiratory depression. Finally, elderly are not recommended. Many additional agents are cur-
patients, especially those with Alzheimers disease, Parkin- rently being tested. Participation in clinical trials is an-
sons disease, or dementia with Lewy bodies, are especially other option available to patients with dementia.
susceptible to extrapyramidal side effects. Certain interventions for specic medical conditions
For all these reasons, medications should be used with such as the use of antihypertensive medications to control
considerable care, and polypharmacy should be avoided blood pressure, use of aspirin to prevent further strokes,
whenever possible. In nonemergency situations or when and prescription of levodopa as a general treatment of
neuropsychiatric symptoms are not severe, nonpharma- Parkinsons disease may also lead to positive effects on
cognition but are beyond the purview of this practice ies have signicant methodological problems and none
guideline. resolves the question of superiority (164). There are also
no data on whether or how to switch from one cholines-
1. Cholinesterase inhibitors terase inhibitor to another.
As would be expected with cholinesterase inhibitors,
a. Alzheimers disease and general considerations common side effects in clinical trials are associated with
In 1993 tacrine became the rst agent approved specically cholinergic excess, particularly nausea and vomiting, but
for the treatment of cognitive symptoms in Alzheimers dis- these symptoms tend to be mild to moderate in severity
ease. Tacrine is a reversible cholinesterase inhibitor with for all agents. In the randomized clinical trials noted ear-
evidence for efcacy from multiple double-blind placebo- lier, these side effects were observed in approximately
controlled trials (131135) that is thought to work by in- 10%20% of patients (136159). Additional cholinergic
creasing the availability of intrasynaptic acetylcholine in side effects include muscle cramps; bradycardia, which
the brains of patients with Alzheimers disease. The FDA can be dangerous in individuals with cardiac conduction
approved other cholinesterase inhibitorsdonepezil, ri- problems; decreased appetite and weight; and increased
vastigmine, and galantaminein 1997, 2000, and 2001, gastrointestinal acid, a particular concern in those with a
respectively, for treatment of cognitive decline in mild to history of ulcers. These side effects occur infrequently
moderate Alzheimers disease. These agents are now pre- with these agents, but bradycardia should be considered a
ferred over tacrine because of tacrines reversible hepatic relative contraindication to their use. In general, cholin-
toxicity and the requirement that it be given 4 times per ergic side effects tend to wane within 24 days, so if pa-
day. Evidence for the efcacy of these medications in mild to tients can tolerate unpleasant effects in the early days of
moderate Alzheimers disease also comes from a substantial treatment, they may be more comfortable later on. Fi-
number of randomized, double-blind, placebo-controlled nally, cholinesterase inhibitors may induce or exacerbate
trials of donepezil (136146), rivastigmine (147152), and urinary obstruction, worsen asthma and chronic obstruc-
galantamine (153159). Results of a smaller number of clin- tive pulmonary disease, cause seizures, induce or worsen
ical trials (106, 107) suggested that cholinesterase inhibi- sleep disturbance, and exaggerate the effects of some mus-
tors might have some limited benets in severe cle relaxants during anesthesia.
Alzheimers disease. In 2006, donepezil was approved by Reversible, direct medication-induced hepatotoxicity
the FDA for this indication. with hepatocellular injury is a unique property of tacrine,
Given the evidence from randomized controlled trials occurring in approximately 30% of those taking it 68
for modest improvement in some patients treated with weeks after initiating the medication (165). Because of this
cholinesterase inhibitors and the lack of established alter- hepatotoxicity, tacrine is very uncommonly used. Hepato-
natives, it is appropriate to offer a trial of one of these toxicity has not been associated with donepezil, rivastig-
agents for patients with mild or moderate Alzheimers dis- mine, or galantamine.
ease for whom the medication is not contraindicated. The main contraindication to use of cholinesterase in-
Many clinicians in fact prescribe cholinesterase inhibitors hibitors is hypersensitivity to the individual drugs. Some
for patients with the entire range of Mini-Mental State considerations in limiting treatment include the existence
Examination (MMSE) scores, with moderate medical or of gastrointestinal disorders such as gastritis, ulcerative dis-
psychiatric comorbidity, or with possible Alzheimers disease, or undiagnosed nausea and vomiting, because cholin-
ease, even though these patients would not have been el- esterase inhibitors will increase gastric acid secretions.
igible for most clinical trials completed to date. Whenever Cholinesterase inhibitors should also be used with care in
cholinesterase inhibitors are prescribed, patients and their patients with sick sinus syndrome or conduction defects,
families should be apprised of the limited potential bene- cerebrovascular disease, or seizures, as well as in patients
ts as well as the potential costs. with asthma or chronic obstructive pulmonary disease.
Results of the numerous large placebo-controlled tri- With respect to dosing and dosage, donepezil is given
als of individual cholinesterase inhibitors have suggested once per day, usually starting at 5 mg/day. This dosage can
similar degrees of efcacy, although tolerability may dif- be increased to 10 mg/day, if tolerated. Some clinicians
fer among the medications. Nonetheless, currently avail- start treatment with 2.5 mg/day for patients who are frail
able data do not allow a fair, unbiased direct comparison or very sensitive to medication side effects and increase
among the cholinesterase inhibitors. Four clinical trials the dose by 2.5-mg increments. Galantamine is started at
have compared cholinesterase inhibitors (two compared 8 mg/day in divided doses and increased gradually to a tar-
donepezil and galantamine, and two compared donepezil get range of 1624 mg/day in divided doses, although cer-
and rivastigmine) (160163), but a number of these stud- tain patients may benet from dosages up to 32 mg/day. A
once-daily formulation of galantamine has recently been cognition back to the level achieved before medication
released. Rivastigmine is started at 3 mg/day in divided discontinuation (166).
doses and increased gradually to a target range of 612
mg/day in divided doses. Doses may be titrated upward b. Vascular dementia and mixed dementia (Alzheimers disease
every 4 weeks. Slower titration can be helpful in managing and vascular dementia)
Trials of cholinesterase inhibitors in patients with vascular
side effects, if these occur. Higher dosages may be effec-
dementia and mixed dementia have produced inconclu-
tive in some patients when lower dosages are not; there-
sive results. In addition, serious concerns about safety and
fore, patients who have not shown clear benet while
potential increases in mortality have arisen with the use of
taking a lower dosage should receive an increased dose, if
these medications in this patient population (167). As a re-
tolerated, before the conclusion is made that the medica-
sult of these factors, as well as the lack of FDA approval
tion is ineffective. Minimal effective dosages are 5 mg/day
for this indication (see Sections III.B.4 and V.B.1.a.2), no
for donepezil, 16 mg/day for galantamine, and 6 mg/day
specic recommendation can be made in favor of the rou-
for rivastigmine.
tine use of cholinesterase inhibitors in patients with vas-
It is uncertain how long patients should be treated with
cular dementia at this time, although individual patients
cholinesterase inhibitors. Data from placebo-controlled
may benet from their use.
clinical trials have demonstrated benets over placebo for
6 months to 2 years with donepezil (136, 137, 139), for up
c. Dementia with Lewy bodies
to 1 year with rivastigmine (150), and for up to 6 months Cholinesterase inhibitors could be considered for pa-
with galantamine (156). A number of open-label exten- tients with dementia with Lewy bodies. Dosing and titra-
sion clinical trials have been conducted examining the ef- tion are similar to those for patients with Alzheimers
cacy of these agents beyond the time in which placebo disease (168, 169).
controls were actually used. Subjects who continued to
take the study drug were compared to a historical con- d. Dementia of Parkinsons disease
trol group, namely a projection of the decline of a placebo Cholinesterase inhibitors should be considered for pa-
control group. The authors of these studies claimed to tients with mild to moderate dementia associated with
demonstrate ongoing efcacy beyond the conclusion of Parkinsons disease. Only rivastigmine has been studied
the actual placebo-controlled trials, but comparisons us- in a randomized, double-blind, placebo-controlled trial
ing projected outcomes of a placebo group are method- (170) with an open-label extension (171) and approved by
ologically problematic and do not establish efcacy. the FDA for this indication. Nevertheless, there is no rea-
In practice, the decision whether to continue treatment son to believe the benet is specic to this cholinesterase
with cholinesterase inhibitors is a highly individualized inhibitor. Dosing and titration are similar to those for pa-
one. Reasons that patients choose to stop taking these tients with Alzheimers disease.
medications include side effects, adverse events, lack of
motivation, lack of perceived efcacy, and cost. Individual e. Mild cognitive impairment
patients may be observed to have some stabilization of The term mild cognitive impairment describes a heter-
symptoms or slowing of their decline. Under these cir- ogeneous group of individuals, with some patients in the
cumstances, a physician might consider continuing the earliest stages of Alzheimers disease and others suffering
medication. Conversely, a patient who is declining rapidly from other conditions. There are no FDA-approved
despite taking cholinesterase inhibitors may be consid- medications for the treatment of mild cognitive impair-
ered a medication nonresponder, and the medication can ment at this time. Clinical trials of cholinesterase inhibi-
be discontinued. Discontinuation of cholinesterase inhib- tors for mild cognitive impairment have enrolled a
itor medication during placebo-controlled trials after 12 narrower and better dened population of patients with
24 weeks has been associated with a regression of cogni- mild cognitive impairment than most clinicians actually
tive improvement to the level of the associated placebo treat in practice, but even with these well-dened pa-
group. Whether resumption of the cholinesterase inhibi- tients the evidence from clinical trials supporting use of
tor reverses this symptomatic worsening is unclear. Some cholinesterase inhibitors is weak (172, 173). Given the in-
patients have shown pronounced deterioration within conclusive data, the potential safety concerns that exist
several weeks of discontinuing cholinesterase inhibitors with this class of medications in this patient population,
and improvement when the medication has been re- and the lack of FDA approval for this indication (re-
started. In contrast, the results of one study suggested that viewed in Sections V.B.1.a.4 and II.C.5.a.1.a), no specic
donepezil-treated patients who had treatment interrupted recommendation can be made in favor of routine use of
for 6 weeks and then restarted treatment never regained cholinesterase inhibitors in patients with mild cognitive
impairment at this time. Nonetheless, individual patients a large randomized trial of cancer and heart disease preven-
may benet from their use. tion in individuals with diabetes mellitus and/or vascular
disease (182), make the case for its use much less compel-
2. Memantine ling. The evidence from the one placebo-controlled, dou-
Memantine is a noncompetitive NMDA receptor antago- ble-blind, multicenter trial of vitamin E for the treatment
nist approved by the FDA for the treatment of moderate of moderate Alzheimers disease is limited (183). Further-
to severe Alzheimers disease. more, vitamin E failed to show efcacy in one study of in-
Given the evidence for its efcacy in randomized con- dividuals with mild cognitive impairment (173). In this
trolled trials (174, 175), memantine should be considered trial nearly one-half of the subjects later received a diag-
for treatment of patients with moderate to severe Alzhei- nosis of Alzheimers disease during the 3 years of observa-
mers disease. Memantine can be prescribed for people tion and hence had early Alzheimers disease at the
either currently taking or not taking a cholinesterase in- beginning of the trial. Nevertheless, after considering the
hibitor. There is modest evidence that the combination of potential risks and benets of vitamin E, some physicians
memantine and donepezil is better than donepezil alone and their patients may elect to use it, particularly at doses
(175), but there is no evidence that this combination is at or below 400 IU daily. Because vitamin E has been as-
better than memantine alone. There are not yet data to sociated with worsening of coagulation defects in patients
argue for or against the use of memantine beyond 6 with vitamin K deciency (184), it should be avoided in
months (108, 176). this population.
In patients with mild Alzheimers disease, the evidence
is suggestive of a small clinical benet of memantine over 4. Other agents
placebo (108, 177), although this result is not conclusive A number of medications marketed for other indications
and additional trials should be performed. Given that have been proposed for the treatment of dementia on the
there are few safety concerns with the use of memantine in basis of epidemiological data or pilot studies (185189),
mild Alzheimers disease, clinicians may consider using it but they are not recommended for routine use at this time
for individual patients. because of lack of efcacy in subsequent studies (190200)
For vascular dementia, the evidence does not support and potential for adverse effects. These other agents in-
the use of memantine (178, 179), although further trials clude aspirin and other NSAIDs, hormone replacement
are necessary. therapy, the hormone melatonin, the botanical agent
Reported adverse events with memantine are infre- ginkgo biloba, the chelating agent desferrioxamine, the
quent, appear to be mild, and include confusion, dizzi- irreversible monoamine oxidase B (MAO-B) selective in-
ness, headache, sedation, agitation, falls, and constipation hibitor selegiline, and a mixture of ergoloid mesylates cur-
(174, 175, 177). Dropout rates during clinical trials have rently marketed under the trade name Hydergine.
generally been the same for memantine as for placebo. Because some of these agents are popular, psychiatrists
Memantine treatment begins at 5 mg once daily, and this should routinely inquire about their use and should advise
dosage is increased by 5 mg/day every week until a target patients and their families that some of these agents are
dosage of 10 mg b.i.d. is reached. A therapeutic dosage marketed with limited quality control and have not been
range for memantine has not been conclusively established. subjected to adequate efcacy evaluations.
One study demonstrated efcacy at a dosage of 10 mg/day
(180), and the effects of dosages above 20 mg/day have not b. Treatments for Psychosis and Agitation
been studied. Because memantine is cleared primarily by As discussed in Section II.B.3, psychosis and agitation oc-
the kidneys, lower dosages (e.g., 10 mg/day) should be con- cur commonly in patients with dementia and are impor-
sidered in patients with compromised renal function. tant targets of psychiatric intervention. In DSM-IV-TR
Alzheimers disease and other dementias with delusions
3. Vitamin E and hallucinations and Alzheimers disease with behav-
Vitamin E is no longer recommended for the treatment of ioral disturbances are classied separately, and provisional
cognitive symptoms of dementia. Previous recommenda- criteria for psychosis of Alzheimers disease have been
tions for its use had balanced the weakness of the evidence published (201). In clinical practice, however, these symp-
for its efcacy with the perceived lack of risk with use of toms frequently co-occur.
vitamin E. However, new safety concerns, namely the un- Treatments that decrease psychotic symptoms (delu-
expected ndings of increased dose-dependent mortality sions and hallucinations) and associated or independent
in a meta-analysis of vitamin E clinical trials (181) and an behavioral disturbances such as aggression, combative-
increased rate of heart failure with vitamin E treatment in ness, and agitation are often essential to increasing the
comfort and safety of patients and easing the burden of the continued use of any intervention for behavioral dis-
provision of care by families and other caregivers. turbances or psychosis must be evaluated and justied on
Clinicians facing the challenge of treating patients with an ongoing basis. In the nursing home setting, this clinical
signicant psychosis or behavioral disturbances must recommendation is also a requirement under regulations
weigh the risk of not treating these complications of de- of the Federal Nursing Home Reform Act of the Omni-
mentia against the risks of active treatment described be- bus Budget Reconciliation Act of 1987 (see Section
low in Sections II.C.5.b.1, II.C.5.b.2, II.C.5.b.3, and III.C.3). In addition, periodic reevaluation and revision of
II.C.5.b.4. This weighing of risks also includes consider- the treatment plan, including a change in dose, a change
ation of the evidence supporting the efcacy of the agent in medication, or medication discontinuation, may be in-
in question, the patients overall medical condition, and dicated. Patients whose symptom severity was relatively
the evidence of risk and benet of any potential treatment low at the time of medication initiation may be more
alternatives, followed by documentation of the reasons for easily withdrawn from psychotropic medications than
using the medication and the fact that a discussion has those with more severe symptoms at the time of treat-
taken place with the patient or caregiver. ment initiation (202).
As outlined in Section II.C.4, there are a number of
nonpharmacological interventions that can be used before 1. Antipsychotics
a trial of an antipsychotic or other medication is begun. Antipsychotics are the primary pharmacological treat-
Consideration and use of behavioral, psychosocial, and ment available for psychotic symptoms in dementia. They
psychotherapeutic treatments is particularly critical, given are also the most commonly used and best-studied phar-
the large number and potential severity of side effects as- macological treatment for agitation. There is consider-
sociated with pharmacotherapy. Interventions for psycho- able evidence from randomized, double-blind, placebo-
sis should be guided by the patients level of distress and controlled trials and meta-analyses for the efcacy of both
the risk to the patient, caregivers, or other patients. If psy- rst-generation (203217) and second-generation agents
chotic symptoms cause minimal distress to the patient and (201, 212, 218227), although this benet is often modest.
are unaccompanied by agitation or combativeness, they Findings from the Clinical Antipsychotic Trials of Inter-
are best treated with environmental measures, including vention Effectiveness (CATIE-AD) study, funded by the
reassurance and redirection. If the symptoms do cause sig- National Institute of Mental Health (NIMH), failed to
nicant distress or are associated with behavior that may demonstrate conclusive benets of second-generation an-
place the patient or others at risk, treatment with low doses tipsychotics over placebo in patients with Alzheimers dis-
of antipsychotic medication is indicated in addition to ease and psychosis or aggression, although there were
nonpharmacological interventions. Treatment with an an- advantages to the medications on certain outcome vari-
tipsychotic medication is also indicated if a patient is agi- ables and the discontinuation rate due to lack of efcacy
tated or combative in the absence of psychosis, as this was lower with olanzapine and risperidone than it was for
indication for antipsychotic use has signicant support in placebo or quetiapine (228).
the literature. The use of these agents should be reevalu- Given the side effects and potential toxicity of antipsy-
ated and their benet documented on an ongoing basis. chotic agents (225, 228), the risks and benets of these
When antipsychotics are ineffective, carbamazepine, val- medications must be reassessed on an ongoing basis. The
proate, or an SSRI may be used in a careful therapeutic lowest effective dose should be sought, and emergent side
trial. If behavioral symptoms are limited to specic times effects should rst be treated by dose reduction. Because
or settings (e.g., a diagnostic study), or if other approaches of the risks involved with the use of antipsychotics, indi-
fail, a low-dose benzodiazepine may prove useful, al- cations for their use should be generally limited to psy-
though side effects in elderly patients can be problematic chosis or behavioral disturbances, and they should not be
(see Section II.C.5.b.2). Although mood stabilizers and used primarily for sleep disorders or anxiety. In addition,
SSRIs are commonly used in clinical practice to treat agi- periodic attempts (e.g., every several months) to reduce or
tation, delusions, and aggression, they have not been con- withdraw antipsychotic medications should be considered
sistently shown to be effective in treating these symptoms, for all patients, while weighing the probability of a relapse
nor is there substantial evidence for their safety. Thus, in and the dangerousness of the target behavior(s) (229). In
making decisions about treatment, these agents should not general, agents with signicant anticholinergic properties
be seen as having improved safety or comparable efcacy, should be avoided in patients with dementia, although
compared to antipsychotic medications. they may be considered under specic circumstances.
As a dementing illness evolves, psychosis and agitation Mild to moderate adverse effects of antipsychotics in-
may wax and wane or may change in character. As a result, clude akathisia, parkinsonism, sedation, peripheral and
central anticholinergic effects, delirium, postural hy- maxima, younger and less frail individuals may tolerate and
potension, cardiac conduction defects, urinary tract infec- respond to somewhat higher doses, and very severely agi-
tions, urinary incontinence, and falls. Antipsychotic tated patients may also need higher dosages. In contrast,
agents are also associated with a risk of more serious com- antipsychotic agents must be used with extreme caution in
plications that must be considered in weighing the risks patients with dementia with Lewy bodies or Parkinsons
and benets of antipsychotic treatment (see Section disease, who can be exquisitely sensitive to the extrapyra-
V.B.2.a.2 for additional details). Serious complications in- midal effects of these agents (232).
clude tardive dyskinesia (the incidence of which increases There are few relative efcacy data to guide the choice
with dose and duration of treatment and which occurs among second-generation antipsychotic agents. The
more commonly in women, in individuals with dementia CATIE-AD trial did not nd signicant differences in ef-
or brain injury, and in elderly patients in general), neuro- cacy or tolerability among olanzapine, quetiapine, and
leptic malignant syndrome (a rare but potentially lethal risperidone, although the time to discontinuation due to
adverse effect of antipsychotic medications that occurs lack of efcacy was longer for olanzapine and risperidone
less frequently with second-generation antipsychotic than for quetiapine (228). Instead, the choice is based
agents), agranulocytosis (with clozapine), hyperlipidemia, most often on the side effect prole. As the overall side-
weight gain, diabetes mellitus, cerebrovascular accidents, effect burden appears to be lower with second-generation
and death. An increased risk of cerebrovascular accidents agents, drugs in this class are usually selected rst. Wide-
has recently been found with the second-generation anti- spread clinical practice is to select the agent whose most
psychotics aripiprazole, olanzapine, and risperidone, al- common side effects are least likely to cause problems for
though not with quetiapine. Meta-analyses of clinical a given patient. For instance, clozapine might be avoided
trials of the second-generation antipsychotics aripipra- if the patient is likely to be sensitive to anticholinergic ef-
zole, olanzapine, quetiapine, and risperidone (225), as fects, or an agent lacking signicant motor side effects
well as of rst-generation antipsychotics (230), have such as aripiprazole, clozapine, or quetiapine might be
found an increased mortality when used in elderly patients chosen if the patient has Parkinsons disease, dementia
with dementia. These concerns have led to black box with Lewy bodies, or other sensitivity to extrapyramidal
warnings on the second-generation antipsychotics (231). side effects. Aripiprazole and quetiapine may be better
Accepted clinical practice is to prescribe antipsychotic rst choices because their overall side effect prole is
agents at standing doses rather than as needed, although as- more benign than that of clozapine (233237).
needed doses may be appropriate for symptoms that occur The side effects of some medications might actually be
infrequently. Oral administration is generally preferred, al- benecial for certain patients. For example, a more sedat-
though an intramuscular injection may sometimes be used ing medication could be given at bedtime for a patient
in an emergency or when a patient is unable to take medi- who has difculty falling asleep in addition to agitation or
cations by mouth (e.g., for a surgical procedure). Low start- psychosis. Antipsychotics are most commonly adminis-
ing dosages are recommended, e.g., 0.250.5 mg/day of tered in the evening, so that maximum blood levels occur
haloperidol, 0.251.0 mg/day of risperidone, 12.5 mg/day when they will help foster sleep and treat behavioral prob-
of clozapine, 1.255.0 mg/day of olanzapine, 12.550 lems that peak in the evening hours (sometimes called
mg/day of quetiapine. The best starting dosages for aripip- sundowning). Most of these medications have long half-
razole and ziprasidone are not known, although the avail- lives, and once-a-day dosing is generally sufcient. The
able evidence suggests that 5 mg/day of aripiprazole may be one exception may be quetiapine, which is usually admin-
safe for most patients. The dose can be increased on the ba- istered twice daily. However, morning doses or twice-a-day
sis of the response of the target symptom(s). The usual doses of the other agents may be helpful for patients with
maximum dosages of these agents for patients with demen- different symptom patterns.
tia are 2 mg/day of haloperidol, 1.52 mg/day of risperi- The availability of a specic formulation of an antipsy-
done, 75100 mg/day of clozapine, 200300 mg/day of chotic may also contribute to the choice of a particular
quetiapine, 10 mg/day of olanzapine, and 15 mg/day of ari- agent. Some antipsychotics are available in liquid form
piprazole. In addition, risperidone causes fewer extrapyra- (e.g., aripiprazole, risperidone, ziprasidone, uphena-
midal symptoms when used at dosages of 1 mg/day than zine, haloperidol), and some (e.g., clozapine, olanzapine,
when used at higher doses (218). Clinicians should keep in risperidone, aripiprazole) are available as rapidly dissolv-
mind that these medications take time to work and that in- ing wafers. Olanzapine, ziprasidone, aripiprazole, uphena-
creasing doses too rapidly may lead to the development of zine, and haloperidol are available in a rapid-onset
side effects rather than more rapid efcacy. Although most injectable form, whereas risperidone, haloperidol, and
patients with dementia do best with dosages below these uphenazine are available in long-acting injectable forms.
With the exception of olanzapine (223), these formula- of action, is responsible for the increased fall risk (247).
tions have not been studied in patients with dementia. Clinical experience suggests that like alcohol, benzodiaz-
epines may lead to disinhibition, although there are few
2. Benzodiazepines data to support this association. The risk of benzodiaze-
Benzodiazepines may have a higher likelihood of side ef- pine dependence is also a concern. If benzodiazepines are
fects and a lower likelihood of benet than antipsychotics prescribed for an extended period (e.g., 1 month), they
(223, 238243); nonetheless, they are occasionally useful in should be tapered rather than stopped abruptly because of
treating agitation in certain patients with dementia, partic- the risk of withdrawal.
ularly those in whom anxiety is prominent. Their long-
term use is generally to be avoided, but they may be partic- 3. Anticonvulsants
ularly useful on an occasional as-needed basis for patients There is some evidence to suggest that carbamazepine
who have only rare episodes of agitation or those who need may have modest benet for agitation when used in low
to be sedated for a particular procedure, such as a tooth ex- doses in patients with dementia (248252). However,
traction or a diagnostic study. Given the risk of disinhibi- given the relatively small body of clinical trials evidence,
tion and consequent worsening of target behaviors, the high risk of drug-drug interactions, and the known
oversedation, falls, and delirium, their use should be kept to tolerability problems expected with long-term use, carba-
a minimum, with a maximum of 13 mg of lorazepam (or mazepine is not recommended for the routine treatment
equivalent doses of other benzodiazepines) in 24 hours. of agitation in patients with dementia.
Among the benzodiazepines, many clinicians favor Routine use of valproate to treat behavioral symptoms
agents such as oxazepam and lorazepam that do not re- in dementia is not recommended based on the current ev-
quire oxidative metabolism in the liver and have no active idence. Most (253255), but not all (256), randomized
metabolites. Temazepam shares these characteristics but placebo-controlled trials showed no benet of valproate,
is more problematic because of its long half-life. Oral compared with placebo. In addition, a 2004 Cochrane re-
lorazepam (or intramuscular in the event of an emer- view (257) concluded that the various formulations of val-
gency) may be given on an as-needed basis in doses from proate had not yet been shown to be effective.
0.5 to 1.0 mg every 46 hours. Standing oral doses of 0.5 Nonetheless, a therapeutic trial of carbamazepine or
1.0 mg may be given from 1 to 4 times per day. Oxazepam valproate may be considered in individual cases (258), for
is absorbed more slowly, so it is less useful on an as-needed example, in patients who are sensitive or unresponsive to
basis. Standing doses of 7.515.0 mg may be given 1 to 4 antipsychotics, who have signicant vascular risk factors,
times per day. Some clinicians prefer long-acting agents, or who do not have psychosis but are mildly agitated.
such as clonazepam (starting at 0.5 mg/day with increases Given the potential toxicity of both of these anticonvul-
up to 2 mg/day) (244). However, such agents must be used sant agents, it is important to identify and monitor target
with caution as described in the next paragraph. symptoms and to discontinue the medication if no im-
The most commonly reported side effects with benzo- provement is observed.
diazepines are sedation, ataxia, amnesia, confusion (even If used, carbamazepine may be given in two to four
delirium), and possibly paradoxical anxiety. These can doses per day, started at a total dosage of 50100 mg/day,
lead to worsening cognition and behavior and increase the and increased gradually as warranted by behavioral re-
risk of falls (245). Benzodiazepines also carry a risk of res- sponse and side effects or until blood levels reach 812
piratory suppression in patients with sleep-related breath- ng/ml. Divalproex sodium may be given in two or three
ing disorders. Because all of these effects are dose related, doses per day and should be started at 125250 mg/day,
the minimum effective dose should be used. Agents with with gradual increases based on behavioral response and
long half-lives (e.g., clonazepam) and long-lived metabo- side effects or until blood levels reach 5060 ng/ml (or,
lites (e.g., diazepam, chlordiazepoxide, clorazepate, u- rarely, 100 ng/ml).
razepam) can take weeks to reach steady-state levels, The principal side effects of carbamazepine include
especially in elderly patients, so they generally are not ataxia, falls, sedation, and confusion, all of which are of par-
used in this patient population. Under unusual circum- ticular concern for elderly patients and those with demen-
stances when they have to be used, it must be with partic- tia. Carbamazepine can cause drug interactions through its
ular caution, with very low starting doses and very gradual effect on the cytochrome P450 system. In rare instances,
dosage increases. Elderly patients taking long-acting ben- carbamazepine can lead to bone marrow suppression or hy-
zodiazepines are more likely to fall, and to suffer hip frac- ponatremia through the syndrome of inappropriate anti-
tures, than those taking short-acting agents (246), diuretic hormone secretion. Valproates principal side
although it is possible that the total dose, not the duration effects are sedation, gastrointestinal disturbances, confu-
sion, ataxia, and falls. Bone marrow suppression, hepatic itated patients with mental retardation, but support for it
toxicity, thrombocytopenia, and hyperammonemia can oc- is quite limited, and side effects and toxicity are com-
cur. Many clinicians monitor the CBC and electrolyte lev- mon, including delirium (210). Therefore, routine use of
els in patients taking carbamazepine and monitor the CBC lithium to treat agitation in patients with dementia is not
and liver function values in patients taking valproate, owing recommended.
to the possibility of bone marrow suppression, hyponatre- Beta-blockers, notably propranolol, metoprolol, and
mia, and liver toxicity. However, these practices are not fol- pindolol, have also been reported to be helpful for some
lowed by all clinicians. A particularly cautious approach is agitated patients with dementia (276). However, most of
warranted when treating elderly patients and those with de- the patients included in the case reports had somewhat
mentia, who may be more vulnerable to adverse effects, atypical clinical features, raising questions about the gen-
particularly central nervous system effects, and yet less eralizability of these reports. In addition, large dosages
likely to be able to report warning symptoms. (e.g., 200300 mg/day of propranolol) were used, and
For additional details concerning the assessment and such dosages create a considerable risk of bradycardia, hy-
monitoring necessary during use of these agents, along potension, and delirium for elderly patients. One small
with their side effects and potential toxicities, the reader is randomized, double-blind, placebo-controlled trial of
referred to APAs Practice Guideline for the Treatment of Pa- propranolol in patients with Alzheimers disease and be-
tients With Bipolar Disorder, 2nd edition (259). havioral disturbance did show benet over placebo for
certain symptoms although it was noted that beta-blocker
4. Other agents use was contraindicated for many subjects who would oth-
Support for the use of trazodone or buspirone is limited to erwise have been eligible for the study (277). Therefore,
data from case series and small clinical trials (214, 260 routine use of beta-blockers to treat agitation in patients
269). Therefore, neither agent can be recommended for with dementia is not recommended.
the routine treatment of agitation and psychosis in pa-
tients with dementia. Although the evidence suggesting c. Treatments for Depression and Related Symptoms
efcacy of SSRIs for agitation is somewhat stronger (262, Recognition and treatment of depression is crucial in indi-
270, 271), further study is needed before they can be rec- viduals with dementia, because the presence of depression
ommended for routine use. Nonetheless, a therapeutic has been associated with higher rates of disability, impaired
trial of trazodone, buspirone, or an SSRI may be appro- quality of life, and greater mortality (278). The best ap-
priate for some nonpsychotic but agitated patients, espe- proach to diagnosing depression in the context of demen-
cially those with relatively mild symptoms or those who tia is not yet clear. Provisional criteria for depression of
are intolerant of or unresponsive to antipsychotics. Alzheimers disease have been proposed but not yet vali-
When patients are taking SSRIs, clinicians need to keep dated (279). The Depression and Bipolar Support Alliance
in mind the serotonin syndrome, caused by excessive sero- Consensus Statement Panel reported that the diagnostic
tonergic activity, usually as a result of serotonergic medi- criteria for depression in individuals with dementing dis-
cations being combined (including buspirone and SSRIs). orders must be revised (105). They recommended that the
Symptoms include delirium, autonomic instability, and in- criteria take into account the instability and uctuation of
creased neuromuscular activity, such as myoclonus. symptoms over time, the reduction in positive affect or
When trazodone is used, the principal side effects are pleasure, and the inclusion of irritability, social with-
postural hypotension, sedation, and dry mouth. Priapism drawal, and isolation as indicators of depression. Until cri-
can occur but is uncommon. Trazodone is generally given teria for depression in dementia are established, patients
before bedtime but can be given in two or three divided should be carefully evaluated for any of the symptoms of
doses per day. It can be started at 2550 mg/day and grad- depression outlined in DSM-IV-TR. Even those patients
ually increased to a maximum dosage of 150250 mg/day. with depressive symptoms who do not meet the diagnostic
When male patients display inappropriate sexual be- criteria for major depression should be considered as can-
havior, a particular problem in patients with frontal lobe didates for depression treatment. The presence of neu-
dementias, medroxyprogesterone and related hormonal rovegetative symptoms, suicidal ideation, and mood-
agents are sometimes recommended (272274), a recom- congruent delusions or hallucinations may indicate a need
mendation supported only by case series at present. Be- for more vigorous and aggressive therapies (such as higher
cause SSRIs may reduce libido and are probably safer, medication dosages, multiple medication trials, or ECT).
they may be tried before hormonal agents (275). Depression may worsen cognitive impairment associ-
Lithium carbonate has also been suggested as a treat- ated with dementia. Therefore, one goal of treating de-
ment for agitation because of its occasional utility for ag- pression in dementia is to maximize cognitive functioning.
Sometimes cognitive decits partially or even fully resolve more common with specic SSRIs than with the entire
with successful treatment of the depression. Nonetheless, class. As with most psychotropic medications, SSRI use is
because as many as one-half of such persons do develop associated with an increased risk of falls in elderly patients
dementia within 5 years (280, 281), caution is urged in rul- (300). Physicians prescribing SSRIs should also be aware
ing out an underlying early dementia in patients with both of the many possible medication interactions associated
affective and cognitive symptoms, particularly when the with the metabolism of these agents through the cyto-
rst episode of depression is in old age. Treatment of de- chrome P450 system.
pression may also reduce other neuropsychiatric symp- Alternative agents to SSRIs include but are not lim-
toms associated with depression such as aggression, ited to venlafaxine, mirtazapine, and bupropion. The se-
anxiety, apathy, and psychosis (282, 283). rotonin-norepinephrine reuptake inhibitor venlafaxine
When treatment for depression is being considered, is metabolized through the cytochrome P450 system,
patients should be evaluated for conditions that may be but because it does not induce or inhibit these enzymes,
causing or contributing to the depression. Among these it is less likely to interact with other drugs metabolized
conditions are other psychiatric disorders (e.g., alcohol or through the same system. One side effect more com-
sedative-hypnotic dependence), other neurological prob- monly seen with venlafaxine than other antidepressants is
lems (e.g., stroke, Parkinsons disease), general medical an elevation in blood pressure, which may be less likely
problems (e.g., thyroid disease, cardiac disease, or cancer), with the sustained release formulation. Duloxetine, an-
and the use of certain medications (e.g., corticosteroids, other inhibitor of serotonin and norepinephrine reup-
benzodiazepines). take, is commonly used to treat major depression, but
clinical experience with its use in geriatric patients with
1. Antidepressants dementia is limited, and there are no published clinical
As described in APAs Practice Guideline for the Treatment of trials to support its use. Mirtazapine, a noradrener-
Patients With Major Depressive Disorder, 2nd edition (284), gic/specic serotonergic antidepressant, can produce se-
many well-designed clinical trials support the efcacy of an- dation and weight gain, especially at low doses. Rare but
tidepressants in depressed elderly patients without dementia potentially serious side effects of mirtazapine are liver
(285288). However, these data may not extrapolate to pa- toxicity and neutropenia. Bupropion, a norepinephrine-
tients with co-occurring dementia. Placebo-controlled tri- dopamine reuptake inhibitor, has been associated with a
als of antidepressants in patients with dementia have shown risk of seizures, especially at high doses, in patients with
mixed results (289296). Despite this mixed evidence, clin- anorexia or with structural neurological problems. Tra-
ical consensus supports a trial of an antidepressant to treat zodone, a serotonin-2 antagonist/reuptake inhibitor, has
clinically signicant, persistent depressed mood in patients sedative side effects and can be used when insomnia or se-
with dementia. SSRIs may be preferred because they ap- vere agitation are prominent. At higher doses, signicant
pear to be better tolerated than other antidepressants (297 side effects include postural hypotension and priapism.
299). Some patients with dementia and depression do not Cyclic antidepressants or MAOIs can be used to treat
tolerate the dosages needed to achieve full remission. depression in patients with dementia if other classes of
When a rapid response is not critical, a very gradual dosage agents have failed or are contraindicated. However, the
increase may increase the likelihood that a therapeutic dos- prominent cardiovascular and anticholinergic side effects
age will be reached and tolerated. After prolonged use, associated with these agents make them undesirable rst-
medications should be withdrawn gradually whenever pos- or second-line agents. The most problematic side effects
sible, in order to avoid withdrawal symptoms. are cardiovascular effects, including orthostatic hypoten-
The reader is referred to APAs Practice Guideline for the sion and cardiac conduction delay, and anticholinergic ef-
Treatment of Patients With Major Depressive Disorder, 2nd fects, including blurred vision, tachycardia, dry mouth,
edition (284) for a detailed discussion of the side effects of urinary retention, constipation, sedation, impaired cogni-
antidepressant agents. Side effects, divided by medication tion, and delirium. If a cyclic antidepressant is used,
class, are briey summarized here. agents with signicant anticholinergic properties such as
Compared to cyclic antidepressants and monoamine imipramine and amitriptyline should be avoided. In terms
oxidase inhibitors (MAOIs), SSRIs tend to have a more fa- of MAOI treatment, only the reversible MAOI moclobe-
vorable side-effect prole and generally have fewer anti- mide has been studied for treating depression in patients
cholinergic and cardiovascular side effects. However, with dementia. Although moclobemide is less toxic than
SSRIs can produce nausea and vomiting, agitation and ak- the irreversible MAOIs, it is not currently available in the
athisia, parkinsonian side effects, sexual dysfunction, United States. If nonselective irreversible MAOIs are pre-
weight loss, and hyponatremia. Some of these effects are scribed, the required dietary restrictions necessitate close
monitoring of food intake, because a patient with demen- 3. Electroconvulsive therapy

