Pharmacological and Nonpharmacological Treatment of Alcohol Dependence

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Pharmacological and Nonpharmacological Treatment of Alcohol Dependence

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Title: Pharmacological and Nonpharmacological Treatment of Alcohol Dependence

1
Pharmacological and Nonpharmacological Treatment
of Alcohol Dependence

Sponsored by
American Society of Addiction Medicine (ASAM)
Supported by
Florida Society of Addiction Medicine (FSAM)
Southern Coast Addiction Technology Transfer
Center (SCATTC)

2
Faculty
Jeffrey D. Kamlet, MD Private Practice, Internal
Medicine Forensic, Addiction, and Bariatric
Medicine Adjunct Professor of Medicine School of
Graduate Health Sciences Barry University Miami,
Florida Vineet Mehta, MD President Center for
Non-Addictive Living Attending Physician Circles
of Care Private Practice, Psychiatry and
Addiction Psychiatry Melbourne, Florida
3
ASAM Disclosure of Relevant Financial
Relationships Content of Activity
Pharmacological and Nonpharmacological Treatment
of Alcohol Dependence 2006 Courses
4
Glossary of Terms

Commercial Interest - ACCME defines a commercial
interest as any proprietary entity producing
healthcare goods or services, with the exemption
of nonprofit or government organizations and
non-healthcarerelated companies.
Financial relationships - Financial relationships
are those relationships in which the individual
benefits by receiving a salary, royalty,
intellectual property rights, consulting fee,
honoraria, ownership interest (eg, stocks, stock
options or other ownership interest, excluding
diversified mutual funds), or other financial
benefit. Financial benefits are usually
associated with roles such as employment,
management position, independent contractor
(including contracted research), consulting,
speaking and teaching, membership on advisory
committees or review panels, board membership,
and other activities from which remuneration is
received, or expected. ACCME considers
relationships of the person involved in the CME
activity to include financial relationships of a
spouse or partner.
Relevant financial relationships - ACCME focuses
on financial relationships with commercial
interests in the 12-month period preceding the
time that the individual is being asked to assume
a role controlling content of the CME activity.
ACCME has not set a minimal dollar amount for
relationships to be significant. Inherent in any
amount is the incentive to maintain or increase
the value of the relationship. ACCME defines
relevant financial relationships as financial
relationships in any amount occurring within the
past 12 months that create a conflict of
interest.
Conflict of Interest - Circumstances create a
conflict of interest when an individual has an
opportunity to affect CME content about products
or services of a commercial interest with which
he/she has a financial relationship.

5
Supported by

Supported by an unrestricted educational grant
from Forest Pharmaceuticals, Inc.

6
Meeting Agenda

100 PM 110 PM Introductions/Welcome
FSAM State Chapter President and Faculty
110 PM 315 PM Presentations
(Each presentation consists of a lecture and Q
A session)
Module 1 Effective Treatment for Alcohol
Dependence Pharmacotherapy Options
Module 2 Effective Treatment for Alcohol
Dependence Integrating Evidence-Based Behavioral
Interventions and Treatments and Psychosocial
Support Services With Pharmacotherapy
Module 3 Concomitant Conditions Psychiatric,
Medical, and Other Substance Use
315 PM 330 PM BREAK
330 PM 500 PM ASAM/NAADAC Panel Discussion
Strengthening Physician/Counselor Relationships
for Improved Patient Outcomes in the Treatment of
Alcohol Dependence
500 PM 515 PM Evaluation and Adjournment

7
To Receive Credit

Complete and return the survey and program
evaluation form to Denise Petrone
Before leaving, please sign the registration card
ASAM will mail you your certificate

8
Effective Treatment for Alcohol Dependence
Pharmacotherapy Options Module 1
9
Program Objectives

At the conclusion of this activity, participants
should be able to
Review clinically relevant developments and
research in the use of disulfiram, naltrexone,
and acamprosate for alcohol dependence disorder
Identify and discuss clinical issues relative to
the use of pharmacotherapy
Review and discuss existing and promising
treatment and management options for alcohol
dependence
Discuss evidence-based behavioral intervention
and treatment, which includes integration of
psychosocial support services with
pharmacotherapy
Review relevant clinical information on
concomitant conditions

10
Module 1 Overview

The scope of the problem
Alcoholism is a brain disease
Pharmacotherapy for alcohol dependence
Pharmacotherapy in practice

11
Prevalence of Alcohol Use
NIAAA National Epidemiologic Survey onAlcohol
and Related Conditions (NESARC)
Any Alcohol Disorder 17.6 million (8.5)
Alcohol Dependence 7.9 million (3.8)
Alcohol Abuse 9.7 million (4.7)
NIAAANational Institute on Alcohol Abuse and
Alcoholism. Grant BF et al (2004).
12
Epidemiology

