Department of Health Sciences, University of York, York, UK.
Centre for Research in Health and Development, York, UK.
Cochrane Database Syst Rev. 2024 Aug 5;8(8):CD011120. doi: 10.1002/14651858.CD011120.pub3.
The prevalence of tobacco use among people living with HIV (PLWH) is up to four times higher than in the general population. Unfortunately, tobacco use increases the risk of progression to AIDS and death. Individual- and group-level interventions, and system-change interventions that are effective in helping PLWH stop using tobacco can markedly improve the health and quality of life of this population. However, clear evidence to guide policy and practice is lacking, which hinders the integration of tobacco use cessation interventions into routine HIV care. This is an update of a review that was published in 2016. We include 11 new studies.
To assess the benefits, harms and tolerability of interventions for tobacco use cessation among people living with HIV. To compare the benefits, harms and tolerability of interventions for tobacco use cessation that are tailored to the needs of people living with HIV with that of non-tailored cessation interventions.
We searched the Cochrane Tobacco Addiction Group's Specialised Register, CENTRAL, MEDLINE, Embase, and PsycINFO in December 2022.
We included randomised controlled trials (RCTs) of individual-/group-level behavioural or pharmacological interventions, or both, for tobacco use cessation, delivered directly to PLWH aged 18 years and over, who use tobacco. We also included RCTs, quasi-RCTs, other non-randomised controlled studies (e.g. controlled before and after studies), and interrupted time series studies of system-change interventions for tobacco use cessation among PLWH. For system-change interventions, participants could be PLWH receiving care, or staff working in healthcare settings and providing care to PLWH; but studies where intervention delivery was by research personnel were excluded. For both individual-/group-level interventions, and system-change interventions, any comparator was eligible.
We followed standard Cochrane methods, and used GRADE to assess certainty of the evidence. The primary measure of benefit was tobacco use cessation at a minimum of six months. Primary measures for harm were adverse events (AEs) and serious adverse events (SAEs). We also measured quit attempts or quit episodes, the receipt of a tobacco use cessation intervention, quality of life, HIV viral load, CD4 count, and the incidence of opportunistic infections.
We identified 17 studies (16 RCTs and one non-randomised study) with a total of 9959 participants; 11 studies are new to this update. Nine studies contributed to meta-analyses (2741 participants). Fifteen studies evaluated individual-/group-level interventions, and two evaluated system-change interventions. Twelve studies were from the USA, two from Switzerland, and there were single studies for France, Russia and South Africa. All studies focused on cigarette smoking cessation. All studies received funding from independent national- or institutional-level funding. Three studies received study medication free of charge from a pharmaceutical company. Of the 16 RCTs, three were at low risk of bias overall, five were at high risk, and eight were at unclear risk. Behavioural support or system-change interventions versus no or less intensive behavioural support Low-certainty evidence (7 studies, 2314 participants) did not demonstrate a clear benefit for tobacco use cessation rates in PLWH randomised to receive behavioural support compared with brief advice or no intervention: risk ratio (RR) 1.11, 95% confidence interval (CI) 0.87 to 1.42, with no evidence of heterogeneity. Abstinence at six months or more was 10% (n = 108/1121) in the control group and 11% (n = 127/1193) in the intervention group. There was no evidence of an effect on tobacco use cessation on system-change interventions: calling the quitline and transferring the call to the patient whilst they are still in hospital ('warm handoff') versus fax referral (RR 3.18, 95% CI 0.76 to 13.99; 1 study, 25 participants; very low-certainty evidence). None of the studies in this comparison assessed SAE. Pharmacological interventions versus placebo, no intervention, or another pharmacotherapy Moderate-certainty evidence (2 studies, 427 participants) suggested that varenicline may help more PLWH to quit smoking than placebo (RR 1.95, 95% CI 1.05 to 3.62) with no evidence of heterogeneity. Abstinence at six months or more was 7% (n = 14/215) in the placebo control group and 13% (n = 27/212) in the varenicline group. There was no evidence of intervention effects from individual studies on behavioural support plus nicotine replacement therapy (NRT) versus brief advice (RR 8.00, 95% CI 0.51 to 126.67; 15 participants; very low-certainty evidence), behavioural support plus NRT versus behavioural support alone (RR 1.47, 95% CI 0.92 to 2.36; 560 participants; low-certainty evidence), varenicline versus NRT (RR 0.93, 95% CI 0.48 to 1.83; 200 participants; very low-certainty evidence), and cytisine versus NRT (RR 1.18, 95% CI 0.66 to 2.11; 200 participants; very low-certainty evidence). Low-certainty evidence (2 studies, 427 participants) did not detect a difference between varenicline and placebo in the proportion of participants experiencing SAEs (8% (n = 17/212) versus 7% (n = 15/215), respectively; RR 1.14, 95% CI 0.58 to 2.22) with no evidence of heterogeneity. Low-certainty evidence from one study indicated similar SAE rates between behavioural support plus NRT and behavioural support only (1.8% (n = 5/279) versus 1.4% (n = 4/281), respectively; RR 1.26, 95% CI 0.34 to 4.64). No studies assessed SAEs for the following: behavioural support plus NRT versus brief advice; varenicline versus NRT and cytisine versus NRT.
AUTHORS' CONCLUSIONS: There is no clear evidence to support or refute the use of behavioural support over brief advice, one type of behavioural support over another, behavioural support plus NRT over behavioural support alone or brief advice, varenicline over NRT, or cytisine over NRT for tobacco use cessation for six months or more among PLWH. Nor is there clear evidence to support or refute the use of system-change interventions such as warm handoff over fax referral, to increase tobacco use cessation or receipt of cessation interventions among PLWH who use tobacco. However, the results must be considered in the context of the small number of studies included. Varenicline likely helps PLWH to quit smoking for six months or more compared to control. We did not find evidence of difference in SAE rates between varenicline and placebo, although the certainty of the evidence is low.