tia cannot be relied on to adhere to these restrictions. Although the data supporting the efcacy and safety of
As with most other medications, low starting doses, ECT in the treatment of depression in dementia are lim-
small dose increases, and long intervals between dose in- ited to one small retrospective chart review study, there are
creases are generally necessary when implementing anti- signicant data supporting its use in geriatric depression in
depressants for elderly patients. Citalopram is started at patients without dementia (306308). Therefore, in the
510 mg/day and increased at several-week intervals to a presence of dementia, ECT should only be considered for
maximum of 40 mg/day. Sertraline may be started at 12.5 treating depression that is severe, life-threatening, or
25.0 mg/day and increased at 12-week intervals up to a does not respond to other treatments. The most common
maximum dosage of 150200 mg/day. signicant side effect is transient confusion, which in
If these agents are ineffective and other agents are cho- turn increases the risk of falls, dehydration, and other
sen, the starting doses are as follows. Venlafaxine can be complications. Twice weekly rather than thrice weekly and
started at a dosage as low as 25 mg/day (extended release, high-dose unilateral (309) or bifrontal rather than bitem-
37.5 mg/day) and increased at approximately weekly in- poral ECT may decrease the risk of cognitive side effects
tervals up to a maximum dosage of 375 mg/day in divided after ECT. Clinicians should refer to The Practice of Elec-
doses (extended release, 225 mg/day). If venlafaxine is troconvulsive Therapy. Recommendations for Treatment,
prescribed, careful monitoring of blood pressure is indi- Training, and Privileging: A Task Force Report of the American
cated. Mirtazapine can be started at a dosage as low as 7.5 Psychiatric Association (310) for a full discussion of the use of
mg at bedtime and increased by 7.5-mg or 15-mg incre- ECT and other potential side effects of ECT treatment.
ments to 4560 mg at bedtime. Lower dosages have been
associated with sedation and appetite increase, both of d. Treatments for Sleep Disturbance
which may be benecial for depressed patients with in- Sleep problems have been reported in 25%50% of pa-
somnia or anorexia. Less sedation is found in dosages over tients with dementia (311, 312), and provisional criteria
15 mg/day. Caution should be used in prescribing this for sleep disturbances associated with Alzheimers disease
agent for patients with liver dysfunction or renal impair- have been proposed (313). Major causes of sleep distur-
ment and for patients who develop signs of infection. Bu- bances in this population include physiological changes
propion can be started at 37.5 mg once or twice per day associated with aging (fragmented nocturnal sleep, multi-
(sustained release, 100 mg/day) and increased slowly to a ple and prolonged awakenings, relative decrease in slow-
maximum dosage of 300 mg/day in divided doses (sus- wave sleep percentage, and increased daytime napping),
tained release, 300 mg/day). No more than 150 mg of im- pathological involvement of the suprachiasmatic nucleus,
mediate release bupropion should be given within any 4- the effects of co-occurring medical or psychiatric disor-
hour period because of the risk of seizures. Duloxetine can ders or medications, untreated pain, and poor sleep hy-
be started at 2040 mg/day and increased slowly to a max- giene (314, 315). Cholinesterase inhibitors can also cause
imum of 6080 mg/day, typically in divided doses. insomnia (141). Some over-the-counter sleep medications
(e.g., diphenhydramine) can contribute to delirium and
2. Psychostimulants and dopamine agonists paradoxically worsen sleep. Thus, it is important to ask if
There is a small amount of evidence (301, 302) that dopa- the patient is using over-the-counter diphenhydramine or
minergic agents such as psychostimulants (d-ampheta- other over-the-counter or herbal preparations to treat
mine, methylphenidate), amantadine, bromocriptine, and sleep disturbance.
bupropion may be helpful in the treatment of severe apa- Treatment of sleep disturbance in dementia is aimed at
thy in patients with dementia. Psychostimulants have also decreasing the frequency and severity of insomnia, inter-
received some support for the treatment of depression in rupted sleep, and nocturnal confusion in patients with de-
elderly individuals with severe general medical disorders mentia. In addition to addressing the sleep complaints of
(303305). In general, these agents may be associated with people with dementia, treatment goals are to increase pa-
tachyarrhythmias, hypertension, restlessness, agitation, tient comfort, decrease disruption to families and care-
sleep disturbances, psychosis, confusion, dyskinesias, and givers, and decrease nocturnal wandering and nighttime
appetite suppression, particularly at high doses, and accidents.
amantadine may also be associated with signicant anticho- Available data do not support the recommendation of a
linergic effects. Starting dosages of dextroamphetamine specic course of action for treating sleep disturbances in
and methylphenidate are 2.55.0 mg in the morning. The patients with dementia. Although the data are sparse, clin-
starting dose can be increased by 2.5 mg every 2 or 3 days ical practice favors beginning with nonpharmacological
to a maximum of 3040 mg/day. approaches when the sleep disorder is an isolated prob-
lem. There are few studies of behavioral, environmental, indication to the use of benzodiazepines or other agents
or pharmacological interventions to improve sleep in this that suppress respiratory drive.
population, although there is some evidence that training If another behavioral or neuropsychiatric condition is
caregivers in how to implement proper sleep hygiene can present, and medications used to treat that condition have
result in improved sleep for patients with dementia (316, sedative properties, clinical practice favors prescribing
317). A number of trials of bright light therapy have been that agent at bedtime, if appropriate, to assist with treat-
conducted but have failed to demonstrate signicant clin- ment of insomnia. For example, an antidepressant with
ical benet (315, 318322). Nevertheless, the psychiatrist sedative properties (e.g., mirtazapine or trazodone) can be
treating a patient for a sleep disorder can follow a number given at bedtime if both sleep disorder and depression are
of general clinical guidelines in developing a treatment present. If the patient has psychotic symptoms and sleep
plan. In meeting the needs of both the patient and his or disturbance, second-generation antipsychotics may be the
her caregivers, clinicians should consider behavioral and initial treatment of choice. If there are clear decits in the
environmental interventions, combine nonpharmacolog- patients sleep hygiene, then education and behavioral
ical and pharmacological therapies, and seek to avoid use management might be the preferred treatment course.
of multiple psychotropic medications (314). Other initial Pharmacological interventions include a number of
steps may include establishing regular sleep and waking agents. Some clinicians prefer 25100 mg of trazodone at
times, limiting daytime sleeping, avoiding uid intake in bedtime for sleep disturbances, whereas others prefer the
the evening, establishing calming bedtime rituals, and nonbenzodiazepine hypnotics such as zolpidem (510 mg
providing adequate daytime physical and mental activities at bedtime) or zaleplon (510 mg at bedtime). Benzodi-
(323325). Underlying medical and psychiatric condi- azepines (e.g., 0.51.0 mg of lorazepam, 7.515.0 mg of
tions that could disturb sleep should be evaluated and oxazepam) may be used but are generally recommended
treated. Medications that could interfere with sleep only for short-term sleep problems because of the possi-
should be adjusted if possible. If the patient lives in a set- bility of tolerance, daytime sleepiness, rebound insom-
ting that can provide adequate supervision without caus- nia, worsening cognition, falls, disinhibition, and
ing undue disruption to others, allowing the patient to delirium. Rebound insomnia and daytime sleepiness can
sleep in the daytime and be awake at night is an alternative occur with any of these agents (327). Triazolam is not rec-
to pharmacological intervention. Pharmacological treat- ommended for individuals with dementia because of its
ment should be instituted only after other measures have association with amnesia. Diphenhydramine, which is
been unsuccessful and the potential benets outweigh the found in most over-the-counter sleep preparations, is
risk of side effects. It is particularly important to identify used by some clinicians, but it is not recommended for
sleep apnea (326), which may affect 33%70% of patients the treatment of patients with dementia because of its an-
with dementia (324). This condition is a relative contra- ticholinergic properties.
III. SPECIFIC CLINICAL FEATURES INFLUENCING THE

