Stead Lindsay F, Lancaster Tim
Department of Primary Care Health Sciences, University of Oxford, Oxford, UK.
Cochrane Database Syst Rev. 2012 Oct 17;10:CD008286. doi: 10.1002/14651858.CD008286.pub2.
Both behavioural support (including brief advice and counselling) and pharmacotherapies (including nicotine replacement therapy (NRT), varenicline and bupropion) are effective in helping people to stop smoking. Combining both treatment approaches is recommended where possible, but the size of the treatment effect with different combinations and in different settings and populations is unclear.
To assess the effect of combining behavioural support and medication to aid smoking cessation, compared to a minimal intervention or usual care, and to identify whether there are different effects depending on characteristics of the treatment setting, intervention, population treated, or take-up of treatment.
We searched the Cochrane Tobacco Addiction Group Specialised Register in July 2012 for records with any mention of pharmacotherapy, including any type of NRT, bupropion, nortriptyline or varenicline.
Randomized or quasi-randomized controlled trials evaluating combinations of pharmacotherapy and behavioural support for smoking cessation, compared to a control receiving usual care or brief advice or less intensive behavioural support. We excluded trials recruiting only pregnant women, trials recruiting only adolescents, and trials with less than six months follow-up.
Search results were prescreened by one author and inclusion or exclusion of potentially relevant trials was agreed by both authors. Data was extracted by one author and checked by the other.The main outcome measure was abstinence from smoking after at least six months of follow-up. We used the most rigorous definition of abstinence for each trial, and biochemically validated rates if available. We calculated the risk ratio (RR) and 95% confidence interval (CI) for each study. Where appropriate, we performed meta-analysis using a Mantel-Haenszel fixed-effect model.
Forty-one studies with a total of more than 20,000 participants met the inclusion criteria. A large proportion of studies recruited people in healthcare settings or with specific health needs. Most studies provided NRT. Behavioural support was typically provided by specialists in cessation counselling, who offered between four and eight contact sessions. The planned maximum duration of contact was typically more than 30 minutes but less than 300 minutes. Overall, studies were at low or unclear risk of bias, and findings were not sensitive to the exclusion of any of the three studies rated at high risk of bias in one domain. One large study (the Lung Health Study) contributed heterogeneity due to a substantially larger treatment effect than seen in other studies (RR 3.88, 95% CI 3.35 to 4.50). Since this study used a particularly intensive intervention which included extended availability of nicotine gum, multiple group sessions and long term maintenance and recycling contacts, the results may not be comparable with the interventions used in other studies, and hence it was not pooled in other analyses. Based on the remaining 40 studies (15,021 participants) there was good evidence for a benefit of combination pharmacotherapy and behavioural treatment compared to usual care or brief advice or less intensive behavioural support (RR 1.82, 95% CI 1.66 to 2.00) with moderate statistical heterogeneity (I² = 40%). The pooled estimate for 31 trials that recruited participants in healthcare settings (RR 2.06, 95% CI 1.81 to 2.34) was higher than for eight trials with community-based recruitment (RR 1.53, 95% CI 1.33 to 1.76). Pooled estimates were lower in a subgroup of trials where the behavioural intervention was provided by specialist counsellors versus trials where counselling was linked to usual care (specialist: RR 1.73, 95% CI 1.55 to 1.93, 28 trials; usual provider: RR 2.41, 95% CI 1.91 to 3.02, 8 trials) but this was largely attributable to the small effect size in two trials using specialist counsellors where the take-up of the planned intervention was low, and one usual provider trial with alarge effect. There was little indirect evidence that the relative effect of an intervention differed according to whether participants in a trial were required to be motivated to make a quit attempt or not. There was only weak evidence that studies offering more sessions had larger effects and there was not clear evidence that increasing the duration of contact increased the effect, but there was more evidence of a dose-response relationship when analyses were limited to trials where the take-up of treatment was high.