Eight million adult United States citizens are
dependent on alcohol
Alcoholism tends to run in families and affects
minors
More than 50 of American adults have a past
history or close relationship with alcoholism
25 of minors have been exposed to familial
alcoholism or alcohol abuse
Alcohol use is implicated in approximately 25
of violent crimes and more than 16,000 fatal car
accidents each year
National alcoholism costs are approximately 185
billion each year

Individuals younger than 18 years of age.
13
Societal Costs of Alcohol Dependence
Total Cost 184.6 Billion
7,466 (4)
24,093 (13)
15,963 (9)
10,085 (5)
2,909 (2)
1,253 (1)
36,499 (20)
86,368 (47)
Cost in millions of US dollars. FASfetal
alcohol syndrome. Key definitions correspond to
pie chart sections in clockwise order beginning
specialty alcohol services at the 12 oclock
position.
Harwood H et al. In NIH Publication No. 98-4327.
Available at http//www.niaaa.nih.gov.
14
Addiction A Brain Disease

Neurological adaptation
Mesolimbic DA system
Animal studies
Human studies

DAdopamine.
15
Brain Reward Pathways

The VTA-nucleus accumbens pathway is
activated by all drugs of dependence, including
alcohol
This pathway is important not only in drug
dependence, but also in essential physiological
behaviors such as eating, drinking, sleeping, and
sex

Messing RO (2001).
16
Relapse and Conditioning

Repeated use of alcohol has caused conditioning
to occur in related circuits
Now cues associated with alcohol use can
activate the reward and withdrawal circuit
This circuit can evoke anticipation of alcohol or
feelings similar to withdrawal, which may
precipitate relapse in an abstinent patient

Messing RO (2001).
17
Overview of Major Neurotransmitters Associated
With Alcohol
18
Dopamine

General Function Regulates motivation,
reinforcement, and fine motor control
Specific Action by Alcohol Initiates a release
at the NAC either directly or from projections
via the mesolimbic system from the VTA
Alcohol-Related Function Mediates motivation and
reinforcement of alcohol consumption
NACnucleus acumbens VTAventral tegmental area.

Swift RM (1999).
19
?-aminobutyric Acid (GABA)

General Function Serves as the primary
inhibitory neurotransmitter in the brain
Specific Action by Alcohol Causes tonic
inhibition of dopaminergic projections to the
VTA and NAC. Prolonged alcohol use causes a
down-regulation of these receptors and a
potential for decreased inhibitory
neurotransmission
Alcohol-Related Function May contribute to
intoxication and sedation inhibition of GABA
function following drinking may contribute to
acute withdrawal symptoms

Swift RM (1999).
20
Glutamate

General Function Serves as the major excitatory
neurotransmitter in the brain
Specific Action by Alcohol Alcohol inhibits
excitatory neurotransmission by inhibiting both
NMDA and non-NMDA (kainite and AMPA) receptors.
Up-regulation of these receptors to compensate
for alcohols antagonistic effect occurs after
prolonged exposure to alcohol, resulting in an
increase in neuroexcitation
Alcohol-Related Function May contribute to acute
withdrawal symptoms inhibition of glutamate
function following drinking cessation may
contribute to intoxication and sedation
NMDAN-methyl-D-aspartate AMPAa-amino-3-hydroxy-
5-methisoxizole-4-propionic acid.

Swift RM (1999).
21
Opioid Peptides

General Function Regulates various functions and
produces morphine-like effects, including pain
relief and mood elevation
Specific Action by Alcohol Alcohol stimulates
ß-endorphin release in both the NAC and VTA
area. ß-endorphin pathways can lead to increased
dopamine release in the NAC
Alcohol-Related Function Contributes to
reinforcement of alcohol consumption, possibly
through interaction with dopamine

Swift RM (1999).
22
Alcohol Dependence Is A Chronic Disease
23
Similar Outcomes to OtherChronic Illnesses

Type 1 DM 30 to 50 relapse each year
requiring additional medical care
HTN and asthma 50 to 70 relapse each year
requiring additional medical care
Addiction 40 to 60 relapse within first year

DMdiabetes mellitus HTNhypertension. McLellan
AT et al (2000).
24

Less than 30 of patients with type 1 DM, HTN,
and asthma adhere to prescribed diet and
behavioral changes designed to improve function
and reduce risk factors.

