a Department of Preventative Cardiology, Ullevål University Hospital, N-0407 Oslo, Norway
b St. Imre Hospital, Budapest, Hungary
c Department of Cardiology and Pneumology, Hospital AK Altona, Hamburg, Germany
d Help2Quit Centre, Royal Shrewsbury Hospital, Shrewsbury, UK
e Tzannio General Hospital, Piraeus, Greece
f University of Basel, Basel, Switzerland
g Monash Medical Centre, Monash Institute of Public Health Services Research, Victoria, Australia
h Department of Pulmonary Medicine, Slotervaart Hospital, Amsterdam, The Netherlands
i GlaxoSmithKline Research and Development, Greenford, Middlesex, UK
* Corresponding author. Tel.: +22-11-79-39; fax: 22-11-99-75
E-mail address: serena.tonstad{at}ulleval.no
Received 16 December 2002; accepted 18 December 2002
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Abstract |
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Methods Six hundred twenty-nine subjects with CVD who smoked 10 cigarettes/day were randomised in a double-blind, multicentre study to receive bupropion SR (150mg twice daily) or placebo for 7 weeks, with a follow-up of 52 weeks. Primary efficacy endpoint: continuous abstinence from smoking from weeks 4 to 7. Secondary endpoints: continuous abstinence (weeks 412, 426 and 452) and weekly point prevalence abstinence. All participants received brief motivational support. Safety was evaluated throughout the study.
Results Continuous smoking abstinence rates from weeks 4 to 7 were significantly higher in subjects receiving bupropion SR compared with placebo (43 vs. 19%, odds ratio [OR]=3.27, 95% confidence interval [CI] 2.244.84; ). Continuous abstinence rates from weeks 4 to 26 and 4 to 52 continued to be more than double for bupropion SR compared with placebo (27 vs. 11%; 22 vs. 9%,
). Weekly point prevalence abstinence was significantly higher for participants who received bupropion SR compared with placebo at weeks 3, 7, 26 and 52
. In both groups, there were no clinically significant changes in blood pressure and heart rate throughout the treatment phase. Overall, 6% of the participants
discontinued study medication due to an adverse event (bupropion SR,
; placebo,
).
Conclusions After 7 weeks of bupropion SR treatment, more than twice as many smokers with CVD had quit smoking at 1 year compared with placebo. The safety profile of bupropion SR was similar to that previously observed in general smoking populations.
Key Words: Smoking cessation Cardiovascular disease Bupropion sustained release
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1. Introduction |
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Bupropion sustained release (bupropion SR) is a non-nicotine-based treatment for use in smoking cessation. Controlled clinical studies involvingapproximately 8000 subjects receiving bupropion SR have now demonstrated the efficacy and tolerability of this agent.913 This efficacy is acknowledged in smoking cessation guidelines1416 and the National Institute for Clinical Excellence has recently recommended its use in smoking cessation.17 Bupropion SR is effective in smokers who may be considered particularly refractory to treatment.11,18 In addition, meta-analyses suggest that the efficacy, tolerability and safety of bupropion SR are unaffected by a previous history of serious conditions such as alcoholism and major depression.19 However, there have been no clinical studies carried out to date that have assessed bupropion SR as an aid to smoking cessation in subjects with CVD. Smokers who have survived a cardiac event but not quit smoking may be more nicotine dependent or face more barriers to quitting than other smokers.
We conducted a double-blind, multicentre, randomised study to assess the efficacy and safety of bupropion SR in subjects with smoking-related CVD.
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2. Methods |
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Subjects were excluded if they had a predisposition for seizure; had a current diagnosis of severe renal, hepatic, haematological, pulmonary or neurological disease; or had a history or current diagnosis of bulimia or anorexia nervosa. Subjects were also excluded if they had an acute or chronic medical condition likely to impair drug absorption, distribution, metabolism or excretion; had a history or current diagnosis of panic disorder, psychosis, or bipolar disorder; or were depressed.
The protocol was approved by the appropriate Independent Ethics Committee or Institutional Review Board and participants provided written informed consent.
