Schizophrenia Clinical Trial
Official title:
Nicotine Replacement Therapy Added to Cognitive Behavioral Therapy for Smoking Cessation in Patients With Major Mental Illness
This proposal seeks to evaluate a pilot smoking cessation treatment program that will combine nicotine replacement therapy with or without bupropion sustained-release (SR) with cognitive behavioral therapy for smoking cessation in patients with major mental illness.
Background:
Seventy-four to 92% of patients with schizophrenia smoke cigarettes compared to 24% of the
adult US population and 18% of adults in Massachusetts (1-3). Patients with schizophrenia
also smoke more cigarettes on average per day (4) and attain higher serum levels of
cotinine, the primary metabolite of nicotine, a finding attributed to deeper smoke
inhalation (5). Cigarette smoking has been identified as the single most important source of
preventable morbidity and premature mortality in the general U.S. population for the last 29
years (6, 7). Compounded by the problem that patients with schizophrenia live a less healthy
lifestyle (8) and may be less likely to receive adequate routine and preventative medical
care (9-12), heavy smoking represents a significant and neglected public health problem for
people with schizophrenia. Patients with schizophrenia clearly have greater morbidity and
early mortality from 'natural causes' than people without schizophrenia (13-22) and are more
likely to die prematurely from cardiovascular or pulmonary disease (14, 19, 23-26). Women
with schizophrenia have been shown to have increased risk of premature death from cancer
(24) and previous studies showing lower mortality from cancer in patients with schizophrenia
compared to the general population have not been confirmed (14, 27, 28). Successful smoking
cessation programs for patients with schizophrenia could reduce this increased medical
morbidity and mortality. A recent report of patterns of nicotine use in a cohort of 50
patients with schizophrenia or schizoaffective disorder underscores this point: the cohort
had a mean age of 47 years and mean age at onset of daily smoking of 20 years; 45.8%
reported they currently have a smoking related health problem; 95.8% had tried
unsuccessfully to cut down on their smoking; 70% had made a serious attempt to quit smoking
(29). Smoking cessation programs for patients with schizophrenia have reported compliance
rates as high as 80% (30).
Nicotinic receptors have been shown to be reduced in number in patients with schizophrenia
(31, 32) and heavy smoking in schizophrenia may be attributable to attempts to overcome this
deficit. Benefits of nicotine to patients with schizophrenia include reversal of some of the
specific cognitive deficits associated with schizophrenia and antipsychotic treatment
[(33-37). Nicotine has been shown to improve learning, visual and spatial working memory,
attention, auditory sensory gating smooth pursuit eye movements and reaction time (38, 39).
The positive effects of chronic nicotine treatment appear to persist over time, and in some
studies, improvements in cognition with chronic nicotine treatment become more robust over
time (40). Smoking cessation in patients with schizophrenia is associated with increase in
positive symptoms (30). Treatment with atypical antipsychotics may enhance the effectiveness
of smoking cessation treatment (41-43). The mechanism of this effect is not known but may be
due to decreased extrapyramidal side effects, improved efficacy for negative symptoms or
effects on glutamatergic systems. Combination of NRT and antidepressant medication has been
shown to increase cessation rates over monotherapy with NRT (44) but not over antidepressant
medication alone (45).
Nicotine replacement therapy (NRT) is a powerful aid to smoking cessation with well
established efficacy (46-49) in non-psychiatric patients and has been proposed as a
potential tool in increasing smoking harm reduction in persons unable to achieve smoking
abstinence (50). Smoking cessation outcomes in patients with schizophrenia using NRT have
been extremely variable. Ziedonis and colleagues used a range of doses of NRT administered
by patch, gum or combination in addition to CBT for up to 10 weeks in 24 patients with
schizophrenia (51). Twelve subjects completed the trial. The cessation rate was 13% at 6
months (51). In one study, atypical antipsychotic agents, in combination with the nicotine
transdermal patch, have been shown to significantly enhance the rate of smoking cessation
(55.6% in the atypical agent group versus 22.2% in the typical group) (41). In this study
the overall end of treatment point prevalence smoking cessation rate in 45 patients with
schizophrenia was 35%. In another study of the acute effects of transdermal nicotine patch
in psychiatric patients, however, no patients quit smoking acutely, and only heavy smokers
reduced their cigarette consumption (52).
Safety of NRT in patients with schizophrenia has only been evaluated on a very small scale.
One important trial examined the effects of a 21 mg nicotine patch on smoking behavior,
nicotine levels in blood and signs of toxicity in patients with schizophrenia (53). In this
crossover trial, 10 male veterans were monitored while wearing nicotine vs placebo patches.