McLellan AT et al (2000).
25
Defining Alcohol Use
26
Defining the Standard Drink

A standard drink 14 g ethanol
12 oz of regular beer or cooler (5 alcohol)
5 oz of table wine (12 alcohol)
1.5 oz of hard liquor (40 alcohol, 80 proof)
The average person metabolizes about 1 standard
drink per hour

NIAAA. Helping Patients Who Drink too Much a
Clinicians Guide NIAAA Web site.
http//pubs.niaaa.nih.gov/publications/Practition
er/CliniciansGuide2005/guide.pdf.
27
US Government Recommended Safe Levels of
Alcohol Consumption

Men 2 drinks per day
Women 1 drink per day

28
At-Risk Drinking

3 out of 10 US adults consume alcohol at levels
that increase their risk for physical, mental
health, and social problems
Of those at risk, about 25 currently have
alcohol abuse or dependence

NIAAA. Helping Patients Who Drink too Much a
Clinicians Guide NIAAA Web site.
http//pubs.niaaa.nih.gov/publications/Practition
er/CliniciansGuide2005/guide.pdf.
29
At-Risk Drinking (Contd)

Defined as drinking at a level that causes or
elevates the risk for alcohol-related problems
or complicates the management of other health
problems
Men
5 or more standard drinks per day
15 or more standard drinks per week
Women
4 or more standard drinks per day
8 or more standard drinks per week

Dawson DA et al (2005). NIAAA. Helping
Patients Who Drink too Much a Clinicians Guide
NIAAA Web site. http//pubs.niaaa.nih.gov/public
ations/Practitioner/CliniciansGuide2005/guide.pdf.

30
Alcohol Abuse

DSM-IV-TR Criteria
Maladaptive pattern of alcohol use leading to
clinically significant impairment or distress,
manifested within a 12-month period by at least
1 of the following
Failure to fulfill role obligations at work,
school, or home
Recurrent use in hazardous situations
Legal problems related to alcohol
Continued use despite alcohol-related socialor
interpersonal problems

DSM-IV-TRDiagnostic and Statistical Manual of
Mental Disorders, 4th edition, text
revision. American Psychiatric Association. In
DSM-IV-TR. 2000.
31
Alcohol Dependence

DSM-IV-TR Criteria
Maladaptive pattern of alcohol use leading to
clinicallysignificant impairment or distress,
manifested within a12-month period by at least 3
of the following
Tolerance
Withdrawal
Loss of control over amount of alcohol consumed
Preoccupation with controlling drinking
Preoccupation with drinking activities
Impairment of social, occupational, or
recreational activities
Use is continued despite persistent problems
related to drinking

American Psychiatric Association. In DSM-IV-TR.
2000.
32
Pharmacologic Treatment of Alcohol Dependence
33
Treatment Overview

Psychosocial treatments help many alcoholics
reduce their drinking or achieve abstinence
40 to 70 relapse within a year
Neuroscientific advances suggest the possibility
of developing medications to enhance the
effectiveness of psychosocial treatments
These medications target neurotransmitter systems
that mediate alcohol reward associated with its
abuse liability and/or ameliorate neurochemical
dysfunction in those with a biological
predisposition to the disease

Litten RZ et al (1996). Swift RM (1999).
34
Neuropharmacological Targets for Treating Alcohol
Dependence

Neurotransmitters and receptors
Acetylcholine
Adenosine (A1, A2 receptors)
Cannabinoid receptors
DA (D1, D2, D3, D4)
GABAA, GABAB receptors
Glutamate (NMDA, AMPA, kainate receptors)
Glycine
Norepinephrine (NE alpha a, beta ß
receptors)
Opioid peptides (mu µ, delta ?, kappa ?
receptors)
Other peptides (vasopressin, neuropeptide Y)
Serotonin (5-HT several receptors, particularly
5-HT3)
Neurotransmitter transporters
Adenosine, DA, 5-HT, NE
Voltage-gated ion channels
L-type, N-type calcium channels sodium channels
Second messengers
G-proteins, phospholipases, protein kinases,
neurosteroids, hormones

Anton RF et al (2003). Litten RZ et al (2005).
35
Current Neuropharmacological Strategies to Reduce
Drinking Behavior

Medications that reduce alcohol seeking or urge
to drink (craving)
Opioid antagonists, ondansetron, topiramate
Medications that reduce the dysphoria and other
symptoms of acute and protracted withdrawal
Acamprosate, sedatives (?-hydroxybutyrate),
baclofen, antiepileptics/mood stabilizers
(carbamazepine, valproate, topiramate)
Medications that reduce impulsivity/attention
deficits
DA agonists and antagonists, 5-HT antagonists
Medications that reduce alcohol bioavailability
Kudzu/bioflavonoids, a2-antagonists
Medications that increase satiety/reduce
appetitive drive
Naltrexone, topiramate, cannabinoid (CB1)
antagonists (?)
Medications that treat comorbid psychiatric
illnesses or reduce psychological distress
Antidepressants (tricyclics, SSRIs),
antipsychotics (typical and atypical),
anxiolytics (buspirone)

SSRIsselective serotonin reuptake inhibitors.
Anton RF et al (2003).
36
Disulfiram Blocks Alcohol Metabolism

Ethanol
? ? alcohol dehydrogenase
Acetaldehyde
? ? aldehyde dehydrogenase
(blocked by Antabuse)
Acetate (Acetyle co-enzyme A)
?
Carbon dioxide and water