2.2. Interventions
We performed a multicentre, randomised, double-blind, placebo-controlled study in subjects from 28 centres across 10 countries.
The study consisted of a 1- to 2-week screening/baseline phase, a 7-week treatment phase and follow-up at 3, 6 and 12 months. Subjects set a target quit date for >7 but 14 days after baseline assessment. At baseline, smoking history and cardiovascular diagnoses were collected, and expiratory carbon monoxide levels were measured using a Bedfont Smokerlyser monitor. Participants were also weighed and two questionnaires (the Fagerström Tolerance Questionnaire20,21 and a Smoking Assessment Questionnaire) were completed. Participants were then randomised in a 1:1 ratio to receive either bupropion SR (150mg/day on days 13; 150mg twice daily on days 449) or placebo during the 7-week treatment phase.
Subjects were contacted by telephone 1 day before their target quit date and reminded that they were due to stop smoking the following day. Three days after this date, subjects were again contacted to provide motivational support. Participants recorded their cigarette consumption (number of cigarettes per day) on a diary card and visited the clinic each week throughout the treatment phase. At each clinic visit, subjects were weighed, vital signs and expiratory carbon monoxide levels measured and brief motivational support (1015 min) was given. At week 7, the Smoking Assessment Questionnaire was completed.
During follow-up, subjects were contacted at monthly intervals to encourage abstinence from smoking and prevent relapse. At weeks 12, 26 and 52, subjects were weighed, expiratory carbon monoxide levels and vital signs were measured and brief motivational support given. Subjects who withdrew or missed a clinic visit were assumed to be smoking.
2.3. Primary outcomes
The primary outcome was defined as continuous abstinence from smoking for a 4-week period from the beginning of week 4 of the treatment phase. Continuous abstinence was assessed by the investigator and confirmed by the subject's self-report of not smoking and an expiratory carbon monoxide level <10ppm. Subjects with missing investigator assessments were assumed to be smokers at that visit.
2.4. Secondary outcomes
Secondary outcomes of efficacy included continuous abstinence from smoking from week 4 to weeks 12, 26 and 52. In addition, weekly point prevalence abstinence (abstinence from smoking for the previous 7-day period) was assessed during the treatment and follow-up phase.
Change in body weight relative to baseline was assessed at the end of the treatment phase (week 7) and at weeks 26 and 52 of the follow-up phase.
At week 7, subjects were asked to evaluate their experience with the study medication, and whether they would recommend it to other smokers (Smoking Assessment Questionnaire).
2.4.1. Safety
Vital signs were recorded throughout the study, and adverse events were recorded throughout the treatment phase and up to week 9. All serious adverse events were collected throughout the treatment phase, after which only serious adverse events related to study medication were recorded.
2.5. Statistics
In the study of Tashkin et al.,11 which examined smokers considered refractory to treatment, the 4-week continuous abstinence rate was 15% for subjects receiving placebo. We considered a 10% increase in the continuous abstinence rate for subjects receiving bupropion SR to be clinically relevant. Therefore, we assumed that 15% of subjects receiving placebo and 25% of subjects receiving bupropion SR would remain continuously abstinent during weeks 47 of the current study. With 620 participants randomised 1:1, the study would have at least 85% power to detect this difference at the two-sided 5% level of significance and detect a difference assuming that 5% of the subjects randomised to placebo and 12% of those randomised to bupropion SR, remained continuously abstinent at6 months.
Data were analysed using SAS®(v.6.12) statistical software. For continuous abstinence data, comparison of the treatment groups was performed using an exact test according to Gart and Cox22,23 stratified by country. For point prevalence abstinence, the treatment groups were compared using the exact test. Change in weight relative to baseline was compared by analysis of covariance including terms for treatment, centre, gender and abstention status, with baseline weight as a covariate.
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3. Results |
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In both treatment groups, subjects with CVD and chronic obstructive pulmonary disease and/or diabetes had similar continuous abstinence rates for weeks 452 compared with CVD only (18 and 15%, respectively).