TREATMENT PLAN
A. DEMOGRAPHIC AND SOCIAL FACTORS care for minor children. On the other hand, older patients
may be frail and have multiple other general medical prob-
1. Age lems that create difculties in diagnosis and treatment as
Patients and families with dementia occurring in middle well as greater disability for a given stage of dementia.
age (e.g., frontotemporal dementia or early-onset Alzhei-
mers disease) may have unique and particularly difcult 2. Gender
challenges in coping with the diagnosis and its impact on Another important demographic factor affecting treat-
their lives. Early age of onset may be associated with a ment is gender. There are more women with dementia,
more rapid rate of decline (328). In addition, they may re- partly because of greater longevity, but also because Alz-
quire assistance with problems not generally seen with heimers disease is more prevalent among women for rea-
older patients, such as relinquishing work responsibilities sons that are not known. In addition, because of their
(particularly if their jobs are such that their dementia puts greater life expectancy (and tendency to marry men older
others at risk), obtaining disability benets, and arranging than themselves), women with dementia are more likely
to have an adult child rather than a spouse as caregiver. sidered in all treatment decisions but has a particular
Unlike an elderly spouse caregiver, who is more likely to impact on decisions about long-term care. A referral to
be retired, adult child caregivers (most often daughters or the local chapter of the Alzheimers Association or to a so-
daughters-in-law) are more likely to have jobs outside the cial worker or another individual knowledgeable about lo-
home and/or to be raising children. These additional cal resources, treatment centers, and Medicaid laws can be
caregiver responsibilities may contribute to earlier insti- important in helping families nd local treatment options
tutionalization for elderly women with dementia. that t their needs and budget.
3. Ethnic and Cultural Background B. CO-OCCURRING CONDITIONS AND

Ethnic diversity affects the presentation, diagnosis, and
OTHER DEMENTIAS
treatment of dementia. Although APOE4 was initially be-
lieved to be a stronger risk factor for Alzheimers disease 1. General Medical Conditions
in whites than in Asians or blacks, it is now believed that Because the likelihood of chronic general medical ill-
APOE4 is associated with similar risks for developing Alz- nesses and the likelihood of dementia both increase with
heimers disease across ethnic groups (329, 330). age, the two commonly coexist. Memory impairment and
Prevalence rates of dementia vary across ethnic groups. aphasia, both of which interfere with the patients ability
For example, compared with whites, blacks may have a to provide a reliable description of symptoms, complicate
higher prevalence of vascular dementia and a lower preva- the assessment and treatment of general medical condi-
lence of Parkinsons disease (331). These differences are also tions. Resistance to physical examination can also compli-
affected by economic, educational, and co-occurring condi- cate assessment, so laboratory testing and radiological
tions (70, 332). One study of 240 blacks of U.S. and Carib- procedures may become particularly important. The in-
bean origin indicated that in both Alzheimers disease and volvement of family members and other caregivers in pro-
vascular dementia, blacks may have higher rates of psychosis, viding history is essential.
whereas whites may have higher rates of depression (333). Many medical conditions are known to have a signi-
Cultural differences may affect the familys perception cant impact on cognitive functioning. The identication
of cognitive symptoms and therefore their report of them and treatment of medical and psychiatric disorders that
to the physician, as well as attitudes toward treatment (334). can adversely affect cognition are especially important.
Ethnicity, race, and culture may inuence interpretation of For example, appropriate management of diabetes melli-
symptoms as well as attitudes toward nursing home place- tus may have benecial effects on cognition (336, 337).
ment; the clinician should be sensitive to varying beliefs
about the desirability of such a step (70, 335). Cultural 2. Delirium
background also has an impact on social networks, caregiv- Dementia predisposes to the development of delirium
ing style, presentation of disease symptoms such as depres- (338341), especially in the presence of general medical
sion, and acceptance of behavioral symptoms. and other neurological illnesses. Delirium in persons with
dementia negatively affects cognitive and functional abil-
4. Other Demographic and Psychosocial Factors ity, quality of life, and life span, as well as increases the
Another critical demographic factor affecting the care of need for institutionalization and rehospitalization and in-
patients with dementia is social support. The availability creases mortality (340).
of a spouse, adult child, or other loved one with the phys- Medications prescribed to treat co-occurring general
ical and emotional ability to supervise and care for the pa- medical conditions can lead to further cognitive impair-
tient, communicate with treating physicians, and otherwise ment or to delirium, even when doses are appropriate and
coordinate care may inuence the patients quality of life blood levels are in the nontoxic range. Prescribed and
as well as the need for institutionalization. In addition, a over-the-counter compounds with anticholinergic activ-
social network of friends, neighbors, and community may ity (e.g., tricyclic antidepressants, low-potency antipsy-
play a key role in supporting the patient and primary care- chotics, diphenhydramine, disopyramide phosphate,
givers. Spiritual supports and religious beliefs have been benztropine), histamine-2 blockade (cimetidine, raniti-
shown to have positive benets for caregivers well-being. dine), and narcotic properties are particularly likely to
These ndings should be taken into account in assessment cause delirium (342344), as are many other classes of
and treatment planning. medications. Of particular relevance to psychiatrists, de-
Resource availability varies widely by geographic re- lirium has been associated with virtually all psychotropic
gion and socioeconomic status. This issue should be con- medications, including lithium, other mood stabilizers,
antidepressants (including SSRIs), antipsychotics, and mon in Parkinsons disease (354) and may exacerbate
benzodiazepines (345). A comprehensive approach to de- functional impairment or be misinterpreted as dementia.
lirium includes prevention by avoidance of unnecessary Data supporting the efcacy of psychotherapy or antide-
medications and use of the lowest effective dosage, early pressants for the treatment of depression associated with
recognition of delirium through vigilant monitoring at Parkinsons disease are modest, but clinical experience
regular intervals, andwhen delirium does developa supports their use.
thorough search for other causes and prompt treatment to
decrease the associated morbidity. 4. Cerebrovascular Disease
Cerebrovascular disease can directly cause or contribute
3. Parkinsons Disease Spectrum Illnesses (Including to dementia by means of single and multiple infarcts,
Parkinsons Disease and Dementia With Lewy Bodies) hemorrhagic lesions, subcortical white matter disease, ar-
The cognitive impairment associated with Parkinsons teritis, and hypertension. For patients with dementia who
disease and related illnesses (including dementia with have a history of cerebrovascular disease or who have ev-
Lewy bodies) requires a broad treatment approach that idence on neurological examination or neuroimaging of
targets both cognitive and noncognitive neuropsychiatric cerebrovascular disease, a careful evaluation is essential to
symptoms. Mild cognitive impairment may be partially determine the etiology of the vascular changes (e.g., hy-
ameliorated by dopaminergic agents prescribed for the pertension, atrial brillation, or valvular disease) and to
treatment of motor symptoms (346), so both cognitive make any needed referrals for further evaluation and
and motor symptoms should be carefully monitored in as- treatment. Epidemiological evidence suggests that good
sessing the benets of dopaminergic enhancing therapies. control of blood pressure and low-dose aspirin might pre-
However, the use of dopaminergic agents predisposes pa- vent or lessen further cognitive decline (355, 356). The
tients to the development of visual hallucinations and acetylcholinesterase inhibitors donepezil and galantamine
other psychotic phenomena (347), especially in patients have shown at most modest efcacy in treating cognitive
with coexisting dementia, so these agents must be used impairment in patients with vascular dementia or mixed
with particular care, and the minimal dosage needed to vascular dementia and Alzheimers disease (357, 358), and
control the motor symptoms should be prescribed. In ad- there are safety concerns about the use of this class of
dition, patients with Parkinsons disease spectrum ill- medications in this population. Because there are no data
nesses are vulnerable to delirium from medications and on the specic treatment of neuropsychiatric complica-
concomitant general medical conditions, as discussed in tions of vascular dementia (359, 360), clinical practice ex-
Section III.B.2. Therefore, the development of these trapolates from studies of Alzheimers disease or studies of
symptoms deserves a thorough evaluation. Both pharma- dementia in general.
cological and behavioral interventions have been shown
to have benecial effects for specic patients with demen- 5. Frontotemporal Dementia Spectrum Disorders
tia. However, strong evidence guiding when to use one The spectrum of frontotemporal lobar degenerative
form over another is lacking. A number of clinical trials syndromes includes frontotemporal dementia, primary
have demonstrated the efcacy of acetylcholinesterase in- progressive aphasia, semantic dementia, corticobasal gan-
hibitors on cognition in dementia with Lewy bodies and glionic degeneration, progressive supranuclear palsy, and
dementia with Parkinsons disease with effects similar to hippocampal sclerosis (361) and account for about 5%
those seen in Alzheimers disease (168, 348, 349). 10% of patients with dementia. Patients with frontotempo-
Noncognitive neuropsychiatric symptoms often re- ral dementia typically have signicant alterations of per-
quire treatment in patients with dementia with Lewy bod- sonality and behavior, and the typical staging schema used
ies. Behavioral disturbances are often difcult to control. for Alzheimers disease (mild, moderate, severe) does not
If psychotic symptoms result in distress or danger, the ju- conform well to the typical natural history of frontotempo-
dicious use of an antipsychotic agent, often at low doses, is ral dementia. Overall, there is very limited evidence sup-
indicated. Although all antipsychotic agents can aggravate porting the use of any particular agent for frontotemporal
the motor disturbances of Parkinsons disease, open-label dementia spectrum disorders (362). Only one small ran-
data support the efcacy of second-generation antipsychot- domized controlled trial has evaluated the safety and/or ef-
ics for the treatment of psychotic symptoms associated with cacy of a treatment for associated cognitive or behavioral
these conditions (350353). Because antipsychotics can features (264, 362). This trial demonstrated that trazodone
dramatically worsen dementia with Lewy bodies, they may be benecial in decreasing problematic behaviors such
should be prescribed very cautiously. Depression is com- as irritability, agitation, depressive symptoms, or eating
problems in patients with frontotemporal dementias. In (84, 87, 371). The use of home health aides, day care, and
helping families understand and address specic aspects of respite care may provide stimulation for patients and
frontotemporal dementia spectrum disorders, psychiatrists needed relief for caregivers. End-of-life care for patients
may want to recommend the book What If Its Not Alzhei- with dementia is extremely demanding of family care-
mers? A Caregivers Guide to Dementia (363). givers, with many reporting high levels of depressive
symptoms while caring for their relatives with dementia.
However, within 3 months of the death, caregivers expe-
C. SITE-SPECIFIC ISSUES rience signicant declines in depressive symptoms (372).
The development of a treatment plan for a patient with
dementia focuses not only on the identication of specic 2. Day Care
symptoms and associated general medical problems but Day care provides a protected environment and appropri-
also depends on features of the environment in which the ate stimulation to patients during the day and gives care-
patient is cared for, as certain issues are specic to partic- givers a needed break to attend to other responsibilities.
ular care settings. Some day care centers specialize in the care of individuals
with dementia and may offer more appropriate activities
1. Home Care and supervision. Anecdotal reports and clinical experience
The majority of Americans with dementia reside in the support the benet to patients of scheduled activities.
community (364), although as many as 90% will receive However, behavioral symptoms can be precipitated by
long-term care during their lifetimes (365). Caring for pa- overstimulation as well as understimulation, so activities
tients with dementia at home presents challenges of social must be selected with care, and participation should be
isolation for the patient and emotional and physical strain adjusted according to each patients response. It is note-
on caregivers and others in the home. Care at home is worthy that problems can arise when patients with differ-
complicated by the need for many family caregivers to ent levels of dementia severity are expected to participate
work outside the home during the day. Providing care at together in the same activities.
home can also have adverse emotional effects on care-
givers, as well as their children. The psychological stress 3. Long-Term Care
on families of individuals with Alzheimers disease and A high proportion of patients with dementia eventually
other dementias appears to be more complex than simply require placement in a long-term-care facility such as a
the burden of caring for a disabled family member (366). nursing home, assisted living facility, or group home.
Older spousal caregivers who experience mental or Placement is usually due to the progression of the illness,
physical strain are at higher risk for health problems and the emergence of behavioral problems, the development
mortality than other caregivers (367, 368). It has been es- of intercurrent medical illness, or the loss of social sup-
timated that 30% of spousal caregivers experience a de- port. Both the patients characteristics (e.g., race, func-
pressive disorder while providing care for a husband or tional dependence, impaired cognition, behavior) and
wife with Alzheimers disease (369). The prevalence of de- caregivers characteristics (e.g., older age, level of caregiver
pressive disorders among adult children caring for a par- burden) are determinants of nursing home placement (335,
ent with Alzheimers disease ranges from 22%, among 373). Approximately two-thirds of the residents of long-
those with no prior history of affective disorder, to 37%, term-care facilities have dementia (374376), and as many
among those with a prior history of depression (369, 370). as 90% of them have behavioral symptoms. The number
Particularly difcult behavior problems for patients with of individuals with dementia living in assisted living facil-
dementia living at home include poor sleep, wandering, ities is now equivalent to the number living in nursing
accusations directed toward caregivers, threatening or homes (377). Thus, these facilities should be tailored to
combative behavior, and reluctance to accept help. How- meet the needs of patients with dementia and to ade-
ever, with assessment and treatment, these symptoms are quately address behavioral symptoms (120, 378). Well-
potentially modiable. Multifaceted interventions with trained staff are crucial to the humane care of patients
the family that provide emotional support, focus on the with dementia. Knowledge about dementia, neuropsychi-
management of the specic behavior problem, and, atric and behavioral symptoms, and approaches to im-
where appropriate, include careful monitoring of the proving caregiver well-being are essential elements of a
pharmacological treatment of behavioral symptoms have staff training program (379, 380).
demonstrated efcacy in reducing caregiver depression, There is little evidence from randomized controlled
caregiver burden, and rate of nursing home placement trials that addresses the optimum care of individuals in
nursing homes. One important element is employing The use of antipsychotic medications in nursing
staff who are committed to working with patients with homes, as elsewhere, for the treatment of behavioral and
dementia and are knowledgeable about dementia and the psychotic symptoms (see reference 387 for a review) re-
management of its noncognitive symptoms. Structured quires consideration of the potential benets and side ef-
activity programs can improve both behavior and mood fects. When used appropriately and cautiously (see
(120). Controlled research on psychotherapeutic inter- Sections II.C.5.b.1, and V.B.2.a.2), these medications can
ventions has been limited (see Section V.A). Other factors be modestly effective in reducing patient distress and in-
valued in nursing homes include privacy, adequate stimu- creasing safety for the patient, other residents, and staff.
lation, maximization of autonomy, and adaptation to Excessive dosing, on the other hand, and sometimes even
change with the progression of the disease (see references appropriate use, can lead to worsening cognition, overse-
381 and 382). Whether design features such as particular dation, falls, and numerous other complications including
colors for walls, doors, and door frames affect quality of increased mortality, and place patients at risk for tardive
care remains unknown. dyskinesia and other serious medical adverse events (see
There is no evidence that specialized dementia care Section V.B.2.a.2). Thus, regulations resulting from the
units produce better outcomes than traditional nursing Omnibus Budget Reconciliation Act of 1987 and good
home units. However, some such units may offer a model clinical practice require documentation of the indications
for the optimal care of patients with dementia in any nurs- for antipsychotic medication treatment, a discussion of
ing home setting. For example, Reimer et al. (383) reported available alternatives with the family or other surrogate
that quality of life for older residents with dementia was the decision makers, and the identication of treatment out-
same or better in a purpose-built and -staffed specialized comes. In the context of these regulations, the psychiatrist
care facility than in traditional institutional settings. should regularly reassess patients for medication response
A particular concern in nursing homes relates to the use and adverse effects, consider which patients may be ap-
of physical restraints and antipsychotic medications, which propriate for withdrawal of antipsychotic medications,
are regulated by the Omnibus Budget Reconciliation Act document the clinical reasoning for maintaining their use,
of 1987. Use of restraints and antipsychotic medications is and reinstate their prescription, as deemed clinically nec-
fairly common in nursing homes, and psychiatrists practic- essary (229). It is noteworthy that a structured education
ing in such settings must be familiar with these regulations, program for nursing and medical staff has been shown to
which generally can be obtained from the nursing home decrease antipsychotic usage in the nursing home setting
administrator, local public library, or regional ofce of the without adverse outcomes (120, 229, 388).
Center for Medicare and Medicaid Services. Although few Additional aspects of physical restraint use and antipsy-
studies are available to guide the appropriate use of re- chotic medication prescribing are described in Sections
straints in nursing homes, restraint use can be decreased by II.B.4.b and II.C.5.b.1, respectively.
strong administrative support for a restraint-free culture,
adoption of philosophy statements that promote a re- 4. Inpatient General Medical or Surgical Services
straint-free environment, staff education programs, effect- Patients with dementia on general medical and surgical
ing environmental changes that reduce the risk of falls or services are at particular risk for three problems, all of
wandering, and careful assessment and treatment of possi- which can lead to aggressive behavior, wandering, climb-
ble causes of agitation. Rates of restraint use have also been ing over bed rails, removal of intravenous lines, and resis-
shown to vary with specic resident characteristics, the tance to needed medical procedures. First, cognitive
number of residents in a facility, and the nurse/resident ra- impairment makes patients with dementia vulnerable to
tio (384386). Although chest or wrist restraints are occa- behavioral problems owing to fear, lack of comprehen-
sionally used for patients who pose an imminent risk of sion, and lack of memory of what they have been told. No
physical harm to themselves or others (e.g., during evalu- data are available to guide treatment recommendations,
ation of a delirium or during an acute-care hospitalization but general practice supports a preventive approach of
for an intercurrent illness), the use of staff to provide con- having family members or aides stay with the patient. Fre-
stant, close supervision is preferable. For long-term-care quent reorientation and explanation of hospital proce-
facilities, geri-chairs may have a place in the care of pa- dures and plans, writing down important information for
tients at extreme risk of falling and for whom all other op- the patient, maintaining adequate light, and avoidance of
tions have failed. Regular use of restraints is not overstimulation may also be useful.
recommended unless alternatives have been exhausted. Second, persons with dementia are at high risk for de-
When they are used, they require periodic reassessment lirium, as discussed in Section III.B.2 (338340, 389). Pre-
and careful documentation. vention of delirium by judicious use of any necessary
medications and elimination of any unnecessary ones, at- 5. General Psychiatric Inpatient Units
tention to uid and electrolyte status, and prompt treat- Individuals with dementia may require admission to a psy-
ment of infectious diseases can also diminish morbidity. chiatric unit for the treatment of psychotic, affective, or
Inouye et al. (26) showed the efcacy of a protocol of ori- behavioral manifestations of neuropsychiatric disorders.
entation strategies and therapeutic activities to prevent For patients who are very frail or who have signicant
delirium in hospitalized older adults, many of whom had general medical illnesses, a geriatric psychiatry or medical
dementia. Occasionally, psychopharmacological treat- psychiatric unit may be helpful when available. Hospital-
ment for cognitive impairment (e.g., with a cholinesterase ization may be indicated because of the severity of symp-
inhibitor) and for behavior disorders (antipsychotic toms, such as psychosis, depression, threats of harm to self
agents) is used in the management of patients with delir- or others, and violent or uncontrollable behavior. It may
ium, but no controlled trials exist (340). also be indicated because of the intensity of services re-
Third, patients with dementia may have difculty quired for treatment such as continuous skilled observa-
understanding and communicating pain, hunger, and tion, ECT, or a medication or diagnostic test that cannot
other uncomfortable states. For this reason, the devel- be performed on an outpatient basis (for literature review,
opment of irritability and/or agitation should prompt a see reference 1).
thorough evaluation to identify an occult medical prob- A thorough search for environmental, general medical,
lem or a possible source of discomfort. A signicant or other psychiatric difculties that may be leading to the
part of the psychiatrists role in this setting is educating neuropsychiatric disturbance will often reveal a treatable
other physicians and hospital staff regarding the diag- problem. Both nonpharmacological and pharmacological
nosis and management of dementia and its behavioral interventions can be tried more readily and aggressively
manifestations. on inpatient units than in outpatient settings.
Part B
BACKGROUND INFORMATION AND REVIEW OF
AVAILABLE EVIDENCE
IV. DISEASE DEFINITION, NATURAL HISTORY,