37
Opioid Antagonists Basic Science

Alcohol consumption affects the production,
release, and activity of opioid peptides1
Opioid peptides mediate some of alcohols
rewarding effects by enhancing midbrain DA
release
Opioid antagonists suppress alcohol-induced
reward2 and general consummatory behaviors3
Genetic high-risk/FH individuals have an
exaggerated alcohol-induced rise in ?-endorphin
level, and are more responsive to naltrexone
treatment4,5

FHpositive family history. 1. Herz A (1997).
2. Swift RM (1999). 3. Boyle AE et al (1998). 4.
Giannoulakis C (1996). 5. King AC et al (1997).
38
Opioid Antagonist Naltrexone Clinical Science

Some studies in alcoholics have found either no
efficacy for naltrexone1 or efficacy among only a
subgroup with medication compliance rates of 80
to 902,3
Adverse events, particularly nausea, can result
in up to 15 of withdrawals from clinical
studies,4 and may limit acceptability in generic
or managed care facilities
Depot naltrexone preparations may enhance
compliance, and one study has demonstrated
efficacy at reducing heavy drinking in men5
Targeted naltrexone might be another useful
strategy to maximize compliance while diminishing
adverse events rates6,7

1. Kranzler HR et al (2000). 2. Volpicelli JR et
al (1997). 3. Litten et al (1998). 4. Croop RS
et al (1997). 5. Garbutt JC et al (2005). 6.
Heinala P et al (2001). 7. Kranzler HR et al
(2003).
39
Opioid Antagonist Naltrexone Clinical Science
(Contd)

Naltrexone 100 mg/day appears more efficacious
than the usual 50 mg/day dose1,2
Identification of the alcoholic subgroup (perhaps
those with a biological disease predisposition)
most responsive to naltrexone is an important
scientific goal3
Current evidence suggests that high craving and
strong FH are strong predictors of a positive
outcome4
Preliminary evidence suggests that allelic
variation at the mu opioid receptor gene is
associated with differential treatment response
to naltrexone5

1. McCaul ME et al (2000). 2. McCaul ME et al
(2000). 3. Johnson BA and Ait-Daoud (2000). 4.
Monterosso JR et al (2001). 5. Oslin DW et al
(2003).
40
Glutamate Antagonist Acamprosate Basic Science

Excitatory neurotransmitter N-methyl-D-aspartate
(NMDA) contributes to alcohols intoxicating,
cognitive, and dependence-forming effects
NMDA antagonist acamprosate reduces the intensity
of post-cessation alcohol craving on exposure to
high-risk drinking situations

Embellished from Spanagel and Zieglgansberger
(1997).
Spanagel and Zieglgansberger (1997).
41
Glutamate Antagonist Acamprosate Clinical
Science

Poorly absorbed, with a bioavailability of
approximately 10
Excreted unmetabolized therefore, no risk of
hepatotoxicity or interaction with alcohol
Should be used with caution in individuals with
renal impairment
Relatively safe, the most common adverse event
is diarrhea

CAMPRAL (acamprosate calcium) delayed-release
tablets prescribing information 2004.Mason et
al (2002).
42
Glutamate Antagonist Acamprosate Clinical
Science (Contd)

Approved for the treatment of alcohol dependence
in 29 countries and in the US in July 2004
Methodological rigor was enhanced in later
studies (e.g., Sass and colleagues1 Whitworth
and colleagues2) by standardization of diagnosing
alcoholism, laboratory measurements, and
psychosocial treatment regimen
Although more than 20 clinical trials have been
conducted, a meta-analysis of 17 positive studies
revealed that acamprosate vs. placebo increased
continuous abstinence rates following 3 (46 vs.
34), 6 (36 vs. 23), and 12 (27 vs. 13)
months of treatment3
Acamprosate also decreases frequency of drinking
and the intensity of a relapse if drinking is
reinstated after abstinence4,5
Predicators of treatment response that have been
examined and found to have NO predictive value
include increased levels of anxiety,
physiological dependence, FH-, late age of onset,
and being female6
For a review, see Johnson and Ait-Daoud (2000)7,
Ait-Daoud and Johnson (2003)8, and Litten et al
(2005)9

1. Sass et al (1996). 2. Whitworth et al (1996).
3. Mann et al. (2004). 4. Chick and Lehert
(2003). 5. Tempesta et al (2000). 6. Verheul et
al (2005). 7. Johnson and Ait-Daoud (2000). 8.
Ait-Daoud and Johnson (2003). 9. Litten et al
(2005).
43
Rationale for Combining Medications

Small to moderate effect sizes for single
medications
Additive or synergistic effects to interact at
multiple neuronal systems
Single medications might be effective at only
particular phases of the illness
Combinations target a wider range of alcohol
subtypes, particularly if there is a differential
genomic environmental response
BUT
Potential for increased adverse events
Potential for lack of effect or unexpected
antagonistic actions

44
Combined Medications for Treating Alcoholism in
the Clinic Acamprosate Plus Naltrexone

To determine the relative efficacy of naltrexone
(50 mg/day) and acamprosate (1998 mg/day) both
alone and in combination
2 2 factorial with 40 men and women per cell
Double-blind placebo-controlled study
Psychotherapy weekly group coping-skills therapy
12-week study duration