The nicotine patch condition was associated with increased nicotine levels without signs of
toxicity and decreased CO levels in 80% of patients. No trials have reported worsening of
psychiatric symptoms with NRT. Larger studies in which NRT is combined with behavioral
support are needed to evaluate the efficacy and safety of NRT in schizophrenia.
Treatment Component:
Subjects will be outpatients who are clinically stable and currently in treatment for
schizophrenia or schizoaffective disorder. Subjects will be recruited through referral from
case managers, residential treatment settings and outpatient treaters. Subjects must smoke
=1/2 pack per day of cigarettes and wish to quit smoking.
Subjects will be randomly assigned to receive cognitive behavioral smoking cessation therapy
CBT) with nicotine patch (NRT) plus placebo or nicotine patch combined with bupropion SR.
Subjects who are unable to tolerate or who have a contraindication to treatment with zyban
may be enrolled to receive CBT and open label NRT alone. All subjects will receive a 12
session group cognitive behavioral therapy (CBT) program designed for smoking cessation
treatment in patients with schizophrenia in addition to pharmacologic treatment.
Evaluation Component:
The evaluation component of this protocol involves monitoring patients for stability of
psychiatric symptoms, serum levels of psychiatric medications, and medication side effects
at baseline and weeks 4, 8, 12 and 14 and degree of smoking reduction or cessation weekly
during the treatment intervention and at 6, 12 and 24 months.
At baseline, subjects will complete a demographic questionnaire. Prior to beginning
treatment, subjects will be evaluated for symptoms of psychosis, depression, anxiety, and
medication side effects with standard clinical rating scales that include the schedule for
assessment of negative symptoms (SANS), positive and negative symptom scale (PANSS),
Hamilton depression scale (HamD), Hamilton anxiety scale (HamA), abnormal involuntary
movement scale (AIMS), Simpson Angus Scale, and SAFTEE. A brief cognitive battery will
include tests of response inhibition (the single trial Stroop), vigilance (continuous
performance test), verbal fluency (FAS), verbal memory (California Verbal Learning Test),
working memory (letter number span), non-verbal memory (Benton visual retention test),
psychomotor ability (grooved peg board task), and executive functioning (trail making or
tower of London). Baseline carbon monoxide (CO) measurements will be used with self report
to verify number of cigarettes smoked per day. Serum will be drawn for cotinine and
antipsychotic levels at baseline. Weight will be checked at baseline, 12 and 24 weeks.
Subjects will set a quit date between weeks 3 and 4. The evaluation battery will be repeated
at week 4 just following the quit date. It will also be repeated at week 12 when patients
discontinue the group and medication treatment. An evaluation that includes the clinical
battery and CO measurement will be performed at week 14, two weeks following termination of
smoking cessation treatment and at week 24. Subjects will also be contacted at 1 and 2 years
for follow up self report of tobacco use and CO measurement.
Specific Aims: Treatment
1. Increase availability of nicotine replacement therapy, which is not currently available
by prescription, to patients with major mental illness.
2. Train staff members with expertise in treating patients with major mental illness to be
Tobacco Treatment Specialists using the training protocol developed by University of
Massachusetts Medical School in collaboration with the Massachusetts Department of
Public Health.
3. Establish a network of centers able to deliver tobacco treatment to patients with major
mental illness.
Specific Aims: Evaluation
1. Evaluate smoking cessation rates, smoking reduction rates and stability of psychiatric
symptoms in patients with schizophrenia and schizoaffective disorder during a smoking
cessation attempt using cognitive behavioral therapy combined with NRT plus placebo and
NRT + bupropion SR.
2. Evaluate safety of nicotine replacement therapy in patients with schizophrenia and
schizoaffective disorder when combined with antipsychotic medications.
3. Evaluate safety of nicotine replacement therapy in patients with schizophrenia and
schizoaffective disorder when combined with bupropion SR and antipsychotic medications.
Hypotheses:
1. Nicotine replacement therapy combined with bupropion SR and cognitive behavioral
therapy will be associated with improvement in smoking cessation and smoking reduction
rates when compared to NRT alone added to CBT in patients with schizophrenia and
schizoaffective disorder.
2. Nicotine replacement therapy combined with bupropion SR will be associated with
improvement in negative symptoms, depression and impulsivity when compared to NRT alone
in patients with schizophrenia and schizoaffective disorder who quit smoking.
3. Concurrent treatment with atypical antipsychotic medications will further enhance the
effectiveness of NRT combined with bupropion SR and NRT plus placebo for smoking
cessation and reduction in patients with schizophrenia and schizoaffective disorder
compared to concurrent treatment with conventional antipsychotics.
4. Patients with low baseline cotinine = 250 ng/ml will have higher cessation rates than
patients with high baseline cotinine >250 ng/ml.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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