AND EPIDEMIOLOGY
Many types of dementias exist, and they have a number of tioning (the ability to think abstractly and to plan, initiate,
features in common. This section contains a discussion of sequence, monitor, and stop complex behavior). The or-
dementia in general and brief descriptions of some of the der of onset and relative prominence of the cognitive dis-
more common types of dementias. turbances and associated symptoms vary with the specic
type of dementia, as discussed in Section IV.F.
Memory impairment is often a prominent early symp-
A. DEFINITION OF DEMENTIA
tom. Individuals with dementia have difculty learning
The essential features of a dementia are acquired multiple new material. These short-term memory problems com-
cognitive decits that usually include memory impair- monly result in losing valuables such as wallets and keys or
ment and at least one of the following phenomena in the forgetting food cooking on the stove. In more severe de-
absence of a delirium that might explain the decit: apha- mentia, individuals also forget previously learned mate-
sia, apraxia, agnosia, or a disturbance in executive func- rial, including the names of loved ones. Individuals with
dementia may have difculty with spatial tasks, such as Individuals with dementia are especially vulnerable to
navigating around the house or in the immediate neigh- the effects of change and psychosocial stressors (such as
borhood. Poor judgment and poor insight are common bereavement or going to the hospital), and these stressors
as well. Individuals may exhibit little or no awareness of can worsen intellectual decits and exacerbate neuropsy-
memory loss or other cognitive decits. They may make chiatric symptoms. Patients with dementia are particu-
unrealistic assessments of their abilities, underestimate larly susceptible to developing delirium, as discussed in
the risks involved in activities such as driving, and make Section III.B.2. Dementia may be accompanied by neuro-
plans that are incongruent with their decits and progno- logical symptoms such as gait difculties, dysarthria, swal-
sis (e.g., planning to start a new business). lowing difculty with consequent choking or aspiration,
In order for a diagnosis of dementia to be made, the urinary and fecal incontinence, seizures, tremor, myoclo-
cognitive decits must be sufciently severe to cause im- nus, and other abnormal movements.
pairment in occupational or social functioning and must
represent a decline from a previous level of functioning. C. DIFFERENTIAL DIAGNOSIS
The nature and degree of impairment are variable and of-
ten depend on the particular social setting of the individ- The differential diagnosis of dementia is described in de-
ual. For example, mild dementia may signicantly impair tail in DSM-IV-TR and is only summarized here (392,
an individuals ability to perform a complex job but not a 393). Age-associated memory changes are modest and not
less demanding one. When memory impairments and/or associated with functional impairment or depression.
other cognitive decits are present in the setting of intact Memory impairment occurs in both delirium and demen-
functional status, the patient is usually given a diagnosis of tia. A new diagnosis of dementia cannot be made when de-
mild cognitive impairment (390) (see Section IV.F.2). lirium is present. Delirium, discussed in Section III.B.2, is
There is not yet a general consensus on the criteria for de- characterized by a reduced ability to maintain and shift at-
ning and diagnosing mild cognitive impairment (391). tention appropriately, uctuating cognitive decits, and
impaired level of consciousness, whereas the decits in de-
mentia tend to be stable or progressive, and level of con-
B. ASSOCIATED FEATURES
sciousness is unaffected. In addition, the onset of delirium
Some individuals with dementia experience a variety of may be acute, and its course is often time limited. Amnestic
neuropsychiatric symptoms that may include disinhibited disorder is characterized by memory impairment without
behavior, making inappropriate jokes, neglecting personal signicant impairment in other cognitive domains. Mental
hygiene, exhibiting undue familiarity with strangers, or dis- retardation has an onset before age 18 years and is charac-
regarding conventional rules of social conduct. They may terized by signicantly subaverage general intellectual
also demonstrate apathy, amotivation, and withdrawal. De- functioning, which may not include memory impairment.
pressed mood, with or without neurovegetative changes, is Schizophrenia may be associated with multiple cognitive
quite common, as are sleep disturbances and anxiety inde- impairments and a decline in functioning, but the cogni-
pendent of depression. Suicidal behavior may occur, espe- tive impairment tends to be less severe and occurs against a
cially in mildly impaired individuals, who are more likely to background of psychotic and behavioral symptoms meet-
have insight into their decits and to be capable of formu- ing the established diagnostic criteria.
lating and carrying out a plan of action. Some patients man- Major depression is an important element of the dif-
ifest catastrophic reactions, overwhelming emotional ferential diagnosis of memory difculties. Particularly in
responses to relatively minor stressors, such as changes in elderly persons, major depressive disorder may be associ-
routine or environment. Occasionally, they may harm oth- ated with reports of memory impairment, difculty con-
ers by striking out. Delusions can occur, especially those in- centrating, and a reduction in intellectual abilities
volving themes of spousal indelity and persecution such as described by history or observed on mental status exami-
the belief that misplaced possessions have been stolen. Mis- nation. Depression and progressive dementia may some-
identications of familiar people as unfamiliar (or vice times be distinguished on the basis of an assessment of the
versa) frequently occur. Delusions that a spouse or care- course and onset of depressive and cognitive symptoms
giver is an imposter are particularly difcult for patients and by response of cognitive symptoms to treatment of
and their families. Hallucinations can occur in all sensory the depression. However, even when the onset of depres-
modalities, but visual hallucinations are most common. sive symptoms precedes or coincides with the onset of
Some patients exhibit a peak period of agitation (or other cognitive symptoms and both resolve with antidepressant
behavioral disturbances) during the evening hours, which is treatment, more than 50% of patients go on to develop
sometimes referred to as sundowning. dementia or mild cognitive impairment within several
years of the depressive episode (280, 394, 395). In addi- underlying etiology and of the availability and timely ap-
tion, among patients with mild cognitive impairment (see plication of effective treatment.
Section IV.F.2), evidence suggests that those who are also
depressed have a greater likelihood of developing Alzhei- E. STAGING OF DEMENTIA
mers disease (396). Dementia must be distinguished from
malingering and factitious disorder, which generally man- Progressive dementias are generally staged globally ac-
ifest patterns of cognitive decits that are inconsistent cording to the level of cognitive and functional impair-
over time and are uncharacteristic of those typically seen ment, and the same categories may be used to describe the
in dementia. degree of severity of any dementia (401, 402). However,
Dementia must also be distinguished from milder the staging criteria have not been well validated for non-
symptoms. Subjective memory complaints are common as Alzheimers dementias. Specic functional staging (FAST
people get older. Many individuals with these complaints staging) has also been developed, is widely used, and can
have subtle, nonprogressive declines in memory, but some be very useful in tracking the course of Alzheimers disease
have more signicant impairment that is more likely to and other dementias (403). The ability to perform a spe-
represent the prodromal phase of Alzheimers disease or cic function depends on baseline skills, acquired decits,
another dementia. The category of mild cognitive impair- and the social environment. Consequently, the severity of
ment (390) was developed to describe individuals in this illness should be assessed in the context of past function-
prodromal phase (see Section IV.F.2) (6, 391, 397). ing in several domains. Behavioral and neuropsychiatric
symptoms are not stage specic.
The CDR is a commonly used scale to stage dementia
D. PREVALENCE AND COURSE
severity (401). Individuals with a CDR of questionable
Exact estimates of the prevalence of dementia depend on (CDR of 0.5) show mild decits in memory and some-
the denition and specic threshold used, but it is clear that times in other areas and have doubtful or mild functional
the prevalence increases dramatically with age. The syn- impairment. When such individuals present for clinical
drome affects approximately 5%8% of individuals over evaluation, they tend to have fairly signicant memory
age 65 years, 15%20% of individuals over age 75 years, impairment that is evident on objective testing as well,
and 25%50% of individuals over age 85 years (398). Alz- and they are typically assigned a diagnosis of mild cogni-
heimers disease is the most common dementia, accounting tive impairment (see Section IV.F.2) or mild dementia.
for 50%75% of the total number of cases of dementia, The Global Deterioration Scale (GDS) distinguishes
with a greater proportion of cases in the higher age ranges. three stages in this range (402). A GDS stage of 2 desig-
Vascular dementia is probably next most common; preva- nates normal aging, in which older persons have subjec-
lence estimates vary widely and depend on the denition of tive decits in cognition and related areas only. Many
vascular dementia used; pure vascular disease may account studies have indicated that persons with these complaints
for 5%20% of cases of dementia, and mixed dementia are at increased risk for decline over subsequent years
Alzheimers disease with vascular dementiaoccurs at least (404406). The GDS stage 3, which includes subtle but
as frequently. Dementia with Lewy bodies may present manifest cognitive decits, generally accompanied by ex-
with frequent falls, hallucinations, and cognitive uctua- ecutive level functional decits, is equivalent to mild cog-
tion as well as mild parkinsonism and may account for up to nitive impairment (391). Such individuals should be
20% of individuals with dementia (399, 400). evaluated over time. Many patients with mild cognitive
The mode of onset and subsequent course of dementia impairment progress to Alzheimers disease or another
depend on the underlying etiology. Typically, Alzheimers dementia, some patients decits remain stable without
disease, dementia with Lewy bodies, and frontotemporal progression, and a few return to normal functioning (6).
dementia have an insidious onset and gradual decline, In community settings, this group of individuals is heter-
whereas vascular dementia may be characterized by a ogeneous; some are similar to those who would be given a
more acute onset and stepwise decline. However, since diagnosis of mild cognitive impairment in a memory
both Alzheimers disease and vascular dementia are com- clinic, whereas others have much more subtle symptoms
mon and the two frequently coexist, a secondary diagnosis that may be consistent with normal aging. Patients who
of vascular dementia or a diagnosis of mixed dementia is have been systematically diagnosed as having mild cogni-
often made when a gradually progressive dementia occurs tive impairment in memory clinics tend to be more homo-
in the setting of known cerebrovascular disease. Other de- geneous and more likely to progress to dementia.
mentias may be progressive, static, or occasionally remit- Individuals with mild dementia (MMSE score of >18,
ting. The reversibility of a dementia is a function of the GDS or FAST stage 4, CDR of 1) are likely to have dif-
culties with balancing a checkbook, preparing a complex Onset of Alzheimers disease generally occurs in late
meal, or managing a difcult medication schedule. Those life, most commonly in the 60s, 70s, and 80s and beyond,
with moderate impairment (MMSE score of 1018, but in rare instances the disorder appears in the 40s and
GDS or FAST stages 5 and 6, CDR of 2) also have dif- 50s. The incidence of Alzheimers disease also increases
culties with simpler food preparation, household cleanup, with age, and it is estimated at 0.5% per year from age 65
and yard work and may require assistance with some as- 69 years, 1% per year from age 7074 years, 2% per year
pects of self-care (e.g., picking out the proper clothing to from age 7579 years, 3% per year from age 8084 years,
wear). Those whose dementia is severe (MMSE score of and 8% per year from age 85 years onward (409). Progres-
<10, GDS or FAST stages 6 and 7, CDR of 3) require con- sion is gradual but steadily downward, with an average du-
siderable or total assistance with personal care, such as ration from onset of symptoms to death of 810 years.
dressing, bathing, and toileting. Research has shown that Plateaus may occur, but progression generally resumes af-
measurable cognitive abilities remain throughout the ter 1 to several years.
course of severe dementia (407). In the terminal phase, pa- In DSM-IV-TR, Alzheimers disease is subdivided into
tients become bed bound, develop contractures (408), re- the subtypes With Early Onset and With Late Onset,
quire constant care, and may be susceptible to accidents as well as With and Without Behavioral Disturbance.
and infectious diseases, which ultimately prove fatal. Other predominant features of the current clinical pre-
sentation such as psychosis, mood disorder, or personality
change, are coded with their own Axis I code.
F. SPECIFIC DEMENTIAS
1. Dementia of the Alzheimers Type 2. Mild Cognitive Impairment
Dementia of the Alzheimers type, commonly referred to Mild cognitive impairment is a term used to represent a
as Alzheimers disease, has an insidious onset and gradual variety of mild cognitive syndromes manifested by a mod-
progression. Various patterns of decits are seen, but the est but detectable decline in cognitive function in the set-
disorder begins most commonly with decits in recent ting of largely intact functional status (391). Because it is
memory, which are followed by aphasia, visuospatial per- expected that new treatments will be better at preserving
ceptual impairments, apraxia, and agnosia after several than restoring neuronal function, early recognition of
years. Decits in executive function (e.g., performing these mild syndromes, particularly those thought to rep-
tasks involving multiple steps, such as balancing a check- resent the prodromal phase of Alzheimers disease and
book or preparing a meal) are also typically seen early in other neurodegenerative dementias, are a major focus of
the course of the disease. Neuropsychiatric symptoms are current research. Mild cognitive impairment is conceived
common in Alzheimers disease. Depression, anxiety, ir- of as a transitional state between normal aging and de-
ritability, apathy, and even subtle personality changes are mentia (particularly Alzheimers disease) in which cogni-
fairly common in the early stages of the disease, whereas tive decits are present but function is preserved. As such,
in the middle and later stages of the disease psychotic the population of patients meeting the criteria for mild
symptoms and behavioral disturbances are more com- cognitive impairment is inherently unstable, as many pa-
mon. Patients usually develop incontinence and gait and tients progress to meet the criteria for dementia. More-
motor disturbances, and eventually become mute and over, because mild cognitive impairment lies along a
bed bound. Seizures and myoclonus may also occur late continuum between normal aging and dementia, its pre-
in the disease. cise upper and lower boundaries are difcult to deter-
The diagnosis of Alzheimers disease should be made mine. A variety of research denitions for mild cognitive
only when the patient exhibits the typical symptom prole impairment are in place, but there is no consensus on the
of Alzheimers disease and when other etiologies for the optimal denition. The most widely accepted denition
dementia have been ruled out by careful history, physical requires the following: 1) subjective cognitive complaints,
and neurological examinations, and clinical and labora- 2) evidence of objective decits in cognitive function
tory tests. A denitive diagnosis of Alzheimers disease re- based on age- and education-adjusted norms on standard-
quires both the clinical syndrome and microscopic ized neuropsychological tests, 3) intact daily functioning,
examination of the brain at autopsy, at which time the 4) evidence of cognitive decline from a prior level, and
characteristic plaques and neurobrillary tangles widely 5) evidence of not meeting the criteria for dementia (410).
distributed in the cerebral cortex will be seen. A careful Mild cognitive impairment is sometimes divided into
clinical diagnosis of Alzheimers disease conforms to the subtypes based on the most prominent symptoms. One
pathological diagnosis 70%90% of the time. subtype, referred to as amnestic mild cognitive impair-
ment, may be the prodromal stage of Alzheimers disease strokes also have pathological signs of Alzheimers disease.
(410). A large proportion of patients who meet the criteria The degree to which strokes alone are responsible for de-
for mild cognitive impairment probably have the prodro- mentia is unclear; estimates for the fraction of dementia
mal phase of Alzheimers disease, particularly when short- caused by pure vascular dementia range from 5% to
term memory loss dominates the clinical picture (173). 20% (416). Early treatment of hypertension and vascular
However, it should be noted that, no matter how it is de- disease may prevent further progression. Vascular demen-
ned, mild cognitive impairment is a heterogeneous cat- tia associated with autoimmune disease occurs in concert
egory that includes some individuals with nonprogressive with other symptoms of the specic illness and in the age
decits, some with prodromal Alzheimers disease and group characteristic of the specic disease (e.g., systemic
other dementias, and some for whom a diagnosis of early lupus erythematosus, giant cell arteritis).
Alzheimers disease or another dementia would be more Like Alzheimers disease, vascular dementia is subtyped
appropriate. by DSM-IV-TR according to certain clinical features.
Subtypes available for vascular dementia include With
3. Vascular Dementia Delirium, With Delusions, With Depressed Mood,
Vascular dementia results from the effects of cerebrovas- and Uncomplicated. Clinically signicant behavioral
cular disease on cognitive function. Several cerebrovascu- disturbances can be coded as a modier but are not con-
lar mechanisms can lead to cerebral injury, including large sidered a separate subtype. No subtyping based on age of
vessel infarctions, multiple lacunar infarctions, extensive onset is used. More formal diagnostic criteria, typically
subcortical and periventricular white matter disease, and focused on differentiating pure vascular dementia from a
microvascular changes. These types of tissue injuries are mixture of Alzheimers disease and vascular pathology, are
usually due to atherosclerotic disease or amyloid angiop- used in the research setting (417). These criteria vary
athy. Autoimmune mechanisms are far less likely. widely, particularly to the extent that they stress clinical
The full range of clinical symptoms in vascular demen- versus radiographic evidence for stroke, and there is no
tia is not well understood. The best known syndrome is consensus on optimal criteria for vascular dementia at this
cognitive impairment that occurs shortly after a clinically time (5, 418, 419).
recognized stroke (within 3 months), with evidence of in-
farctions in brain areas relevant to the impaired cognitive 4. Dementia of Parkinsons Disease and Dementia With
functions. Neurological signs and symptoms consistent Lewy Bodies
with cerebrovascular damage (hemiparesis or hemiano- Lewy bodies are commonly found at autopsy in individu-
pia) are usually present. There is no specic cognitive als with late-life dementia. There are two subtypes of
prole of vascular dementia, although executive and at- Lewy body disease depending on whether Parkinsons dis-
tentional decits may be more pronounced than impair- ease precedes cognitive impairment by more than 1 year
ment in short-term memory. The pattern of cognitive (Parkinsons disease dementia) or whether the cognitive
decits is often patchy, depending on which regions of the impairment is the dominant symptom (dementia with
brain have been damaged (411). Lewy bodies). Whether or not these entities are best
The incidence and prevalence of vascular dementia classied as one condition or as distinct ones is still un-
mirror those of Alzheimers disease in that vascular de- resolved. Parkinsons disease is a slowly progressive neu-
mentia becomes increasingly common with advanced age rological condition characterized by tremor, rigidity,
(412414). The relationship between Alzheimers disease bradykinesia, and postural instability; its onset is typically
and vascular dementia is complex. Alzheimers disease and in middle to late life. Estimates of the prevalence of de-
strokes are both common and frequently coexist (al- mentia in Parkinsons disease vary. One large longitudinal
though often only one diagnosis is recognized during a study found that dementia developed in nearly 80% of pa-
persons life). In addition, a wide variety of evidence from tients followed for 8 years (420). The dementia associated
neuroimaging, neuropathological, epidemiological, and with Parkinsons disease has an insidious onset and slow
genetic studies suggests that the two share common risk progression and is characterized by cognitive and motor
factors, such as hypertension, diabetes, hypercholesterol- slowing, executive dysfunction, and impairments in mem-
emia, hyperhomocysteinemia, as well as others (415). ory retrieval and exibility. Parkinsons disease is impor-
There is also considerable neuropathological overlap be- tant to psychiatrists because of the high prevalence of
tween the two conditions. Many patients with typical associated depression and the frequent occurrence of psy-
pathological signs of Alzheimers disease have cerebrovas- chotic symptoms such as visual hallucinations during
cular disease as well, whereas other patients with clear pharmacological treatment of the primary motor decit.
Dementia with Lewy bodies has been recognized clini- campal sclerosis (361, 426). Argyrophilic grain disease
cally only in the last 1015 years (421, 422). In many ways may also be included in this group of conditions (427). In
it is clinically similar to Alzheimers disease. Important frontotemporal dementia spectrum disorders, structural
clinical differences that distinguish dementia with Lewy brain imaging typically reveals prominent frontal and/or
bodies include visual hallucinations that appear earlier in temporal atrophy, with relative sparing of the parietal and
the disease course and tend to be more prominent, parkin- occipital lobes. The formal diagnosis of Picks disease,
sonian features such as postural instability and falls that ap- which is only one of the numerous neuropathological sub-
pear early in the disease course, cognitive uctuations types of this condition, depends on the neuropathological
lasting days to weeks, and a somewhat more rapid evolu- nding of Pick inclusion bodies (361). About one-third of
tion. Patients with dementia with Lewy bodies are mark- cases are familial, and a number of specic genetic defects
edly sensitive to the extrapyramidal effects of antipsychotic have been identied (29). The disorder most commonly
medications, and these medications should be used only manifests in patients ages 5060 years, although it can oc-
with the utmost caution in these patients. Dementia with cur among older or younger individuals. The course is
Lewy bodies may account for as many as 7%26% of de- progressive and can be more rapid than that of Alzhei-
mentia cases, depending on the criteria used (423, 424). mers disease, although there is signicant heterogeneity.
The disorder is particularly likely to come to psychiatric Once thought to be rare, these conditions have been
attention because of a patients prominent psychotic symp- found to be more common, and careful assessment may
toms and sensitivity to antipsychotic medications. reveal cases previously missed. These conditions are im-
The neuropathology of Parkinsons disease and de- portant for psychiatrists because they often present with a
mentia with Lewy bodies are identical and include an variety of psychiatric symptoms, including disinhibition,
abundance of Lewy inclusion bodies in both subcortical apathy, depression, anxiety, personality change, substance
and cortical regions (422). Because autopsies often reveal abuse, family conict, and impaired work performance,
both the neuropathologies of dementia with Lewy bodies that initially overshadow the cognitive impairment, com-
and Alzheimers disease, controversy exists about the in- plicating and delaying the proper diagnosis.
dependence of the two diseases. The development of valid
clinical and pathological diagnostic criteria for dementia 6. Other Progressive Dementing Disorders
with Lewy bodies is an area of active research. Other disorders that can lead to progressive dementia in-
clude Huntingtons disease and Creutzfeldt-Jakob dis-
5. Dementia Due to Frontotemporal Dementia ease. Huntingtons disease is an autosomal dominant
Spectrum Disorders disorder that affects the basal ganglia and other subcorti-
Frontotemporal dementia (formerly referred to as Picks cal structures and includes motor, behavioral, mood, and
disease and sometimes referred to as frontotemporal lo- cognitive symptoms. Creutzfeldt-Jakob disease is a rap-
bar degeneration) is characterized in its early stages by idly progressive spongiform encephalopathy associated
changes in personality, signicant apathy, executive dys- with a prion (proteinaceous infectious particle). Variant
function, deterioration of social skills, emotional blunt- Creutzfeldt-Jakob disease, thought to be due to introduc-
ing, behavioral disinhibition, and prominent language tion into the human food chain of scrapie-like prion dis-
abnormalities. Difculties with memory, apraxia, and ease, usually presents before age 40 years with psychiatric
other features of dementia usually follow later in the symptoms. Cognitive decline is rapid, with death usually
course. As the dementia progresses, it may be accompa- occurring within 1.5 years.
nied by extreme agitation. Individuals may develop such
severe problems with language, attention, or behavior 7. Dementia Due to Other Causes
that it may be difcult to assess the degree of cognitive im- In addition to the preceding categories, a number of
pairment. Early prominent changes in personality and be- general medical conditions can cause dementia (428).
havior, severe apathy, and/or early language decits help These conditions include structural lesions (e.g., pri-
to distinguish this group of disorders from Alzheimers mary or secondary brain tumors, subdural hematoma,
disease. Two sets of diagnostic criteria for frontotemporal slowly progressive or normal-pressure hydrocephalus),
dementia spectrum disorders have been proposed (361, head trauma, endocrine conditions (e.g., hypothyroid-
425). The criteria of McKhann et al. include several dis- ism, hypercalcemia, hypoglycemia), nutritional condi-
orders previously considered to be distinct: progressive tions (e.g., deciency of vitamin B12, thiamine, or niacin),
supranuclear palsy, corticobasal ganglionic degeneration, other infectious conditions (e.g., HIV, neurosyphilis, Cryp-
amyotrophic lateral sclerosis with dementia, and hippo- tococcus), derangements of renal and hepatic function, neu-
rological conditions (e.g., multiple sclerosis), effects of abuse, especially alcohol abuse. It is critical that psychia-
medications (e.g., benzodiazepines, beta-blockers, anticho- trists caring for individuals with dementia be familiar with
linergics), autoimmune diseases (e.g., lupus erythematosus, the general medical and neurological causes of dementia
vasculitis, Hashimotos encephalopathy, neurosarcoidosis), in order to ensure that the diagnosis is accurate and, in
environmental toxins (e.g., heavy metals, organic hydro- particular, that potentially treatable conditions are not
carbons), and the toxic effect of long-standing substance missed.
V. REVIEW OF AVAILABLE EVIDENCE