3.3.1. Point prevalence abstinence
Weekly point prevalence abstinence for the bupropion SR group remained more than double that of the placebo group throughout the study. Statistical analysis revealed significantly greater weekly point prevalence abstinence in participants receiving bupropion SR compared with placebo at all prespecified time points (Fig. 4).
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3.3.2. Body weight
During the treatment phase, subjects receiving bupropion SR who had abstained from smokingfrom the beginning of week 4 to the end of week 7 gained an average of 1.15kg less weight than those receiving placebo (95% CI 0.461.83kg). However, participants who remained abstinent at week 52 experienced a similar overall gain in weight, regardless of treatment group, with bupropion SR-treated subjects gaining an average of 0.9kg more at week 52 (95% CI 1.19 to 2.80kg).
3.3.3. Smoking assessment questionnaire
Responses to the Smoking Assessment Questionnaire were more positive for bupropion SR than placebo in four of the seven questions (Fig. 5). At the end of treatment, 61% of subjects in thebupropion SR group considered that the urge to smoke was not a problem, compared with 37% of those receiving placebo. Both treatment groups generally felt that side effects were not a problem. However, 28% of subjects receiving bupropion SR felt that altered sleeping patterns were a problem compared with 16% for placebo.
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3.4. Safety
A total of 64% (201/313) of subjects receiving bupropion SR and 58% (181/313) of those receiving placebo experienced at least one adverse event whilst on treatment (and 2 weeks thereafter). The most frequently reported events were insomnia (24% bupropion SR; 12% placebo) and dry mouth (18% bupropion SR; 10% placebo) [Table 2]. The frequency with which these events were reported was similar regardless of disease group (CVD or CVD and chronic obstructive pulmonary disease and/or diabetes) or age.
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A total of 36 participants (6%) discontinued from the study due to an adverse event (bupropion SR [5%]; placebo
[6%]) (Table 2). Eight participants experienced a total of nine serious adverse events during the study, and five of these occurred during treatment (bupropion SR
, placebo
). Three events were considered to be possibly a worsening of a preexisting condition, angina pectoris
and vascular disease
. Glaucoma
and lupus erythematodes disseminatus
were also reported. Only one of these events was considered possibly related to study treatment (lupus), and none led to discontinuation of study medication. One event (worsening of congestive heart failure) occurred following the screening visit, prior to the receipt of study medication, in a patient ultimately randomised to placebo.
Within a week of finishing treatment, three serious adverse events were reported. One subject had received bupropion SR during the treatment phase, and the event (vestibular disorder) was not considered to be related to study medication. The two remaining events (chest pain, dyspnoea) were reported by one subject who had received placebo.
There were four deaths during the study (two patients receiving bupropion SR and two receiving placebo), and none was related to study medication. All deaths occurred during the follow-up phase and occurred between 66 and 313 days after the last dose of study medication.
3.4.1. Vital signs
No overall treatment effect was observed in systolic and diastolic blood pressure and heart rate (mean changes in beats per minute from baseline to week 7 were 2.15 and 0.80, for bupropion SR and placebo, respectively). No clinically significant change in vital signs was seen for either treatment during the follow-up phase to week 52. At week 52, the mean change from baseline in systolic blood pressure with bupropion SR and placebo was +1.5 and +3.5mmHg, respectively. The corresponding change from baseline in diastolic blood pressure with bupropion SR was +0.7mmHg compared with +2.2mmHg for placebo.
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4. Discussion |
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Smokers in the present study were recruited in the settings of primary and secondary/tertiary care in addition to smoking cessation clinics. Thus, these smokers were clearly different from smokers recruited to previous studies of bupropion SR conducted in subjects recruited from a general smoking population, with the exception of one study carried out in patients with chronic obstructive pulmonary disease.11 All patients were diagnosed with a cardiovascular condition, over one-quarter were also diagnosed with chronic obstructive pulmonary disease and/or diabetes, and most (96%) were taking concomitant medications. Furthermore, the mean pack year history (49.6 years) and mean number of quit attempts (5.4) were higher than observed in previous bupropion SR studies in general smoking populations.9,10 However, this smoking profile was similar to that of subjects with chronic obstructive pulmonary disease recruited in a more recent bupropion SR study11 in that both of these populations were older, less healthy, had smoked for a longer period of time and made more quit attempts than participants in earlier studies.9,10 In addition, both study populations comprised subjects with chronic smoking histories who continued the habit despite developing smoking-related diseases, and who may therefore be particularly refractory to smoking-cessation treatment.