Kiefer et al (2003).
45
Comparing and Combining Naltrexone and
Acamprosate in Relapse Prevention of Alcoholism
(N160)
Naltrexone Plus AcamprosateNaltrexoneAcamprosate
Placebo
1.0
0.9
0.8
0.7
0.6
Proportion of Survivors (Nonrelapse)
0.5
0.4
0.3
0.2
0.1
0
10
20
30
40
50
60
70
80
Time, d
Kiefer et al (2003).
46
Medications Currently Approved for Alcohol
Dependence

Disulfiram (Antabuse)
Naltrexone (ReVia)
Acamprosate (Campral)

Antabuse Florham Park, NJ Odyssey
Pharmaceuticals, Inc. Campral St. Louis, Mo
Forest Pharmaceuticals, Inc. ReVia Wilmington,
De DuPont Pharmaceuticals.
47
Disulfiram (Antabuse)
Antabuse Florham Park, NJ Odyssey
Pharmaceuticals, Inc.
48
Naltrexone (ReVia)
ReVia Wilmington, De DuPont Pharmaceuticals.
49
Acamprosate (Campral)
CrClcreatinine clearance.
Campral St. Louis, Mo Forest Pharmaceuticals,
Inc.
50
Is the Primary Care Office Appropriate for
Treatment?

Willingness and knowledge of primary care
physician
Stage of change (see Module 2) and willingness
of patient
Severity and chronicity of alcohol use disorder
(ASAM criteria)
Psychosocial support available within family and
community
Prior treatment response
Availability of psychosocial and behavioral
treatments
Adherence to treatment plan

51
Monitoring Pharmacotherapy for Alcohol Dependence

Watch for evidence of alcohol and drug use
Ask about alcohol and drug use
Consider blood and urine testing (alcohol and
drug screens, biologic indicators-transaminase
level)
Evaluate adherence to medication and all aspects
of treatment plan
Monitor Alcoholics Anonymous or other group
attendance
Involve other care givers
Evaluate for ongoing psychiatric illness
Evaluate other stressors
Monitor side effects
Provide support

52
Patient Selection for Pharmacotherapy

Research has yet to fully define subtypes of
patients with alcohol dependence who respond to
pharmacotherapy
Naltrexone may be best for those with a FH of
alcohol dependence and significant craving
Medication is only useful for patients who are
interested in treating their alcohol abuse or
dependence
Some physicians provide pharmacotherapy to all
their patients with alcohol abuse and dependence,
whereas other physicians have not yet used these
medications
Medication adherence is a significant problem
Pharmacotherapy may not be effective in limiting
other substance use

53
Summary

Alcohol dependence is a brain disease
Alcohol dependence is a chronic disease
Naltrexone, acamprosate, and disulfiram are
effective in limiting alcohol use
Alcohol dependence can be addressed with
pharmacotherapy in a primary care office
When integrated with psychosocial and behavioral
interventions

54
Effective Treatment for Alcohol Dependence
Integrating Evidence-Based Behavioral
Interventions and Treatments and Psychosocial
Support Services With Pharmacotherapy

Module 2

55
Introduction Module 2

Screening
Brief interventions
Evidence-based psychosocial and behavioral
treatment approaches
Project MATCH
Alcoholics Anonymous (AA)
Integration of pharmacotherapy and
nonpharmacotherapy

MATCHmatching alcoholism treatments to client
heterogeneity.
56
Clinical Indications for Screening

Key opportunities include
As part of a routine examination
Before prescribing a medication that interacts
with alcohol
In the emergency department or urgent care center
In response to family member concerns

57
Clinical Indications for Screening (Contd)

In patients who
Are pregnant or trying to conceive
Are likely to drink heavily, such as smokers,
adolescents, and young adults
Have health problems that might be
alcohol-induced, such as cardiac arrhythmia,
dyspepsia, liver disease, depression or anxiety,
insomnia, and trauma
Have a chronic illness not responding to
treatment as expected, such as chronic pain,
diabetes, gastrointestinal disorders, depression,
heart disease, and hypertension
A patient with signs of an emerging problem

58
Purpose of Screening

To determine if there are indicators of an
alcohol problem requiring further assessment and
perhaps clinical intervention

59
Step 1 Ask About Alcohol UseHelping Patients
Who Drink Too Much NIAAA 2005
Prescreen Do you sometimes drink alcoholic
beverages?
No
Yes
Screening Complete
Ask the screening question about heavy
drinking days How many times in the past year
have you had 5 or more drinks in a day? (for
men) 4 or more drinks in a day? (for women)
60
Is screening positive? 1 or more heavy drinking
days or AUDIT score of gt5 for men or gt4 for women
No
Yes