A. SPECIFIC PSYCHOTHERAPIES/PSYCHOSOCIAL At this time there is insufcient evidence to claim su-
periority of either behavioral approaches or pharmaco-
TREATMENTS
logical approaches (117, 214). Studies combining the two
Specic psychosocial treatments for dementia can be di- types of approaches are almost nonexistent, although they
vided into four broad groups: behavior oriented, emotion are often combined in clinical practice. In a randomized
oriented, cognition oriented, and stimulation oriented. placebo-controlled trial that included 149 patients with
Few of these treatments have been subjected to rigorous Alzheimers disease and agitation, haloperidol (mean dose
double-blind, randomized, controlled trials, although of 1.8 mg/day), trazodone (mean dose of 200 mg/day), and
some are supported by research ndings and have gained behavior management techniques were compared over a
clinical acceptance. Published studies have generally been 16-week period. Overall, 34% of the patients improved,
based on small samples and have been of limited duration, but there were no differences between treatment groups,
and many of the reports fail to fully characterize the inter- although fewer episodes of bradykinesia and parkinsonian
vention, the nature or stage of the subjects dementia, their gait occurred in the behavior management group (214). In
baseline status, or the persistence of any improvement. a study that included 153 community-dwelling patients
with Alzheimers disease, routine medical care was com-
1. Behavior-Oriented Approaches pared with a structured program combining exercise
Behavioral interventions have not been shown to improve training and caregiver training in the management of
the overall functioning of patients with dementia, but problematic behaviors; the results showed no statistically
there is some evidence that they can be effective in lessen- signicant reduction in nursing home admissions due to
ing or eliminating some specic problem behaviors, as de- behavioral disturbances but did show improvement in
scribed in literature reviews (112, 115). For example, mood and physical role function (117). In another study,
behavioral interventions such as scheduled toileting can 12 nursing homes or residential homes were randomly as-
reduce frequent urinary incontinence (429). The evidence signed to receive a 6-month training and education inter-
from a few well-designed studies of behavioral manage- vention or to provide usual care. The patients in the
ment therapy shows that behavioral interventions can be intervention homes did slightly better in cognition and
somewhat benecial for improving mood and disruptive mood than the patients in the homes that provided usual
behavior. A body of literature consisting of small trials or care, but there was no difference between groups on mea-
single case studies supports the short-term benets of be- sures of behavior (118).
haviorally focused interventions (118, 430436). For ex-
ample, results of a small randomized controlled study (32 2. Emotion-Oriented Approaches
subjects in each group) of a four-session aggressive behav- Emotion-oriented interventions include reminiscence
ior management training program for caregivers showed a therapy (438), validation therapy (439, 440), supportive
trend toward lower rates of aggression in the experimental psychotherapy (441), sensory integration (442), and sim-
group, compared to the control group (P = 0.071), but that ulated presence therapy (443).
difference was not statistically signicant (431). In addi- Reminiscence therapy, in which the aim is to stimulate
tion, a review of the literature revealed modest effective- memory and mood in the context of the patients life his-
ness of such treatments (113). Nonetheless, with some tory, has been shown in three studies of confused elderly
exceptions, the limited available follow-up data have sug- persons (122124) to be associated with modest short-
gested that the benets do not persist beyond the duration lived gains in mood, behavior, and cognition. A single
of the interventions (116, 437). small study of validation therapy, in which the aim is to re-
store self-worth and reduce stress by validating emotional presence, and aromatherapy, some of which overlap with
ties to the past, found that validation therapy did not im- emotion-oriented interventions in their content. They are
prove cognitive, functional, and mood measures more intended to mobilize the patients available cognitive re-
than reality orientation or no intervention (444). For nurs- sources by providing stimulation and enrichment. Benets
ing home residents with moderate to severe dementia, a of music therapy may include improving mood, decreasing
staff training program emphasizing emotion-oriented care behavior problems, enhancing socialization and quality of
(which combined validation therapy, sensory stimulation, life, and encouraging emotional expression (468).
and reminiscence) found no effects on cognitive, func- There is some evidence that, while they are in use,
tional, or behavioral outcomes (445). Supportive psycho- these interventions decrease behavioral problems and im-
therapy has received little or no formal scientic study, but prove mood. Rovner et al. (120) tested the efcacy of an
some clinicians nd it useful in helping mildly impaired intervention combining activities, guidelines for psycho-
patients adjust to their illness. Cochrane reviews of valida- tropic drug use, and educational rounds to reduce behav-
tion therapy, reminiscence, and Snoezelen (controlled ior disorders in 89 nursing home patients with moderate
multisensory stimulation) did not identify reliable empiri- to severe dementia. After 6 months, the prevalence of be-
cal evidence of efcacy of these interventions (446448). havior disorders and psychotropic drug and restraint use
was signicantly lower in the experimental group, com-
pared with usual care controls. Camberg et al. (121) tested
3. Cognition-Oriented Approaches
the efcacy of simulated presence to reduce agitation and
Cognition-oriented techniques include reality orientation
withdrawn behaviors in 54 nursing home residents with
(449) and skills training (450). The aim of these treatments
severe dementia. Simulated presence was an audiotaped,
is to restore cognitive decits, often in a classroom setting.
individualized telephone conversation consisting of recol-
In a number of studies of both institutionalized and non-
lections of the persons life; control comparisons were a
institutionalized patients, reality orientation has produced
placebo audiotape (e.g., someone reading a newspaper)
modest but transient improvement in verbal orientation
and usual care. Whenever study subjects exhibited agi-
(122, 451460). Some studies have also demonstrated
tated or withdrawn behaviors, they were exposed to the
slight transient improvement in other measures of cogni-
assigned intervention. According to staff observation logs
tion, function, behavior, and social interaction. However,
(with raters blind to treatment assignment), simulated
there have also been case reports of anger, frustration, and
presence signicantly reduced rates of agitation, com-
depression precipitated by reality orientation (127).
pared with usual care or placebo (121).
There is some evidence of benet from cognitive re-
Baker et al. (469) tested the effectiveness of multisen-
mediation and from skills (or memory) training. Spector
sory stimulation in 50 patients with moderate to severe
et al. (125) conducted a single-blind, multicenter, con-
dementia attending a day treatment program and found
trolled clinical trial comparing a cognitive stimulation
short-lived improvements in mood, attention, and behav-
program with routine care for 201 patients with dementia
ior. However, a second trial (470) involving 136 patients
attending day treatment programs or residing in nursing
failed to nd differences in these outcomes, compared to
homes. They found improvements in scores on the
outcomes of a control condition consisting of an activities
MMSE and the Alzheimers Disease Assessment Scale
program. Robichaud et al. (442) similarly found no im-
Cognitive Subscale (ADAS-cog) and in quality-of-life
provements in mood, cognition, or behavior in response
measures. Other studies have reported short-lived gains
to a sensory integration intervention in 40 nursing home
with ultimate return to baseline levels of cognition and
residents with dementia. Two studies have investigated
behavior and no generalization of skills to other areas of
the efcacy of aromatherapy to reduce agitation in nurs-
cognition (450, 461467). In addition, there have been re-
ing home residents with severe dementia. Ballard et al.
ports of frustration in patients and depression in care-
(471) reported reduced agitation and improved quality of
givers associated with this type of intervention (86). The
life, whereas Snow et al. (472) found no benet. Five re-
modest and transient improvements observed with some
cent studies have investigated the benets of exercise; four
of these treatments may not justify the cost of the inter-
studies (117, 473475) reported improved mobility, phys-
vention or the risk of adverse effects.
ical endurance, strength, and mood, whereas one study
(476) found no change in mobility and function. Addi-
4. Stimulation-Oriented Approaches tional support for this approach comes from the work of
These treatments include recreational activities or thera- Teri et al. (119, 477), who have developed a behavioral
pies (e.g., crafts, games, pets), art therapies (e.g., music, protocol for managing Alzheimers disease that includes a
dance, art), exercise, multisensory stimulation, simulated number of stimulation-oriented interventions. The core
of this protocol, identifying and increasing the number of ticentered. Most trials have been 1224 weeks in duration,
previously enjoyed pleasant activities, has been shown in although at least two have lasted 1 year (137, 139), and one
preliminary studies to improve the mood of patients and lasted more than 2 years (136). Studies have generally
caregivers alike. been conducted with community-dwelling patients, al-
In general, the data supporting efcacy for stimula- though one trial included nursing home residents with
tion-oriented therapies are limited either by small num- moderate to severe dementia (145). The majority of stud-
bers of subjects (459, 478, 479) or use of multiple ies have enrolled patients with mild to moderate Alzhei-
interventions (478); nevertheless, there is anecdotal and mers disease (MMSE scores in the 1026 range), although
common sense support for their inclusion as part of the at least two have focused on patients with moderate to se-
humane care of patients with dementia. vere dementia (MMSE scores in the 517 range) (107,
142), and one focused exclusively on patients with early
Alzheimers disease with MMSE scores in the 2126
B. SOMATIC TREATMENTS range (146, 480).
Published studies consistently have found a benet of
1. Treatments for Cognitive and Functional Losses donepezil over placebo in both cognitive and functional
a. Cholinesterase Inhibitors measures, including measures of clinicians impressions of
improvement. The size of the effect of donepezil has like-
1. Alzheimers disease wise been consistent across most studies, with improve-
a. Tacrine ment over placebo of about 1 point on the MMSE and 3
The efcacy of tacrine in mild to moderate Alzheimers points on the ADAS-cog. On cessation of donepezil, im-
disease has been extensively studied, although its effects provement was lost over a 36-week period in all studies
on patients with more severe or very mild Alzheimers dis- that examined this outcome. In one study in which done-
ease or with other forms of dementia have not been as- pezil treatment was interrupted for 6 weeks and then re-
sessed. At least ve double-blind placebo-controlled trials instated at the original dose, patients cognition and
with parallel-group comparisons including a total of more function did not return to the level achieved prior to
than 2,000 patients have been reported (131135). Over- donepezil discontinuation (166). Most studies comparing
all, these clinical trials consistently demonstrated differ- 5 mg/day dosing with 10 mg/day found greater benet
ences between tacrine and placebo. Approximately 30% with the higher dosage (138, 140), although this result has
40% of patients taking tacrine who completed the trials not been found in some studies comparing these dosages
showed modest improvements in cognitive and functional (141). Donepezil is administered once daily.
measures over study periods ranging from 6 to 30 weeks, The question of whether donepezil treatment delays
compared to up to 10% of those taking placebo. Modest nursing home placement is an important one and has been
improvement in these studies corresponded to maintain- addressed in two studies. One study found a delay in nurs-
ing or improving function by an amount typically lost ing home placement in patients treated with open-label
over 6 months in untreated groups of similar patients with donepezil for up to 240 weeks (481). However, these nd-
Alzheimers disease. Response appeared to be related to ings have been contested on methodological grounds
dose, at least in the largest clinical trial (133), in which pa- (482). The AD2000 trial conducted in the United King-
tients who could tolerate 120160 mg/day were more dom followed 565 community-dwelling patients randomly
likely to respond. However, only approximately 60% of assigned to receive donepezil or placebo for more than 2
the patients were able to complete the tacrine trials even years (136). Although donepezil-treated patients had bet-
at moderate doses; 30% of the subjects were dropped ter cognitive and activities of daily living scores than the
from these trials prior to completion because of elevation placebo group, there was no difference in the primary end-
in hepatic transaminases, and another 10% had to leave point of time to institutionalization. However, the trial was
because of other adverse effects, mainly cholinergic ef- underpowered, had a high dropout rate, and may have
fects (e.g., nausea and vomiting). The benets and adverse been inuenced by treatment interruptions (483).
effects of administration beyond 30 weeks are unknown.
c. Rivastigmine
b. Donepezil The efcacy of rivastigmine has been evaluated in at least
The efcacy of donepezil has been evaluated in more than eight randomized, placebo-controlled, double-blind stud-
15 randomized, double-blind, placebo-controlled trials ies of patients with Alzheimers disease (147152). The
(136146). Trial sizes have varied from fewer than 20 sub- sizes of the studies have varied from 50 subjects (148) to as
jects to 818 subjects (138), and many trials have been mul- many as 725 subjects (149). The duration of most trials was
26 weeks or shorter, although one trial lasted 12 months Of concern, in one unpublished trial of donepezil for
(150). All trials thus far have been conducted with com- vascular dementia, there was a signicantly higher rate of
munity-dwelling patients with mild to moderate dementia death in the subjects taking donepezil than in the placebo
severity (480). group (167), raising a signicant safety concern that re-
These studies consistently have found a benet of ri- quires further study.
vastigmine over placebo on both cognitive and functional
measures, including measures of clinicians impressions of 3. Dementia with Lewy bodies
improvement. The size of the effect of rivastigmine has One 20-week, randomized, double-blind, placebo-controlled
likewise been consistent across most studies, with im- study with 120 subjects examined the effects on cognition of
provement over placebo of about 1 point on the MMSE 612 mg/day of rivastigmine in patients with Lewy body
and 3 points on the ADAS-cog, a magnitude of effect sim- dementia (168). The results showed overall cognitive ben-
ilar to that of donepezil. The dosage range found to have ets with rivastigmine, compared with placebo, although
maximum efcacy is 612 mg/day in divided doses. differences were not statistically signicant for all mea-
sures. A small 4-week, placebo-controlled, double-blind,
d. Galantamine double-crossover, randomized trial of donepezil also
The efcacy of galantamine has been evaluated in at least demonstrated cognitive benets in subjects with Lewy
eight randomized, placebo-controlled, double-blind body dementia (169).
studies (153159). The numbers of subjects have ranged
from under 100 to 978 (157). Duration of most trials was 4. Parkinsons disease dementia
one-half year or shorter. All trials thus far have been con- In a 24-week, randomized, double-blind, placebo-controlled
ducted with community-dwelling patients with mild to study with 541 subjects, the effects on cognition and func-
moderate Alzheimers disease (480). tion of 312 mg/day of rivastigmine were examined in pa-
These studies consistently have found a benet of gal- tients with mild to moderate Parkinsons disease dementia
antamine over placebo in both cognitive and functional (170). Improved cognition and function were found in the
measures, including measures of clinicians impressions of rivastigmine group, compared with the placebo group, and
improvement. The size of the effect of galantamine has rivastigmine was tolerated by this patient population. In a
likewise been consistent across most studies, with im- 48-week open-label active treatment (312 mg/day of ri-
provement over placebo of about 1 point on the MMSE vastigmine) extension study that included 334 subjects
and 3 points on the ADAS-cog, a magnitude of effect sim- who completed the above-mentioned 24-week study, cog-
ilar to that of donepezil. The dosage range found to have nitive and functional benets appeared to continue over
maximum efcacy is 1624 mg/day in divided doses. An time (171). Patients treated with placebo in the initial
extended release, once-daily dosing form of galantamine study who were then treated with rivastigmine in the
has recently been released. open-label study had improvements in cognitive and
functional scores similar to those of the patients who re-
2. Vascular dementia ceived rivastigmine in the initial study.
A number of randomized, double-blind, placebo-controlled
trials have been conducted in patients with vascular de- 5. Mild cognitive impairment
mentia or mixed Alzheimers disease and vascular de- Two randomized, double-blind, placebo-controlled stud-
mentia. In two 24-week trials conducted with patients ies have investigated donepezil for the treatment of mild
with probable or possible vascular dementia (616 subjects cognitive impairment, neither of which demonstrated
and 603 subjects, respectively), donepezil (5 mg/day and benet in the primary study outcomes. In one study of 270
10 mg/day) was compared to placebo (484, 485). Im- subjects, there was no benet of donepezil on most (but
provements in measures of cognition and function were not all) cognitive tests studied, including the primary ef-
found in patients given either dose of donepezil, al- cacy measures (172). The second study included 769 sub-
though in one of the trials (484) one of the two primary jects with mild cognitive impairment and used a primary
outcome measures did not demonstrate benet of done- endpoint of progression from mild cognitive impairment
pezil, compared with placebo. The effect size was com- to meeting the criteria for the diagnosis of possible or
parable to that found in Alzheimers disease trials. Two probable Alzheimers disease over a 3-year period (173).
6-month trials of galantamine (592 and 786 subjects, re- Although fewer donepezil-treated subjects had pro-
spectively) in patients with vascular dementia or mixed gressed to Alzheimers disease in the rst year of the study,
Alzheimers disease and vascular dementia had similar compared to placebo-treated subjects, there was no differ-
ndings (358, 486). ence between the groups by the end of 3 years. Donepezil-
treated subjects did better than the placebo group on a pezil, random assignment to treatment with memantine
number of cognitive tests, but this modest difference did led to improvement in cognition and function, compared
not persist beyond 18 months. to random assignment to the placebo group (175). One
There have been two randomized, placebo-controlled, unpublished study did not show any benet of memantine
clinical trials of galantamine in subjects with mild cogni- over placebo (487). In a trial that included 166 subjects
tive impairment. Each study was of 2 years duration and with severe dementia due to Alzheimers disease or vascu-
included approximately 1,000 patients. Overall, there lar dementia, cognitive and functional improvement was
were no statistically signicant benets for galantamine greater with memantine than with placebo (180).
compared to placebo, either in increasing the time to the In summary, there is evidence supporting the use of
onset of dementia or improving cognitive function, activ- memantine for moderate to severe Alzheimers disease,
ities of daily living, or global assessment ratings. Of con- and memantine is approved by the FDA for this use. Data
cern in these two trials together, 13 subjects who were are not yet available to argue for or against the use of me-
taking galantamine died, compared to one subject who re- mantine beyond 6 months (108, 176).
ceived placebo. This nding was statistically signicant
2. Vascular dementia
and represents a precaution in the use of galantamine in
There have been two large 6-month clinical trials (with
this patient population. It is noteworthy that the rates of
579 and 321 subjects, respectively) of memantine to treat
death in these two trials were much lower in both the pla-
patients with mild to moderate vascular dementia (178,
cebo and the galantamine groups than would have been
179). In both trials, cognition and behavior improved, but
expected based on previously conducted clinical trials in
there was no demonstrated functional improvement and
patients with actual dementia. As in trials of cholinester-
no improvement on clinical global ratings of change (Cli-
ase inhibitors for Alzheimers disease subjects, there were
nicians Interview-Based Impression of Change Plus). No
substantial dropouts due to adverse events in the trials for
studies of memantine have been conducted with patients
subjects with mild cognitive impairment.
with severe vascular dementia alone. Nonetheless, in one
b. Memantine randomized placebo-controlled trial that included 166
patients with severe dementia, of which 51% had vascular
1. Alzheimers disease dementia and 49% had Alzheimers disease, there was im-
Memantine, a noncompetitive NMDA antagonist, has provement in cognitive and functional outcome measures
been studied extensively in recent years for the treatment for both the Alzheimers disease and vascular dementia
of Alzheimers disease and vascular dementia. Trials have subjects (180).
ranged from 6 weeks to 6 months in duration and have
primarily included outpatients, although one study in- c. Vitamin E
cluded nursing home residents (180). Studies have en- There has been considerable interest in vitamin E (-
rolled patients with moderate to severe dementia (MMSE tocopherol) as a treatment for Alzheimers disease and other
scores ranging from 3 to 15) as well as mild to moderate dementias because of its antioxidant properties and efcacy
dementia (MMSE scores ranging from 10 to 24). in Parkinsons disease. Vitamin E has been shown to slow
Among randomized placebo-controlled trials that have nerve cell damage and delay death in animal models and cell
included patients with mild to moderate Alzheimers dis- cultures (including damage associated with amyloid deposi-
ease, two unpublished trials did not nd benet of meman- tion) and thus may be relevant to the development and pro-
tine over placebo (487), whereas one trial demonstrated gression of Alzheimers disease (183, 488490).
cognitive and functional improvement with memantine, One large clinical trial of vitamin E for treatment of
compared to placebo (177). A meta-analysis of these three Alzheimers disease has been conducted (183). This pla-
trials showed a statistically signicant but very small advan- cebo-controlled, double-blind, multicenter trial included
tage to memantine over placebo (108). Nonetheless, the 341 subjects with moderate Alzheimers disease (CDR of
FDA has not approved the use of memantine for treatment 2) who were randomly assigned to receive 1,000 IU b.i.d.
of mild Alzheimers disease. of vitamin E alone, 5 mg b.i.d. of selegiline alone, both
Among studies of patients with moderate to severe Alz- agents, or placebo. Vitamin E alone, selegiline alone, and
heimers disease, two published trials (with 252 and 404 the combination each delayed reaching the study endpoints
subjects, respectively) (174, 175) found cognitive and (dened as a poor outcome, namely death, institutionaliza-
functional improvement with memantine, compared with tion, or signicant functional decline). The benet ob-
placebo. In one of those studies, which included only pa- served was equivalent to a delay of approximately 57
tients who were already taking stable dosages of done- months in reaching the composite endpoint. It is note-
worthy that no evidence was found for improvement in naproxen, and diclofenac) did not show benet over pla-
function or cognition, compared to baseline. Despite the cebo in slowing the cognitive decline in Alzheimers dis-
evidence for a better functional outcome in the treatment ease (190192). Moreover, several studies have suggested
groups, compared to the placebo group, all groups cardiac toxicity, especially with more selective cyclooxy-
showed similar rates of cognitive decline during the 2- genase-2 inhibitors. Finally, use of aspirin and NSAIDs
year study period. There are no studies of the effects of vi- can be associated with other signicant adverse events
tamin E in subjects with Alzheimers disease with mild or such as gastrointestinal bleeding and impairment of renal
severe impairment or in subjects with other dementias. function. Thus, NSAIDs are not recommended for the
There are also no data concerning the effect of vitamin E treatment of Alzheimers disease.
in combination with medications other than selegiline. Hormone replacement therapy is known to affect cog-
In one clinical trial, the effects of donepezil, vitamin E, nitive function (492) and was shown to be benecial in the
and placebo were compared in patients with mild cogni- treatment of dementia in at least two case series (493,
tive impairment (173). These patients were followed for 3 494). It was also associated with later onset and/or de-
years. Overall, no differences were found between vitamin creased risk of cognitive decline in at least two observa-
E (2,000 IU/day) and placebo on measures of cognition, tional studies of postmenopausal women (495, 496). In
level of function, or progression to dementia. contrast, in the prospective Womens Health Initiative
Although vitamin E has been widely used clinically and Memory Study (WHIMS), increased rates of conversion
in numerous clinical trials for a variety of indications and to Alzheimers disease were found in women age 65 years
has been considered to have low toxicity, more recent ev- or older who were randomly assigned to receive an estro-
idence suggests that vitamin E may be associated with a gen/progestin combination compared with those who re-
small but signicantly increased risk for morbidity and ceived placebo (193). Results of a number of other
possibly even mortality. At high doses, it may worsen prospective trials also showed no benet of estrogen over
blood coagulation defects in patients with vitamin K de- placebo in the treatment of cognitive symptoms of Alzhei-
ciency (184). Of greater concern is evidence linking vita- mers disease (194, 195). Therefore, hormone replacement
min E usage in clinical trials to increased mortality in a therapy is not recommended for use in the treatment of
dose-dependent fashion. A meta-analysis of 11 clinical tri- cognitive symptoms of Alzheimers disease.
als of vitamin E in a mixed population that included some There is also interest in the hormone melatonin and in
individuals with signicant cardiac disease found a very botanical agents such as ginkgo biloba, which are available
small but statistically signicant increase in mortality in without a prescription. There are no data supporting the
trials using doses greater than 400 IU/day and a dose- use of most of these agents in Alzheimers disease. Nu-
dependent increase in mortality with doses above 150 merous clinical trials of ginkgo biloba have been con-
IU/day (181). In addition, a carefully conducted large, ducted. Most of these have been small trials with
randomized clinical trial of vitamin E (400 IU/day) for the considerable methodological problems (497). In one
prevention of heart disease or cancer in patients with dia- randomized placebo-controlled trial that included 309
betes mellitus and/or vascular disease had an unanticipated subjects, 1-year efcacy of ginkgo was found in subjects
nding that vitamin E was associated with an increased risk with Alzheimers disease or vascular dementia, but there
of heart failure (182). were signicant methodological problems with the trial,
including a very high dropout rate (498). In a large, 26-
d. Other Agents week, randomized, double-blind, placebo-controlled trial
A number of medications marketed for other indications that included 513 subjects with mild to moderate Alzhei-
have been proposed for the treatment of dementia on the mers disease (MMSE score of 1024), the effects of 120
basis of epidemiological data or pilot studies. Aspirin and mg/day of ginkgo, 240 mg/day of ginkgo, and placebo
other NSAIDs have been proposed because of epidemi- were compared (196). There was no advantage to ginkgo
ological data suggesting that they protect against the de- over placebo for cognitive function, but these results are
velopment of dementia (185189) and because of qualied by the fact that there was very little cognitive de-
hypotheses regarding the involvement of inammatory cline in the placebo group as well. At this point, the pre-
mechanisms in the pathogenesis of Alzheimers disease ponderance of the evidence does not support the routine
(491). In a single small treatment trial for patients with use of ginkgo for the treatment of dementia (197, 198).
Alzheimers disease, patients receiving 100150 mg/day The chelating agent desferrioxamine has also been
of indomethacin experienced less decline over 6 months studied as a possible treatment for Alzheimers disease on
than did a matched control group (186). However, a num- the basis of hypotheses regarding heavy metals in the
ber of larger studies with other NSAIDs (rofecoxib, pathogenesis of the disease. In one small single-blind trial,
there was some evidence of a decrease in cognitive decline 1990 review (210) identied seven double-blind, placebo-
over 2 years (499). One study of another chelating agent controlled, randomized, parallel-group clinical trials in-
failed to conrm this nding (500). Because chelating cluding 252 patients studied over periods of 38 weeks
agents are quite toxic and support for them is so weak, (203209). Despite some methodological aws, notably
they are not recommended for the treatment of dementia. small numbers of subjects and a lack of diagnostic speci-
Newer agents that chelate copper and zinc are in clinical city, these studies, when taken together, constitute rea-
development as potential Alzheimers disease therapies sonable evidence for a modest improvement in target
because they may lower beta-amyloid burden (501). symptoms in some patients treated with rst-generation
As reviewed in a Cochrane meta-analysis that included antipsychotic medications. A meta-analysis of these seven
negative trials, the irreversible MAO-B inhibitor sele- trials (210), using clinician assessment of improvement in
giline has been studied in a large number of randomized a variety of behavioral symptoms as the primary outcome,
controlled clinical trials, with mixed results (199). One showed improvement in 59% of the subjects taking anti-
large trial comparing selegiline with vitamin E and pla- psychotics and 41% of those taking placebo. The studies
cebo demonstrated some benet of selegiline over pla- used a wide variety of dosages (ranging from 66 to 267
cebo (183), but numerous other trials have not shown mg/day in chlorpromazine equivalents), and efcacy for
clinically meaningful benet. Although use of selegiline at behavioral symptoms was not correlated with standard-
dosages of 510 mg/day is generally safe and well toler- ized dose. Adverse effects were common, but specic rates
ated, few clinicians actually use this medication in clinical are not available. Dropout rates were also high, whether
practice for the treatment of cognitive decline in dementia. associated with side effects or poor efcacy.
Selegiline use is considered contraindicated in combination In a more recent meta-analysis of studies of rst-
with meperidine, SSRIs, or tricyclic antidepressants. Use generation antipsychotics in patients with dementia, clini-
of the selegiline patch for treatment of dementia has not cally signicant improvement was found in 64% of patients
been studied. treated with active medication versus 38% of patients
A mixture of ergoloid mesylates is currently marketed treated with placebo, translating to an effect size of 26%
under the trade name Hydergine for the treatment of (211). No differences in efcacy were seen among the dif-
nonspecic cognitive impairment. It has been available ferent agents used. Signicant side effects were found in
for at least 40 years and has been studied in at least 150 25% more of the patients who received active treatment,
clinical trials, seven of which were double-blind, placebo- compared with those who received placebo. This meta-
controlled, randomized trials with a parallel-group design analysis did not include a number of more recent studies
involving a total of 297 patients with diagnoses consistent (212216); however, the data from these newer studies
with Alzheimers disease. Studies have been conducted in generally conformed to the results of the meta-analyses
patients with vascular dementia as well. Although a num- (210, 211). In another review of antipsychotics used in de-
ber of trials have produced weakly positive results, these mentia (217), which also included several trials of second-
have generally been on isolated cognitive measures or on generation antipsychotic agents, mean improvement rates
measures of psychiatric symptoms, and the overall evi- were 61% with antipsychotics and 35% with placebo,
dence suggests little or no effect (200). Side effects are yielding a treatment effect of 26%. The modest treatment
usually mild and affect the gastrointestinal system. Dos- effects estimated by these meta-analyses and reviews are
ages used in the studies ranged from 3 to 9 mg/day. generally consistent with results from placebo-controlled
trials of second-generation antipsychotics.
Second-generation antipsychotic agents have also been
2. Treatments for Psychosis and Agitation
studied in well-controlled trials in patients with dementia.
Because treatments for psychosis and behavioral distur-
Three placebo-controlled trials of risperidone have been
bances overlap to a considerable extent, and because in-
conducted among nursing home residents with severe de-
vestigations often include subjects with both groups of
mentia complicated by agitation and/or psychosis (212,
symptoms, they are grouped together in this discussion.
218). In the rst trial, a xed-dose study that included 625
patients, the response rates of 45% and 50% for 1 mg/day
a. Antipsychotics
and 2 mg/day, respectively, were signicantly different
1. Efficacy than placebo (33%) (the 0.5-mg/day dose was not more
First-generation antipsychotic medications (also known effective than placebo). Parkinsonism was seen in 21% of
as conventional or typical antipsychotic agents) have patients who received 2 mg/day, and it was concluded that
been extensively studied in the treatment of psychosis and 1 mg/day represented the most effective dose. In the sec-
agitation in individuals with dementia. For example, a ond trial, a exible-dose study that included 344 patients,
response rates were 47%, 63%, and 54%, respectively, for haloperidol was conducted in a group of elderly nursing
placebo, haloperidol (mean dosage 1.2 mg/day), and ris- home patients with operationally dened psychosis, crite-
peridone (mean dosage 1.1 mg/day); these response rates ria for which were implemented before the development
did not differ statistically. Secondary outcomes related to of the recently proposed clinical criteria for the psychosis
aggression decreased in the two active treatment groups, of Alzheimers disease (201). Results from the subgroup of
compared with the placebo group, but cognitive and func- 284 patients with Alzheimers disease were analyzed sepa-
tional outcomes were not different across treatment rately. In these subjects, the mean daily dosage of haloperi-
groups. In the third trial, the effects of exibly dosed ris- dol was 2 mg/day at endpoint, whereas that of quetiapine
peridone were compared to those of placebo in 337 nurs- was about 120 mg/day. Neither of the treatment groups
ing home patients with severe dementia who required differed with respect to reduction in measures of psycho-
treatment for aggression; a signicant difference in resis, the primary outcome of the trial. One secondary
sponse rates of 37% for placebo and 63% for risperidone measure of agitation showed improvement with both ha-
(mean dosage 1 mg/day) was found (219). loperidol and quetiapine treatment but not placebo.
Three clinical trials have been conducted to study the These studies led to a second placebo-controlled trial of
effects of oral olanzapine for the treatment of persisting 100 mg/day of quetiapine, achieved by day 4, or 200
agitation and/or psychosis in patients with severe demen- mg/day, achieved by day 8, in which the participants were
tia. The rst trial, reported only as an abstract, compared 333 nursing home residents with dementia (227). A dose
exibly dosed olanzapine (mean dosage of about 2.3 of quetiapine at 200 mg/day was superior to placebo on
mg/day) with placebo in 238 patients, and no difference in numerous outcomes, with less benet seen at 100 mg/day.
efcacy or tolerability was found. This negative result may A more critical review of the data will be possible once the
in part be explained by the mean dosages being too low trial results are published. A placebo-controlled trial of
(502). In the second trial, in which participants consisted of quetiapine in a group of 93 subjects with Alzheimers dis-
206 nursing home residents, response rates of 66%, 57%, ease and agitation failed to show any benet over placebo
and 43% were found with xed dosages of 5, 10, and 15 for the medication (506).
mg/day of olanzapine, respectively, versus 36% for pla- Three placebo-controlled studies of aripiprazole have
cebo (the response rates with 5 mg/day and 10 mg/day been published or presented in abstract form. In all three
were signicantly different from those with placebo) (220). studies, the primary outcomes were not reached, but sig-
Some patients from this trial received follow-up open- nicance on individual outcomes was shown. In a pla-
label, exible-dose treatment for 18 weeks; the results cebo-controlled trial that included 208 outpatients who
were consistent with the ndings of the original report met the clinical criteria for psychosis of Alzheimers dis-
(221). The third trial included 652 residents of nursing ease (201), there was no difference between exibly dosed
homes or continuing care hospitals who met the opera- aripiprazole (mean dosage of 10 mg/day) and placebo on
tional criteria for psychosis (222). Patients were assigned the primary outcome variable of psychosis, although post
to treatment with olanzapine at doses of 1, 2.5, 5, or 7.5 hoc analyses showed benets at some time points (224).
mg/day or placebo; no drug-placebo differences were seen The second study, with ndings presented in abstract
in measures of psychosis or other behavioral features. form, was a placebo-controlled study of xed-dose aripip-
Meehan et al. (223) studied acute treatment of agita- razole conducted with 587 nursing home residents with
tion with intramuscular olanzapine in a group of 272 in- dementia and psychotic features (507). A signicant effect
patients or nursing home residents with Alzheimers was found only for the 10-mg/day dose on the primary
disease and/or vascular dementia. Olanzapine at doses of outcome, a measure of psychosis, with 50% of patients
2.5 and 5.0 mg was found to be superior to placebo in who received placebo and approximately 68% who re-
treating agitation at 2 hours; the response rates were 62%, ceived 10 mg/day of aripiprazole considered to have re-
66.7%, and 37.3%, respectively. The response rate for sponded clinically. The third study, with ndings presented
those treated with intramuscular lorazepam was 72.1%; in abstract form, was a placebo-controlled exible-dose
all response rates for participants who received active study conducted with 256 nursing home residents with
treatment were different from those for participants who dementia and psychotic features (508). The results
received placebo group but not from each other. Adverse showed no drug-placebo difference in the primary out-
events were not signicantly different between groups. come with a mean aripiprazole dosage of 8.6 mg/day. A
Evidence for the use of quetiapine is limited to ndings fuller appreciation of these studies will be possible once
from three open-label trials that suggested possible bene- the results are published.
ts for agitation (503505). A 10-week, multicenter, pla- Clozapine has been found to be useful in controlling
cebo-controlled trial of exibly dosed quetiapine versus psychotic symptoms in patients with Parkinsons disease
(233) and dementia with Lewy bodies (234) and may also mentia beyond 812 weeks of follow-up, although these
be useful for patients with Alzheimers disease who are medications are often used for much longer periods of
sensitive to the extrapyramidal effects of rst-generation time in clinical practice. Extensive clinical experience has
antipsychotic agents (509). Currently no specic data are suggested that they are sometimes helpful for longer pe-
available on the use of ziprasidone in the treatment of el- riods of time. Several studies of the effects of withdrawal
derly patients. of treatment have suggested that a substantial proportion
A recent meta-analysis that included the randomized of patients can be withdrawn from treatment successfully
controlled trials described in preceding paragraphs after a period of time (40, 229).
showed that benets tended to be greater for symptoms
2. Side effects and toxicity
of agitation than for psychosis (225). These data also
demonstrate a signicant placebo response, a nding that a. Serious side effects
underscores the importance of nonpharmacological inter- Antipsychotic agents are associated with a risk of serious
ventions for relief of these signs and symptoms. The non- complications that must be considered in weighing the
specic aspects of clinical trial participation (e.g., risks and benets of antipsychotic treatment.
increased attention from staff), as well as the frequent Tardive dyskinesia, whose incidence increases with
clinical evaluations that occur during a clinical trial, may increasing dose and duration of treatment and which oc-
contribute to the improvement seen in patients in the pla- curs more commonly in women, is also more common in
cebo arm of a trial. Finally, much of the data discussed ear- individuals with dementia and in elderly patients in gen-
lier are from studies that have not been published yet, so eral. The risk may be as high as 30% for elderly patients
they will need to be reevaluated. with signicant exposure to rst-generation antipsychotic
The available studies comparing antipsychotics to one agents (510512). This risk may be considerably lower
another are of limited power but suggest no clinically sig- with the use of second-generation antipsychotics. For ex-
nicant differences in efcacy (40, 210, 212, 215, 225). ample, Jeste et al. (513) reported a cumulative incidence of
The rst direct comparison of second-generation antipsy- tardive dyskinesia of 2.6% in 330 patients with dementia
chotics with placebo in patients with Alzheimers demen- treated openly with risperidone (mean dosage of about
tia has been undertaken as part of the NIMH-funded 1 mg/day) for a median of 273 days. This gure is much
CATIE-AD (228). In this trial 421 outpatients with Alz- lower than that reported for older people treated with
heimers disease and psychosis and/or aggression were rst-generation antipsychotics (511) and is consistent
randomly assigned to treatment with olanzapine, quetia- with data reported in a recent prospective longitudinal
pine, risperidone, or placebo with dosages adjusted as study of risperidone and haloperidol in older subjects with
needed and followed for as long as 36 weeks. There were mixed psychiatric disorders (514). There are, however, no
no differences among treatments in the main outcome, placebo-controlled studies addressing this issue and no
time to all-cause discontinuation, with initial treatments studies employing withdrawal maneuvers. Clozapine is
maintained for about 8 weeks. Time to discontinuation the agent least associated with tardive dyskinesia, al-
due to lack of efcacy, however, favored olanzapine and though the rare occurrence of clozapine-induced tardive
risperidone, both of which were maintained for about 24 dyskinesia has been reported (515).
weeks, whereas quetiapine and placebo were maintained Neuroleptic malignant syndrome is a rare but po-
for approximately 9 weeks. Time to discontinuation due tentially lethal adverse effect of antipsychotic medica-
to adverse events or intolerability favored placebo, with tions. It occurs less frequently with second-generation
discontinuation in 24% of patients who received olanza- antipsychotic agents than with rst-generation agents,
pine, 16% of patients who received quetiapine, 18% of but it has been reported with both types (516520). The
patients who received risperidone, and 5% of patients core features of this syndrome are muscle rigidity (leading
who received placebo. Although there were no differences to elevated serum creatinine phosphokinase levels), fever,
in improvement as rated with the Clinical Global Impres- leukocytosis, tremor, delirium, autonomic instability, and
sion of Change (olanzapine 32%, quetiapine 26%, ris- diaphoresis. Older age and dementia may increase the risk
peridone 29%, placebo 21%), some symptom ratings of neuroleptic malignant syndrome.
favored the drugs over the rst 12 weeks. Adverse effects Clozapine is associated with risk of agranulocytosis
offset advantages in efcacy of second-generation anti- (about 1%), which is more common in elderly patients
psychotic drugs for treatment of psychosis, aggression, or than in younger patients (509), and regular monitoring of
agitation in patients with Alzheimers disease. blood counts is required. Other antipsychotics may rarely
It is important to note that there are limited data on the be associated with this adverse event, but its incidence is
efcacy of antipsychotic medications for patients with de- so infrequent that routine monitoring of blood counts for
this syndrome is not required for patients who take other Finally, a recent meta-analysis of randomized con-
antipsychotics. trolled clinical trials of second-generation antipsychotics
Metabolic abnormalities caused by second-generation in patients with dementia performed by Schneider et al.
antipsychotic medications are not well studied in individ- (525) compared mortality in the treatment and placebo
uals with dementia but may be more common with use of groups during the clinical trial period. In total, the meta-
these agents in older individuals (258). These metabolic analysis included 15 trials, three of aripiprazole, ve of
abnormalities include hyperlipidemia, weight gain, and olanzapine, three of quetiapine, and ve of risperidone.
diabetes mellitus (228). The subjects were nursing home residents in 11 of the
There is also evidence of an increased risk of cere- trials and outpatients in the remaining four trials; a total
brovascular adverse events with at least three of the of 3,353 subjects received medication and 1,757 received
second-generation antipsychotics (aripiprazole, olanza- placebo. When data from all the trials were pooled, the
pine, and risperidone) when used in the treatment of pa- odds ratio for death in subjects who received second-
tients with dementia. In October 2002, Health Canada generation antipsychotics was 1.54, compared to the pla-
issued a letter to health care professionals stating that ris- cebo group, with a 95% CI of 1.062.23. Although for no
peridone use may be associated with cerebrovascular individual medication or individual trial was the odds ratio
events in elderly patients with dementia (521). In April of death in the medication group statistically different
2003, the FDA issued a similar warning regarding risk of from that for the placebo group, for all medications and
cerebrovascular events with risperidone in patients with for 12 of the 15 trials the odds ratio favored placebo over
dementia and noted that risperidone had not yet been the medication.
shown to be safe or effective in treating dementia-related This nding has been underscored by the black box
psychosis (522). Pooled data from four placebo-controlled warning applied by the FDA on April 11, 2005, to all of
trials suggested a rate of cerebrovascular events (vari- the second-generation antipsychotics, stating that analy-
ably dened) of 4% in patients treated with risperidone, sis of 17 placebo-controlled trials of aripiprazole, olanza-
compared with about 2% in those treated with placebo. pine, quetiapine, or risperidone in patients with dementia
The available data suggest that the risk is greater among showed a death rate of about 4.5% in those receiving ac-
those with pre-existing risk factors for cerebrovascular tive treatment versus about 2.6% in those receiving pla-
disease. cebo. Causes of death were varied, with the most common
In January 2004, Eli Lilly and Company issued a warn- being cardiovascular (heart failure, sudden death) or in-
ing to prescribers that there was an increased incidence of fectious (pneumonia) in nature (231).
cerebrovascular adverse events in patients with dementia There is also evidence that rst-generation antipsy-
who were treated with olanzapine (1.3%) versus placebo chotics are similarly associated with increased mortality
(0.4%), as well as increased mortality (3.5% vs. 1.5%) among patients who take them and that this increased
(523). In February 2005, Bristol-Myers Squibb issued a mortality may exceed that found with second-generation
warning to prescribers that there was an increased risk of antipsychotics. In a large retrospective review of 22,890
cerebrovascular adverse events in patients with dementia patients over age 65 years in Pennsylvania who received
who were treated with aripiprazole (1.3% vs. 0.6% in either rst- or second-generation antipsychotic agents
those given placebo). between 1994 and 2003, Wang et al. (230) found a 1.37
At present no warning has been issued regarding que- relative risk (CI, 1.271.49) of death among users of rst-
tiapine and increased risk of cerebrovascular events. generation agents versus users of second-generation
Schneider et al. (225, 524) reported an event rate of 0.8% agents. The risk was highest with higher doses and closer
for quetiapine and 1.9% for placebo among placebo- to the initiation of treatment. The increased risk was in-
controlled studies of quetiapine in the dementia popula- dependent of the presence of dementia and of residence
tion. They also noted that the 95% condence intervals (nursing home versus community). The magnitude of this
(CIs) for the relative risks for risperidone, olanzapine, and difference was such that the authors concluded that for
aripiprazole all indicated increased risk for such events, every 100 patients treated with rst-generation antipsy-
whereas the CI for quetiapine could not distinguish chotics instead of second-generation agents, there would
among increased risk, decreased risk, or no risk. It is pos- be seven additional deaths. At this time, there is no FDA
sible that patients with existing cerebrovascular disease or black box warning on rst-generation antipsychotics.
other risk factors might be most susceptible to these Clinicians facing the challenge of treating patients
events. However, this possibility has yet to be denitively with signicant psychosis or behavioral disturbances
addressed with studies designed to assess side effects or ef- must weigh the risk of not treating these complications of
cacy as a function of baseline medical condition. dementia against the risks of active treatment described
in this section. Clinicians must take into account the ev- age of 0.95 mg/day) and 16% among subjects who received
idence supporting the efcacy of the agent in question, placebo. These results are similar to those from a smaller
the morbidity and risk associated with the target symp- study by Chan et al. (215) in which risperidone and halo-
toms, the patients general medical condition, and the ev- peridol were compared and are also consistent with the re-
idence of risk and benet of any alternative treatment sults of a large meta-analysis of randomized controlled
being considered. trials of risperidone, which found an overall odds ratio for
extrapyramidal signs and symptoms of 1.80 (CI, 1.352.42)
b. Mild to moderate side effects for risperidone versus placebo (225). These studies also
In addition to their association with the serious side ef- showed a greater risk of sedation. In the trial of De Deyn et
fects described in Section V.B.2.a.2.a, antipsychotic med- al. (212), sedation affected 12% of patients taking risperi-
ications are associated with numerous more common but done but only 4.4% of those who received placebo, a nding
milder side effects. also conrmed by the meta-analysis (odds ratio, 2.43; CI,
First-generation antipsychotic agents have a broad 1.783.32). In the meta-analysis, a higher rate of peripheral
range of common side effects that vary with medication edema was found in patients treated with risperidone, com-
potency, although any side effect can be seen with any pared to those who received placebo (225). Risperidone may
agent. Reviews regarding rst-generation agents have also cause an abnormal gait in some patients (225).
cited side effects including akathisia, parkinsonism, seda- For olanzapine, side effect information is primarily
tion, peripheral and central anticholinergic effects, pos- available from the one randomized controlled trial that
tural hypotension, cardiac conduction defects, and falls demonstrated clear clinical efcacy (220); in one other
(211). Most of these data come from short-term controlled clinical trial, the doses used were not sufcient to help or
trials; evidence regarding long-term safety is generally harm or to provide meaningful information about side ef-
lacking. Data available from other studies in the elderly fects (502), and in the other trial specic characteristics
population, however, indicate that caution is warranted. were not described for the side effects that occurred (222).
For instance, rates of tardive dyskinesia are ve- to sixfold In the one trial with side effect information, sedation (at
greater in older than in younger populations after long- rates of 25%36%) and abnormal gait (at rates of 14%
term treatment with rst-generation agents (511). For 20%) were observed at all dosages used (515 mg/day).
practical purposes, side effects often guide selection of Results of the meta-analysis of randomized controlled tri-
these agents when used in patients with dementia. High- als of olanzapine showed substantially increased risk with
potency agents (e.g., haloperidol, uphenazine) are most the medication, compared to placebo, of sedation (odds
strongly associated with akathisia (which can worsen the ratio, 4.00; CI, 2.277.04) and urinary tract infections or
target symptoms) and parkinsonian symptoms. Low- incontinence (odds ratio, 6.69; CI, 1.2735.10) (225).
potency agents (e.g., thioridazine, chlorpromazine) are as- Gait abnormalities also developed in more subjects taking
sociated with sedation (which can lead to worsening cog- olanzapine than in those who received placebo (225).
nition or falls), central anticholinergic effects (e.g., In the one trial comparing quetiapine to haloperidol,
confusion, delirium), postural hypotension (which can also tolerability of quetiapine was superior, with comparable
lead to falls), and a variety of peripheral anticholinergic ef- effects on a simple measure of agitation (527). Several
fects (e.g., dry mouth, constipation, bladder dysfunction, measures of parkinsonism showed worsening with halo-
tachycardia). When individuals with dementia have co- peridol but no difference between quetiapine and placebo
occurring extrapyramidal disorders (as in dementia with (527). Sedation was seen in 4.1% of patients who received
Lewy bodies), extraordinary sensitivity to rst-generation placebo versus 25.3% and 36.2% of those who received
antipsychotic agents may be seen (526). quetiapine and haloperidol, respectively. In the subse-
Risperidone treatment of patients with dementia is asso- quent trial in which the most efcacious dosage of que-
ciated with a low to moderate risk of dose-related parkin- tiapine was 200 mg/day, sedation occurred in 17.6% of
sonism. In the large trial by Katz et al. (218), the rates of patients taking 200 mg/day, compared with 11.3% of
parkinsonism were 21%, 13%, and 7% among patients who those taking 100 mg/day and 6.5% of those who received
received 2 mg/day of risperidone, 1 mg/day of risperidone, placebo (227). A recent meta-analysis of randomized con-
and placebo, respectively. In the trial of De Deyn et al. trolled trials of quetiapine similarly found an odds ratio
(212), the incidence of parkinsonism was 15% for subjects for sedation of 3.90 (CI, 1.4110.78) for quetiapine versus
who received risperidone at a mean endpoint dosage of placebo (225).
1.1 mg/day and 11% for subjects who received placebo. Aripiprazole treatment of patients with dementia is
Brodaty et al. (219) found an incidence of parkinsonism of commonly associated with sedation, occurring in 5%
23% among subjects who received risperidone (mean dos- 15% of those treated versus 1% of those receiving placebo.
In the one published randomized controlled trial, 8% of 533), four placebo-controlled trials have not demonstrated
aripiprazole-treated subjects but only 1% of placebo- efcacy. In a 6-week, randomized, placebo-controlled trial
treated subjects experienced sedation (224). This nding that included 172 nursing home residents with Alzheimers
was conrmed in a recent meta-analysis that focused on disease and secondary mania, subjects treated with dival-
adverse events (225). Regarding ziprasidone in the treat- proex sodium had no more improvement in symptoms of
ment of patients with dementia, there are insufcient data mania than did subjects treated with placebo (253). In an-
to make assertions regarding safety and tolerability. other randomized placebo-controlled study conducted
Most short-term side effects can be minimized by us- with 42 patients with Alzheimers disease and behavioral
ing the lowest effective dose. This principle is particularly disturbances, valproic acid (dosage of 480 mg/day) was not
important in order to minimize sedation and akathisia, more effective than placebo in reducing overall agitation,
both of which can actually worsen target symptoms (528). although in secondary analyses certain individual symp-
It may also be helpful to select an agent with the side effect toms were improved (254). However, because these results
prole most suited to a given patient. Anticholinergic were derived from an analysis of secondary outcomes, they
agents may be effective in the treatment of parkinsonian are not sufcient to dene practice. In another 6-week,
side effects, but the high risk of associated cognitive de- randomized, placebo-controlled trial that included 56
cline, delirium, and other anticholinergic effects suggests nursing home residents with dementia and behavioral
that they should be used only with extreme caution for el- disturbance, results were suggestive of benet with dival-
derly patients both with and without dementia. proex sodium; 68% of the treatment group had improve-
ment in agitation, compared with 52% of the control
b. Benzodiazepines group (256). The largest study, which prospectively ad-
The use of benzodiazepines in the treatment of behavioral dressed agitation as the primary outcome in 153 nursing
symptoms in dementia has been studied in at least eight ran- home residents with Alzheimers disease, found no differ-
domized clinical trials. In six studies including a total of 873 ence between divalproex sodium (mean dosage of 800
subjects, benzodiazepines were compared to antipsychotics mg/day) and placebo in either the primary outcome (agi-
administered orally (238243). In two studies, benzodiaze- tation) or secondary outcome measures (255).
pines were compared to placebo (529, 530). Most of these There are no controlled trials of newer anticonvulsants
studies were limited by the presence of poorly specied di- such as lamotrigine, gabapentin, and topiramate. The few
agnoses, a mixture of target symptoms, limited outcome case reports and case series that suggest benet with gaba-
measures, and, in most cases, high doses of long-acting pentin (e.g., reference 534) do not provide sufcient evi-
agents. Nonetheless, they demonstrated that benzodiaze- dence to recommend their use.
pines perform better than placebo but not as well as anti-
psychotics in reducing behavior problems. These results are d. Other Agents
supported by a more recent randomized controlled trial of A number of other agents have been proposed for the
comparing intramuscular lorazepam with intramuscular treatment of agitation in patients with dementia (reviewed
olanzapine, which showed equal efcacy of lorazepam and in references 210, 535, 536). Efcacy data for these agents
olanzapine at 2 hours but inferior efcacy of lorazepam at generally come from case reports or small open trials, of-
24 hours (223). There are no data concerning the efcacy of ten of mixed populations.
benzodiazepines after 8 weeks or whether one benzodiaze- For example, data on trazodone are primarily from case
pine is more effective than another. reports, case series (260, 261), and a few small trials (262)
in which decreased irritability, anxiety, restlessness, and
c. Anticonvulsants affective disturbance was reported in a total of 13 patients.
Use of carbamazepine has support from several case series In a small double-blind, randomized clinical trial that was
(248), a small open trial (249), a double-blind nonrandom- not placebo controlled, improvement in agitation with tra-
ized trial (250a), and two double-blind randomized trials zodone was comparable to that seen with haloperidol
(250b, 250c) that showed modest benet for agitation at (263). However, in the largest and only placebo-controlled
low doses, with low side-effect rates over a short treatment trial, which included 37 patients receiving trazodone, no
period. One of these trials was followed by an open-label benet of trazodone, compared to placebo, was found
extension that further supported efcacy, safety, and toler- (214). A small randomized, placebo-controlled, double-
ability (251). One small randomized crossover trial showed blind study of trazodone in patients with frontotemporal
nonsignicant decreases in behavioral measures (252). dementia showed benet over placebo (264).
Although several favorable case reports and open trials Preliminary data suggest that SSRIs may be useful in
have been reported for the anticonvulsant valproate (531 the treatment of agitation (262, 270). These preliminary
reports are supported by two case series and a small con- with placebo. Selective serotonin reuptake inhibitors ap-
trolled trial showing benet of a variety of SSRIs for re- pear to be the most promising for treating depression in
duction of agitation in patients with frontotemporal patients with dementia, with sertraline having superior ef-
dementia (537539), although one trial of paroxetine in ficacy, compared with placebo (292) and citalopram im-
patients with frontotemporal dementia did not demon- proving affective symptoms in one study of patients with
strate improvement in symptoms but did show worsen- dementia (289). The cyclic antidepressants, however,
ing of cognition (540). A rigorous placebo-controlled were either no more effective than placebo or produced
trial examined the short-term benet of citalopram ver- signicant side effects. Head-to-head comparisons of
sus perphenazine in inpatients with agitation or psy- SSRIs to cyclic antidepressants and a SSRI (sertraline) to a
chotic features (271). Double-blind treatment lasted no serotonin-norepinephrine reuptake inhibitor (venlafax-
more than 3 weeks. Although both perphenazine and cit- ine) showed equal efcacy in treating depression but bet-
alopram, compared to placebo, produced clinical im- ter tolerability of SSRIs over cyclic antidepressants (297
provement on general measures of behavior, improvement 299).
in agitation and aggression specically was seen only Although clinical trials support the efcacy of antide-
with citalopram. Patients taking citalopram had few side pressants in the treatment of depressed elderly patients
effects. without dementia (285), extrapolating these data to pa-
The effects of buspirone for treatment of agitation or tients with co-occurring dementia should be done cau-
anxiety in elderly patients with dementia have been re- tiously. The reader is referred to APAs Practice Guideline
ported in a number of case reports (265267) and assessed for the Treatment of Patients With Major Depressive Disorder,
in two open trials (268, 269). These limited data are insuf- 2nd edition (284) for a summary of this literature.
cient to establish efcacy. Data concerning the treatment of other affective symp-
A 6-week, randomized, double-blind, placebo-controlled toms such as apathy are much sparser. There is minimal ev-
trial of propranolol that included 31 subjects with Alzhei- idence that dopaminergic agents, such as psychostimulants
mers disease and behavioral disturbance who resided in (d-amphetamine, methylphenidate), amantadine, bromo-
nursing homes showed benet of the medication, com- criptine, and bupropion, are helpful in the treatment of
pared with placebo, for certain symptoms, although it was severe apathy, but case reports have suggested that ef-
noted that use of beta-blockers was contraindicated for cacy studies are warranted (301, 302). Psychostimulants
many subjects who would otherwise have been eligible for have also received some support for the treatment of de-
the study (277). The mean dose was 106 mg/day. The pression in elderly individuals with severe general medical
benets noted in the 6-week trial were lost to a great ex- disorders (303305).
tent over the ensuing 6 months of open-label treatment.
b. Electroconvulsive Therapy
The data supporting the efcacy and safety of ECT in the
3. Treatments for Depression and Related Symptoms
treatment of depression in dementia are limited to the re-
a. Antidepressants sults of one small retrospective chart review (306). Several
Over the last 15 years, eight placebo-controlled studies larger, prospective studies have supported the efcacy of
have examined the efcacy of antidepressants in patients ECT in the acute treatment of geriatric depression (307,
with dementia. Four trials were conducted with SSRIs, 308).
one with citalopram, one with uoxetine, and two with
sertraline (289292). Three trials assessed cyclic antide- 4. Treatments for Sleep Disturbance
pressants (imipramine, maprotiline, and clomipramine) The available data do not suggest a specic course of action
(293295), and one trial examined an MAOI (moclobe- for treating sleep disturbances in patients with dementia.
mide) (296). The available evidence is mixed for the ef- Several small trials of bright light therapy exist, but they
cacy of these medications for the treatment of depression have not shown effectiveness in improving sleep problems
in patients with dementia, with some trials demonstrating and their associated behavioral and mood disturbances
superiority over placebo and others failing to show differ- (315, 318322). In one small study, improvement in MMSE
ences in efcacy. Among the explanations for the variabil- scores (3 points) was reported with bright light therapy
ity in trial results are differences in patient selection (320). In another small study, patients with vascular demen-
criteria and differences in the sensitivity of the rating tia, but not patients with Alzheimers disease, had a decrease
scales used in the various trials (541). Studies that have in nighttime activity with bright light therapy (318). How-
used the most restrictive criteria for depression generally ever, four randomized controlled trials of bright light ther-
reported better response to active treatment, compared apy have failed to show increases in nocturnal sleep time or
decreases in nighttime activity, sleep latency time, agitation, time napping, daily exercise) resulted in improved sleep,
or depression (315, 318, 319, 321, 322, 542). better maintenance of a consistent bedtime and rising
Behavioral interventions and pharmacological agents time, fewer naps during the day, and more physical ac-
are often utilized to address the sleep problems of pa- tivity in the form of walking (317). Likewise, only a few
tients with dementia. In one study, nocturnal sleep was pharmacological agents used to treat sleep problems
improved by targeting daytime activities of nursing have been rigorously studied in this population. Al-
home residents during periods when they were most though 3 mg of melatonin at bedtime was found to pro-
likely to nap (543). In another study, caregiver education long sleep and decrease nighttime activity in a small
and improved sleep hygiene were found to improve sleep sample (544), a randomized controlled trial that in-
quality in patients with dementia (316). A sleep hygiene cluded 157 individuals showed no benet of 10 mg of
behavioral intervention for patients with dementia was melatonin or 2.5 mg of slow-release melatonin, com-
evaluated in a small trial (317). In this study, training for pared with placebo (545). Galantamine, an acetylcho-
caregivers in how to implement proper sleep hygiene linesterase inhibitor, did not improve sleep quality in
principles (e.g., consistent rising times, minimizing day- patients with dementia (546).
Part C
FUTURE RESEARCH NEEDS
A review of currently available treatments suggests a num- include neuroprotective strategies, neurotropic approaches
ber of areas for further study. Several of these are in the such as use of nerve cell growth factors and cell transplants,
realm of evaluation and assessment. Better detection and and use of antioxidants (548, 549). In addition, medications
evaluation of dementia, especially in the prodromal and that directly enhance cognition by activating intact cogni-
early stages, will be particularly important if treatments are tive systems might improve performance and function. As
developed that slow progression. Identication of specic the understanding of other dementing disorders advances,
biomarkers and renements in imaging techniques may fa- targeted therapies must be developed and tested for these
cilitate diagnosis and treatment planning as well as provide illnesses as well. Efforts to prevent stroke and to decrease its
insight into categorization of dementia syndromes (13, destructive effect on brain tissue are particularly important
14). Earlier and more accurate detection of noncognitive avenues for dementia prevention (550, 551).
symptoms may facilitate optimal intervention. Another arena is the optimal pharmacological treat-
More accurate assessments of potentially dangerous be- ment of behavioral and neuropsychiatric symptoms, in-
haviors such as driving are needed (54, 61). The develop- cluding psychosis, agitation, depression, and sleep
ment of more clinically meaningful outcome measures and disturbance (225, 552). Many current recommendations
more rened neuropsychological tests, the development of are extrapolated from small uncontrolled studies of agents
functional assessments, and wider use of hard endpoints, no longer in common use and/or at doses well above those
such as institutionalization and mortality, would allow for used in current practice. There is a critical need for well-
more condence in making treatment recommendations. designed, randomized, controlled trials of potential treat-
In the realm of pharmacological treatments, there is a ments for these neuropsychiatric symptoms.
critical need for medications with greater ability to improve Further research into psychosocial, psychotherapeutic,
cognition or halt the progression of dementia (547). and behavioral interventions is also needed (116). Random-
Among the leads being actively studied are agents that pre- ized controlled trials or alternative methods that apply ran-
vent plaque deposition, inhibit beta and gamma secretase, domized controlled trial methods to the study of behavioral
remove plaque and insoluble amyloid fragments, and pre- interventions are of particular importance. One aspect of
vent the formation of and remove neurobrillary tangles dementia care that deserves further study is the rehabilita-
(tau deposition); other approaches currently being studied tion model, which focuses on identifying and maximizing
remaining abilities as a way to maximize function. Further Research is also needed to identify which patients will
research into this and other strategies may help to identify benet from alternative living environments and supple-
specic aspects of these therapies that benet persons with mental caregiving and to support the development of
dementia. Similarly, research is needed to better character- treatment sites that are more comfortable, less costly, and
ize the aspects of nursing homes and other environments equally safe and effective for the care of individuals with
most likely to improve patient outcomes. moderate to severe dementia (553).
Research is needed on models of care delivery for pa- Further studies of caregivers should identify the most
tients with dementia and their family (4). There is also a effective interventions for relieving burden and identify-
need to study how changes in payment for health services ing those caregivers at highest risk for developing adverse
affect the care of individuals with dementia. outcomes (554).
INDIVIDUALS AND ORGANIZATIONS THAT