Bupropion SR was significantly more effective than placebo as an aid to smoking cessation for smokers with CVD and the odds of being continuously abstinent by week 4 and maintaining this until weeks 26 and 52, were around three times greater for bupropion SR. Weekly point prevalence analysis (continuous abstinence 7 days prior to each clinic visit) confirmed these findings, with rates being more than double throughout the study for bupropion SR compared with placebo. Notably, abstinence rates were comparable to those found in previous clinical studies in a general smoking population9,10,12 and to that estimated in a recent meta-analysis conducted by the National Institute for Clinical Excellence. This meta-analysis reported that treatment with bupropion gave an OR of 2.16 (95% CI 1.513.10) for continuous abstinence compared to placebo.17 The institute estimated that nicotine replacement therapy gave an OR of 1.69 (95% CI 1.571.82) compared to placebo.17
The motivational support provided during this study was minimal (1015 min sessions with existing clinical staff) and similar to that provided in previous trials of bupropion SR. Furthermore, the weight gain in subjects treated with bupropion SR was noticeably less than that in the placebo group while they were receiving treatment. This finding is significant because individuals often start smoking again if they gain weight,24 and although the benefit appears to be short term, bupropion SR may help to alleviate this.
Responses to the Smoking Assessment Questionnaire add further support to these central efficacy findings. More than half of subjects confirmed that the urge to smoke was not a problem with bupropion SR, and the majority stated theywould recommend their treatment to others. This is in line with findings from a previous study in 91 chronic smokers, where bupropion SR was found to ameliorate selected nicotine withdrawal effects (difficulty in concentrating, irritability and depression).25
We hypothesised that as the current study examined persistent smokers with serious disease, there may be an increase in the rate of adverse events and in vital sign abnormalities (particularly blood pressure and pulse rate) compared with previous studies of general smoking populations. However, bupropion SR was well tolerated with a safety profile comparable to that seen previously and with few discontinuations due to adverse events. Importantly, although bupropion is a norepinephrine reuptake inhibitor its administration had no impact on vital signs such as blood pressure. There were no cases of seizure or severe hypersensitivity reactions in this study. Each of these adverse events has previously been reported to occur in about 0.1% of subjects treated with bupropion SR,26,27 thus, less than one case of each would be expected in the current study.
In this study we have shown that treatment with bupropion SR can significantly improve rates of smoking abstinence over placebo in a population of smokers with stable CVD who had previously been recalcitrant to quitting. The safety profile and positive patient responses further suggest that bupropion SR is a valuable medication for smoking cessation in smokers with CVD.
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Acknowledgments |
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Australia: Krum H., McKiernan M., Silagy C., Stuckey B. Austria: Irsigler K., Pilger E., Vetter N. Germany: Fritz H., Kaspari S., Krause H., Lindemann L., von Olshausen K. Greece: Chalkidis C., Manolis A., Vardas P. Hungary: Farsang C., Hankóczy J. Netherlands: Deckers J., Meyboom-de-Jong B., van Spiegel P. New Zealand: Kerr D., Rea H. Norway: Aaserud E., Tonstad S. Switzerland: Perruchoud A. UK: Hajek P., Lewis K., Murphy M.
We would also like to thank Professor P. Hajek, at St. Bartholomew's and the Royal London School of Medicine (London, UK) who developed the motivational support programme utilised in this study.
This study was supported by an educational grant from GlaxoSmithKline.
In addition to Dr Tonstad, several other individuals took part in designing the study. Analyses were performed by GlaxoSmithKline, however, all data were available to the authors for analysis. The data interpretation, report writing, and decision to submit the paper have involved all the authors, including those employed by GlaxoSmithKline. Drs Tonstad, Manolis, Perruchoud and Van Spiegel have all received honoraria from GlaxoSmithKline for giving lectures.
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References |
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