Your patient needs additional evaluation. For a
more complete picture of the drinking pattern,
determine the weekly average
On average, how may days a week do you have an
alcoholic drink?
On a typical drinking day, how many drinks do you
have?
Record heavy drinking days in the past year and
the
weekly average in chart

Advise staying within maximum drinking limits
For healthy men up to age 65
No more than 4 drinks in a day AND
No more than 14 drinks in a week
For healthy women (and healthy men over age 65)
No more than 3 drinks in a day AND
No more than 7 drinks in a week
Recommend lower limits or abstinence as medically
indicated, for example, for patients who
Take medications that interact with alcohol
Have a health condition exacerbated by alcohol
Are pregnant (advise abstinence)
Express openness to talking about alcohol use and
any concerns it may raise
Rescreen annually

Assess for alcohol abuse or dependence
Please refer to NIAAA Clinicians Guide for
Interview Version form.
AUDITalcohol use disorders identification test.
61
Brief Interventions

Empirically based
Utilized by general medical and MH practitioners
For patients not needing, wanting, or ready to
accept specialty care
Brief, structured, time limited, and directed
toward a specific goal
Goal may be for the patient to try abstinence,
moderation, or harm reduction
Approach is client centered, empathetic,
engaging, noncoercive, and flexible

62
Brief Interventions (Contd)

Intended mainly for less severe and nondependent
drinkers or those in early stages
Applied in a broad array of settings outside
traditional treatment programs such as
office-based practices and other nonspecialized
treatment settings
Effective and cost effective

63
What We Know About Brief Intervention

Decreases alcohol use in both men and women
Decreases healthcare utilization
Decreases costs
1 to 4 sessions are effective
Physicians can be trained to conduct brief
interventions

64
(No Transcript)
65
Goals of Brief Intervention

Reduce risk of harm from continued substance use
Abstinence provides the greatest degree of harm
reduction and safety, but the specific goal for
each individual is determined by consumption
patterns, consequences, risks, and, above all,
individual choice
Only the client can choose the goal, no matter
what you recommend and think is best!

66
Appropriate Patients for Office-Based Physician
Intervention

Patients with low to moderately severe
alcohol/drug problems
Patients with more severe problems who are not
ready to take action and/or accept referral for
specialist consultation or treatment
Patients determined to try to reduce/stop on
their own with minimal guidance before
considering other treatment options
Intended mainly for less severe and nondependent
drinkers or those in early stages
Applied in a broad array of settings outside
traditional treatment programs such as
office-based practices and other nonspecialized
treatment settings

67
Physicians Stance

Be friendly and nonthreatening
Convey an attitude of curiosity and concern
Avoid being authoritarian or judgmental
Reassure that all information is confidential

68
Provide Objective Feedback

State your findings clearly, empathetically, and
nonjudgmentally
Stick to the facts about the nature/severity of
problem and its consequences without drawing
firm conclusions
Draw connection between substance use and other
health problems/risks, wherever possible
State your medical concerns

69
Inform Patients About...

Safe consumption limits for alcohol
Definitions of substance ABUSE and DEPENDENCY
Added risks posed by family history of alcohol or
drug problems
Your confidence in their ability to change
Your willingness to help

70
Advise Patient to ABSTAIN if

Evidence of substance abuse or dependence
Pregnant or trying to conceive
Contraindicated medical/psychiatric condition or
medication
Significant family history of alcohol/drug
problems (at least 1 parent, grandparent, or
sibling)

71
Advise Patient to CUT DOWN if

Drinking above low-risk levels without current
evidence or prior history of alcohol dependence
Initial recommendation to abstain from
alcohol/drugs has been rejected

72
Stages of Change

People with alcohol/drug problems generally fall
into 1 of 5 stages along a continuum of readiness
to change
This provides a useful framework for determining
how best to approach patients in each stage of
change and what types of interventions are most
likely to be effective

73
Stages of Change (Contd)

Precontemplation Patient does not see the
behavior as a problem, no desire to change (in
denial)
Contemplation Patient beginning to see the
behavior as a problem, but still wavering
(sitting on the fence) yes, but
Preparation Patient is considering options for
change
Action Patient taking specific steps to change
Maintenance Patient preventing relapse

74
The Wheel of Change
75
Assessing Patients Readiness to Change

Response to your feedback and advice offers
strong clues about the patients readiness to
change
ASK What are your thoughts about these findings?
ASK To what extent do you view your drinking as
a problem?
ASK Do you see a need for change?