SUBMITTED COMMENTS
George S. Alexopoulos, M.D. Katie Maslow, M.S.W.
Paul Appelbaum, M.D. Helen S. Mayberg, M.D.
Steven Barczi, M.D. Barnett S. Meyers, M.D.
Dan G. Blazer, M.D., M.P.H., Ph.D. Jacobo Mintzer, M.D.
Frank W. Brown, M.D. Gary S. Moak, M.D.
Kathleen C. Buckwalter, Ph.D., R.N., F.A.A.N. Victor Molinari, Ph.D., A.B.P.P.
Debra Cherry, Ph.D. Lawrence J. Nardozzi, M.M.M., M.D., D.F.A.P.A., C.P.E.
Mirean Coleman, M.S.W., L.C.S.W., C.T. Suzann Ogland-Hand, Ph.D.
Christopher Colenda, M.D., M.P.H. Ronald C. Petersen, M.D., Ph.D.
Yeates Conwell, M.D. Jill Pettigrew, M.B.B.S., F.R.A.N.Z.C.P.
John R. M. Copeland, M.D., F.R.C.P., F.R.C.Psych. Kiran Rabheru, M.D., F.R.C.P.C.
Jeffrey L. Cummings, M.D. Barry Reisberg, M.D.
M. L. Donnelly, M.D., F.R.C.P.C. Robert G. Robinson, M.D.
Brian Draper, M.B.B.S., M.D., F.R.A.N.Z.C.P. Robert M. Rohrbaugh, M.D.
Elizabeth Edgerly, Ph.D. Jules Rosen, M.D.
Barbara Else, M.P.A., MT-BC Eugene H. Rubin, M.D., Ph.D.
Serge Gauthier, M.D., F.R.C.P.C. Kenneth M. Sakauye, M.D.
David S. Geldmacher, M.D. Stephen F. Signer, M.D., C.M.
George T. Grossberg, M.D. Elizabeth Sloan, M.S., L.C.P.C.
Elizabeth Heck Gould, M.S.W., L.C.S.W. Gary W. Small, M.D.
Nathan Herrmann, M.D., F.R.C.P.C. John A. Snowdon, M.D., M.Phil., F.R.C.Psych.
Al Herzog, M.D. Ann M. Steffen, Ph.D.
Dilip V. Jeste, M.D. David C. Steffens, M.D., M.H.S.
Jason Karlawish, M.D. Robert Stern, M.D., Ph.D.
Daniel Kaufer, M.D. Nicholas E. Stratas, M.D., D.L.F.A.P.A.
Kristy Klein, M.S.W. David L. Sultzer, M.D.
David Knopman, M.D. Trey Sunderland, M.D.
Edward C. Lauterbach, M.D., F.A.N.P.A., D.F.A.P.A. Can H. Tang, M.D.
J. Kenneth Le Clair, M.D., F.R.C.P.C Linda Teri, Ph.D.
Peter A. Lichtenberg, Ph.D., A.B.P.P. Larry E. Tune, M.D.
Benjamin Liptzin, M.D. Peter J. Whitehouse, M.D., Ph.D.
Constantine Lyketsos, M.D., M.H.S. Antonette Zeiss, Ph.D.
Alzheimers Association Association of Family Psychiatrists