AUTHORS' CONCLUSIONS: Interventions that combine pharmacotherapy and behavioural support increase smoking cessation success compared to a minimal intervention or usual care. Further trials would be unlikely to change this conclusion. We did not find strong evidence from indirect comparisons that offering more intensive behavioural support was associated with larger treatment effects but this could be because intensive interventions are less likely to be delivered in full.
行为支持(包括简短建议和咨询)和药物治疗(包括尼古丁替代疗法(NRT)、伐尼克兰和安非他酮)在帮助人们戒烟方面均有效。建议尽可能将两种治疗方法结合使用,但不同组合以及在不同环境和人群中的治疗效果大小尚不清楚。
评估与最低限度干预或常规护理相比,联合行为支持和药物治疗辅助戒烟的效果,并确定根据治疗环境、干预措施、治疗人群或治疗接受情况的特征是否存在不同效果。
我们于2012年7月检索了Cochrane烟草成瘾小组专业注册库,以查找任何提及药物治疗的记录,包括任何类型的NRT、安非他酮、去甲替林或伐尼克兰。
评估药物治疗与行为支持相结合用于戒烟的随机或半随机对照试验,与接受常规护理、简短建议或强度较低的行为支持的对照组进行比较。我们排除了仅招募孕妇的试验、仅招募青少年的试验以及随访时间少于六个月的试验。
检索结果由一位作者进行预筛选,两位作者共同商定纳入或排除潜在相关试验。数据由一位作者提取,另一位作者进行核对。主要结局指标是至少随访六个月后的戒烟情况。我们对每个试验使用最严格的戒烟定义,如有可用则采用生化验证率。我们计算了每项研究的风险比(RR)和95%置信区间(CI)。在适当情况下,我们使用Mantel-Haenszel固定效应模型进行荟萃分析。
41项研究共纳入20,000多名参与者,符合纳入标准。很大一部分研究招募了医疗机构中的人群或有特定健康需求的人群。大多数研究提供了NRT。行为支持通常由戒烟咨询专家提供,他们提供4至8次接触性咨询。计划的最大接触时长通常超过30分钟但少于300分钟。总体而言,研究的偏倚风险较低或不明确,且研究结果对排除在一个领域中被评为高偏倚风险的三项研究中的任何一项均不敏感。一项大型研究(肺部健康研究)造成了异质性,因为其治疗效果比其他研究大得多(RR 3.88,95%CI 3.35至4.50)。由于该研究使用了特别强化的干预措施,包括延长尼古丁口香糖的供应、多次小组咨询以及长期维持和循环接触,其结果可能与其他研究中使用的干预措施不可比,因此未纳入其他分析。基于其余40项研究(15,021名参与者),有充分证据表明与常规护理、简短建议或强度较低的行为支持相比,联合药物治疗和行为治疗有益(RR 1.82,95%CI 1.66至2.00),具有中度统计学异质性(I² = 40%)。在医疗机构招募参与者的31项试验的合并估计值(RR 2.06,95%CI 1.81至2.34)高于在社区招募的8项试验(RR 1.53,95%CI 1.33至1.76)。在行为干预由专家顾问提供的试验亚组中,合并估计值低于咨询与常规护理相关的试验(专家:RR 1.73,95%CI 1.55至1.93,28项试验;常规提供者:RR 2.41,95%CI 1.91至3.02,8项试验),但这主要归因于两项使用专家顾问的试验中计划干预的接受率较低导致的小效应量,以及一项常规提供者试验中的大效应。几乎没有间接证据表明干预的相对效果因试验参与者是否需要有戒烟动机而有所不同。仅有微弱证据表明提供更多咨询次数的研究有更大效果,且没有明确证据表明增加接触时长会增加效果,但当分析仅限于治疗接受率高的试验时,有更多剂量反应关系的证据。
与最低限度干预或常规护理相比,联合药物治疗和行为支持的干预措施可提高戒烟成功率。进一步的试验不太可能改变这一结论。我们没有从间接比较中找到有力证据表明提供更强化的行为支持与更大的治疗效果相关,但这可能是因为强化干预不太可能完全实施。