76
Responding to Patient Resistance

Be prepared for a range of patient reactions,
including shame, dismay, or anger
Avoid reacting to patient resistance as a
challenge to your medical authority
Avoid getting into arguments or debates about how
much drinking is too much
Avoid using the label addict or alcoholic
Emphasize to the patient that only he or she can
make the decision to change

77
Willing to Consider Changing Your Drinking?

If NO, then
Restate your concerns
Encourage reflection of pros and cons of change
versus no change
What are the barriers to change?
Reaffirm your willingness to help when the
patient is ready and, at the very least, to
reevaluate at a later time

78
If Patient Is NOT Willing to Consider Change

Do not react to patient resistance as a challenge
to your medical judgment or authority
Avoid getting into arguments or debates about how
much drinking is too much
Avoid using the label addict or alcoholic
Emphasize to patients that only they can make the
decision to change you have no desire to
pressure them to change
Agree to disagree restate your concerns about
need for change
Your primary goal is to maintain an ongoing
dialogue about their alcohol use and to continue
to encourage change

79
Willing to Consider Changing Your Drinking?

If YES, then
Negotiate a Plan of Action based on
Problem severity
Stage of readiness to change
Level of involvement you, as the primary care
physician, are willing and/or able to provide
Community resources for alcohol dependence
treatment

80
Substance Abuse Treatment Options

Medical detoxification
Inpatient
Outpatient
Residential treatment
Outpatient treatment
Office-based treatment
Addiction psychologist or psychiatrist
Addiction medicine specialist
AA or other self-help program

81
Scientifically Based Approaches to Addiction
Treatment

Cognitive-behavioral therapy
Community reinforcement
Motivational enhancement therapy
12-step facilitation
Contingency management
Pharmacologic therapies
Systems treatment
Behavioral couples therapy
Multidimensional family therapy

National Institute on Drug Abuse (1999). Onken
L (2002).
82
Alcoholics Anonymous

More people use AA than any other resource to
address problems with alcohol.
McCrady Miller (1993)
Weisner, Greenfield, Room (1995)

McCrady Miller (1993). Weisner C et al (1995).
83
12-Step Programs

Accessible
Inclusive
Adaptable/diverse
Growing
Inexpensive
Successful

84
Estimated AA Membership (January 2004)

Members in United States 1,187,168
Groups in United States 52,735
Members Worldwide 2,066,851
Groups Worldwide 104,589
(AA is found in over 150 countries)

AA. Available at http//alcoholics-anonymous.org.
2005.
85
Efficacy of AA
Timko C et al (2000).
86
AA Activities That Positively Correlated to
Drinking Outcomes

Having a sponsor
Engaging in 12-step work
Leading a meeting
Increasing ones degree of participation in the
organization compared to a previous time
Sponsoring other AA members
Working the last 7 of 12 steps

87
Integration Is Necessary

Pharmacotherapy for alcohol dependence should
always be accompanied by psychosocial and/or
behavioral treatments

88
Integration

Monitor abstinence and adherence to treatment
Support abstinence, pharmacotherapy, and
psychosocial/behavioral treatment
Discuss medication as it fits with recovery,
psychotherapy, and AA
Involve other caregivers
Ongoing evaluation of appropriate level of care
Evaluate for ongoing psychiatric illness
Evaluate other stressors
Provide support

89
Summary

Screening should be done in all primary care
offices
Brief interventions are effective
Many psychosocial and behavioral treatmentsare
effective
Integration of pharmacotherapy and
nonpharmacotherapy is necessary

90
Concomitant Conditions Psychiatric, Medical,
and Other Substance Use

Module 3

91
Medical Comorbidities
92
Some Early Clues to Problem Drinking

Injuries
Infections
Gastritis and duodenitis
Hematologic effects
Early hepatic markers

93
As Alcoholism Progresses, the Clinician Will Also
Observe

Hepatic effects
Cardiac effects
Pancreatic effects
Nervous system effects
Mental health effects
Cancer

94
Psychiatric Comorbidities
95
Initial Evaluation and Treatment of Psychiatric
Disorders

In those with active substance use, the following
must be taken into account
Psychiatric symptoms associated with substance
use and withdrawal
Consequences of substance use
Substance induced psychiatric disorders
Withdrawal syndromes
Overlapping symptoms, enmeshed course

96
High Rates of Psychiatric Comorbidity in Alcohol
Dependence

78 of male alcoholics have a coexisting lifetime
history of a psychiatric disorder
86 of female alcoholics have a coexisting
lifetime history of a psychiatric disorder

Kessler RC et al (1997).
97
ECA Data
Lifetime Prevalence ()
ECAepidemiologic catchment area.
98
ECA Data (Contd)

Patients with a psychiatric disorder
22 also had an alcohol disorder
15 also has a drug disorder
Patients with an alcohol disorder
37 had a psychiatric disorder
Patients with a drug disorder
53 had a psychiatric disorder

99
Lifetime Prevalence ofAlcohol Use
Abuse/dependence. BDIbipolar disorder type I
BDIIbipolar disorder type II DYSdysthymia
GPgeneral population MDmajor depression
OCDobsessive compulsive disorder PDpanic
disorder SZschizophrenia. Regler DA et al
(1990).
100
Evaluation

Diagnosis difficult due to symptom overlap and
enmeshed course
Account for substance-induced psychiatric
disorder and withdrawal associated symptoms
History of psychiatric illness
Onset
Periods of abstinence
Family history
Prior treatment
Denial, inadequate history
Relapse
May require multiple visits