American Academy of Psychoanalysis and Dynamic Canadian Academy of Geriatric Psychiatry
Psychiatry Canadian Coalition for Seniors Mental Health
American Association for Geriatric Psychiatry Canadian Psychiatric Association
American Association of Directors of Psychiatric Residency Group for the Advancement of Psychiatry
Training Magellan Health Services, Inc.
American Association of Suicidology National Association of Social Workers
American College of Neuropsychopharmacology National Sleep Foundation
American Music Therapy Association Royal Australian and New Zealand College of Psychiatrists
American Neuropsychiatric Association Society for Behavioral and Cognitive Neurology
American Psychiatric Nurses Association Society of Biological Psychiatry
Association for Behavioral and Cognitive Therapies World Federation for Mental Health
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randomly assigned to the two groups; both the subjects and the investigators are blind
to the assignments.
[A] Randomized clinical trial. Same as above, but not double-blind.
[B] Clinical trial. A prospective study in which an intervention is made and the results of
that intervention are tracked longitudinally; study does not meet standards for a ran-
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[C] Cohort or longitudinal study. A study in which subjects are prospectively followed over
time without any specic intervention.
[D] Case-control study. A study in which a group of patients is identied in the present and
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[F] Review. A qualitative review and discussion of previously published literature without
a quantitative synthesis of the data.
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PR A C T I CE G UI D E L INE FOR T H E

