Smoking Cessation Clinical Trial
Official title:
The STOP Study: Real World Effectiveness of Zyban Treatment in a Clinical Population
Despite the significant health, social and economic costs of cigarette smoking, 17% of
Ontarians still currently smoke. Use of smoking cessation pharmacotherapy such as Zyban
(bupropion HCl) has been shown to double quit rates but such medications are under-utilized
by smokers attempting to quit. It has been suggested that the high price of pharmacotherapy
may act as a barrier to accessing such treatment.The main objective of this study is to
evaluate the methods and effectiveness of providing smokers who want to quit with 8 weeks of
free Zyban in combination with smoking cessation counselling through family health teams and
community health centres across the province.
Hypothesis: Ontario smokers who receive 8-weeks of free bupropion in combination with brief
counselling will have higher smoking cessation rates than the standard population cessation
rates.
Nicotine dependence, like other addictive disorders, can be characterized as a chronic,
relapsing disease (Leshner, 1997). Although there is significant morbidity and mortality
associated with this disorder, the majority of smokers are not treated adequately to the
widely accepted goal of complete long-term abstinence from smoking. This may be due to the
under-utilization of accepted pharmacotherapies for the treatment of tobacco dependence.
Bupropion (Zyban) Bupropion is the first line of non-nicotine-based pharmacotherapy for
smoking cessation. Several large-scale clinical trials have shown bupropion to be an
efficacious smoking cessation aid (Hurt et al., 1997; Jorenby et al., 1999; Ahluwalia et
al., 2002). In one such study, a 44% abstinence rate was reported for seven weeks of
treatment with bupropion at 300 mg/day, compared to 19% for placebo (Hurt et al, 1997). A
recent meta-analysis has reported that bupropion monotherapy approximately doubles the rate
of smoking cessation (OR 1.94) (Hughes et al, 2007).
Despite its efficacy, bupropion's mechanism of action is unclear. Attenuation of
abstinence-associated increase in craving and withdrawal symptoms has been suggested as
possible mechanisms of bupropion's effect on smoking behaviour in a few randomized clinical
trials (Jorneby et al., 1999; Shiffman et al., 2000; Lerman et al., 2002; Durcan et al,
2002). However, these effects are not universally demonstrated (Hurt et al., 1997; Shiffman
et al., 2000). Other possible bio-behavioral mechanisms have remained largely unexplored.
Using positron emission tomography (PET) it has been shown that in contrast to untreated
smokers, when bupropion-treated smokers were exposed to cigarette-related cues there was
less metabolic activation in their anterior cingulate cortex, a region of the brain
previously shown to be activated by cigarette cues (Brody et al., 2004;Brody et al., 2002).
STOP Study Background and Rationale
Treatment with pharmacotherapy such as nicotine replacement therapy (NRT) or Zyban is a safe
and effective smoking cessation strategy that can double the chance of quitting successfully
over the long-term (Cornuz, 2007). However, research has shown that most smokers who are
interested in quitting do not use pharmacotherapy to aid in their quit attempt.
Misconceptions about the harmful effects of nicotine are a strong barrier to the use of
pharmacotherapy. The cost of pharmacotherapy may also be a significant contributor to the
under-utilization of smoking cessation aids such as NRT and Zyban. Karnath (2001) suggested
that the high cost of successful pharmacotherapy treatment for smoking cessation may be a
barrier for some individuals. Moreover, Cokkinides et al (2005) reported that smokers with
private insurance were more likely to use smoking cessation pharmacotherapies than smokers
without insurance. The addition of free NRT to a group behavioural cessation program
substantiated these claims by showing an increase in quit rates from 38% to 65% (Alberg et
al, 2004). These studies suggest that economic barriers may prevent smokers from using
pharmacotherapy in their attempts to quit smoking.
The study proposed herein will introduce free bupropion as another treatment option for
smoking cessation for Ontario smokers. Community Health Centres and Aboriginal Health Access
Centres are interdisciplinary health models that are able to help individuals who would
otherwise be prevented from accessing health services due to social and geographic barriers.
As they aim to eliminate these other barriers and consequently control for them, they are an
ideal health model for determining whether eliminating the economic barriers of smoking
cessation improves smoking cessation rates. Family Health Teams are more recent health
models that provide integrated and interdisciplinary primary health care. Since they are
able to treat large and diverse populations, they are an ideal health model for accessing
Ontario smokers.
Objectives
1. To evaluate the effectiveness of 8-weeks of free bupropion in combination with brief
counselling through family health teams, community health centres and aboriginal health
access centres in Ontario for smoking cessation.
2. To determine whether distributing free bupropion in combination with brief counselling
increases smoking cessation rates in Ontario smokers compared to CTUMS survey data for
Ontario over the same time period.
;
Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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