101
Treatment Guidelines

Nonaddicting medications, if possible
Educate about addiction and psychiatric illness
Account for complex feelings, attitudes, and bias
toward comorbidity and treatment
Chronic illness model

102
Psychotherapy

Essential to treatment of psychiatric illness
Combine with knowledge of 12 steps
Cognitive behavioral or interpersonal therapy

103
Other Substance Use Is the Norm
104
Lifetime Prevalence of Alcohol Dependence in Drug
Dependence
Alcohol Abuse/Dependence Lifetime Prevalence ()
THCtetrahydrocannabinol.
105
Estimated Prevalence of Dependence Among 15- to
54-Year-Olds, 1990-1992 (NCS)
NCSNational Comorbidity Survey. Adapted from
Anthony JC et al. Exp Clin Psychopharmacol.
19942244-268.
106
Other Substance Use

Use of other drugs complicates treatment of
alcohol dependence
Pharmacotherapies are only available for alcohol
and opioids (maintenance treatment)
Other substance use responds to psychosocial and
behavioral interventions and treatments
Other substance use will be addressed in
addiction treatment programs

107
Summary

Medical and psychiatric comorbidities as well as
use of other substances complicate the treatment
of alcohol dependence

108
Course Summary

Pharmacotherapy for alcohol dependence has the
potential to improve outcomes when integrated
with the psychosocial and behavioral therapies
during the first 12 to 18 months of recovery
the highest risk period for relapse

109
Case Vignettes
110
Case 1

Susan is a 40-year-old executive who has come in
for evaluation of a sleep disturbance. Her
alcohol screen was negative, but she admits that
she drinks 1 to 2 glasses of wine about 2 times
per week. She denies any work-related stress,
legal issues, and drug use. Her family history is
negative for alcohol dependence, but she does
state that her marriage is a bit troubled.
1. Is her alcohol use a concern? Why or why not?

111

Case 1 (Contd)
Due to the reference made to marital
difficulties, you obtain a release of information
and contact her husband. He describes a
remarkably different situation, stating that he
is considering a divorce due to Susans drinking.
He says that she drinks daily, often at least a
bottle of wine, but she is adept at hiding it so
he is not sure how much she actually drinks. She
is performing poorly at her new job in fact she
is on probation. This is her third job in the
past 2 years. He has noticed morning sweats and a
tremor. Her father died a very heavy drinker.

1. What treatment recommendations would you
consider at this time?
112

Case 1 (Contd)
Susan returns for a follow up appointment aware
of your discussion with her husband. She admits
to drinking one to two bottles of wine per night,
a marked increase in tolerance, regular
withdrawal symptoms and dysfunction in multiple
areas of her life. She is now seeking your help.

1. What is her differential diagnosis? 2. Would
you prescribe a pharmacological treatment? If
so, discuss why and which one.
113

Case 2
John is a 24-year-old construction worker who has
been sent in for evaluation by his employer after
a urine drug screen revealed cannabis. He admits
to occasional use, and says it was bad luck
that resulted in the positive urinalysis. He
wants to return to work and says he will quit
using cannabis immediately. He describes regular
alcohol use, primarily beer, about 4 cans a day
on weekends. The physical exam is normal,
laboratory tests are normal, and he does not have
a family history of alcohol or drug-related
problems.

1. What are your concerns about his
presentation? 2. What is your treatment
plan? 3. How would you advise his supervisor?
114

Case 2 (Contd)
Six months later you see John in the emergency
room after he cut off three fingertips at work.
His drug screen is positive for methamphetamine,
cannabis, and alcohol. He has been threatened
with job loss. He lives alone and does not have
any close friends or family. John admits to daily
use of a combination of alcohol and other drugs
his tolerance for alcohol has dramatically
increased. He states that he is happy with his
lifestyle, making good money and partying. He
does want to keep his job.

1. What is your differential diagnosis
now? 2. How would you go about discussing this
situation with John?
115

Case 2 (Contd)
John agrees to quit methamphetamine and cannabis,
but does not want to stop drinking. His
supervisor wants him clean and sober, or he
cannot keep his job.

1. How would you advise John? 2. How would you
advise his supervisor? 3. What treatment
recommendations would you make? 4. Would you
prescribe a pharmacological treatment? If so,
discuss why and which one.
116
Acknowledgments

Slides have been provided by
Addiction Technology Transfer Center (ATTC)
National Institute on Alcohol Abuse and
Alcoholism (NIAAA)
Bankole Johnson, MD
Norman S. Miller, MD
John Patz, DO
Edwin A. Salsitz, MD, FASAM
Marvin D. Seppala, MD
Valerie Slaymaker, PhD
J. Scott Tonigan, PhD
Arnold M. Washton, PhD
Clinical Practice Guidelines for Substance Use
Disorders- Veterans Administration Office of
Quality and Performance