Treatment of Patients With

WORK GROUP ON ALZHEIMERS DISEASE AND OTHER DEMENTIAS

STEERING COMMITTEE ON PRACTICE GUIDELINES

AREA AND COMPONENT LIAISONS

OVERVIEW OF GUIDELINE DEVELOPMENT PROCESS. . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 7

GUIDE TO USING THIS PRACTICE GUIDELINE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 8

PART A: TREATMENT RECOMMENDATIONS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 11

II. FORMULATION AND IMPLEMENTATION OF A TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 14

III. SPECIFIC CLINICAL FEATURES INFLUENCING THE TREATMENT PLAN . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 37

PART B: BACKGROUND INFORMATION AND REVIEW OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . 42

IV. DISEASE DEFINITION, NATURAL HISTORY, AND EPIDEMIOLOGY . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 42

V. REVIEW OF AVAILABLE EVIDENCE . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 48

PART C: FUTURE RESEARCH NEEDS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 61

INDIVIDUALS AND ORGANIZATIONS THAT SUBMITTED COMMENTS . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . 63

STATEMENT OF INTENT OVERVIEW OF GUIDELINE

TA BL E 1. DSM-IV-TR Diagnostic Criteria for 294.1x Dementia of the Alzheimers Type

II. FORMULATION AND IMPLEMENTATION OF A

tients, usually together with their caregivers, at regular B. PSYCHIATRIC MANAGEMENT

monitoring of food intake, because a patient with demen- 3. Electroconvulsive therapy

III. SPECIFIC CLINICAL FEATURES INFLUENCING THE

3. Ethnic and Cultural Background B. CO-OCCURRING CONDITIONS AND

IV. DISEASE DEFINITION, NATURAL HISTORY,

V. REVIEW OF AVAILABLE EVIDENCE

INDIVIDUALS AND ORGANIZATIONS THAT

Alzheimers Association Association of Family Psychiatrists

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