HIV 感染者(PLWH)的烟草使用率是普通人群的 4 倍以上。不幸的是,烟草使用会增加进展为艾滋病和死亡的风险。针对 PLWH 的个体和团体层面的干预措施,以及能够有效帮助 PLWH 戒烟的系统层面的干预措施,可以显著改善这一人群的健康和生活质量。然而,缺乏明确的证据来指导政策和实践,这阻碍了将戒烟干预措施纳入常规 HIV 护理。这是对 2016 年发表的一篇综述的更新。我们纳入了 11 项新研究。
评估针对 HIV 感染者的烟草使用戒烟干预措施的益处、危害和耐受性。比较针对 HIV 感染者的需求量身定制的戒烟干预措施与非定制戒烟干预措施的益处、危害和耐受性。
我们于 2022 年 12 月在 Cochrane 烟草成瘾组的专业注册库、CENTRAL、MEDLINE、Embase 和 PsycINFO 中进行了检索。
我们纳入了直接针对年龄在 18 岁及以上、使用烟草的 PLWH 的个体/团体层面的行为或药物干预措施,或两者联合的随机对照试验(RCTs)。我们还纳入了针对 HIV 感染者的烟草使用戒烟的 RCTs、准 RCTs、其他非随机对照研究(如对照前后研究)和系统层面的干预措施的中断时间序列研究。对于系统层面的干预措施,参与者可以是正在接受护理的 PLWH,也可以是在医疗保健环境中为 PLWH 提供护理的工作人员;但干预措施由研究人员实施的研究除外。对于个体/团体层面的干预措施和系统层面的干预措施,任何对照措施都是合格的。
我们遵循了标准的 Cochrane 方法,并使用 GRADE 评估证据的确定性。主要测量指标是至少 6 个月的烟草使用戒烟率。主要的危害指标是不良事件(AE)和严重不良事件(SAE)。我们还测量了戒烟尝试或戒烟事件、接受烟草使用戒烟干预、生活质量、HIV 病毒载量、CD4 计数以及机会性感染的发生率。
我们共纳入了 17 项研究(16 项 RCT 和 1 项非随机研究),共纳入 9959 名参与者;其中 11 项研究是本次更新的新研究。9 项研究参与了荟萃分析(2741 名参与者)。15 项研究评估了个体/团体层面的干预措施,2 项研究评估了系统层面的干预措施。12 项研究来自美国,2 项来自瑞士,还有 1 项来自法国、俄罗斯和南非。所有研究都集中在戒烟上。所有研究都得到了独立的国家或机构层面的资助。有 3 项 RCT 收到了制药公司免费提供的研究药物。在 16 项 RCT 中,有 3 项总体上具有低偏倚风险,5 项具有高偏倚风险,8 项具有不确定偏倚风险。
低确定性证据(7 项研究,2314 名参与者)并没有表明,与简短建议或不干预相比,PLWH 接受行为支持的戒烟率有明显的增加:风险比(RR)1.11,95%置信区间(CI)0.87 至 1.42,无明显的异质性。在对照组中,6 个月或更长时间的戒烟率为 10%(n=108/1121),在干预组中为 11%(n=127/1193)。没有证据表明系统层面的干预措施对戒烟有影响:呼叫戒烟热线并在患者仍在住院时将电话转接给患者(RR 3.18,95%CI 0.76 至 13.99;1 项研究,25 名参与者;极低确定性证据)。没有一项比较研究评估 SAE。
药物干预与安慰剂、无干预或其他药物治疗相比:中等确定性证据(2 项研究,427 名参与者)表明,与安慰剂相比,伐伦克林可能有助于更多的 PLWH 戒烟(RR 1.95,95%CI 1.05 至 3.62),无明显的异质性。在安慰剂对照组中,6 个月或更长时间的戒烟率为 7%(n=14/215),在伐伦克林组中为 13%(n=27/212)。没有来自单个研究的干预效果证据表明,行为支持加尼古丁替代疗法(NRT)与简短建议(RR 8.00,95%CI 0.51 至 126.67;15 名参与者;极低确定性证据)、行为支持加 NRT 与行为支持单独(RR 1.47,95%CI 0.92 至 2.36;560 名参与者;低确定性证据)、伐伦克林与 NRT(RR 0.93,95%CI 0.48 至 1.83;200 名参与者;极低确定性证据)和 Cytisine 与 NRT(RR 1.18,95%CI 0.66 至 2.11;200 名参与者;极低确定性证据)之间存在差异。中等确定性证据(2 项研究,427 名参与者)未发现伐伦克林与安慰剂在参与者经历 SAE 的比例上存在差异(8%(n=17/212)与 7%(n=15/215),RR 1.14,95%CI 0.58 至 2.22),无明显的异质性。一项低确定性研究表明,在行为支持加 NRT 与行为支持加 NRT 之间,SAE 发生率相似(1.8%(n=5/279)与 1.4%(n=4/281),RR 1.26,95%CI 0.34 至 4.64)。没有研究评估行为支持加 NRT 与简短建议、伐伦克林与 NRT 和 Cytisine 与 NRT 之间的 SAE。
没有明确的证据支持或反驳在 PLWH 中使用行为支持而不是简短建议、一种行为支持而不是另一种、行为支持加 NRT 而不是行为支持单独或简短建议来增加戒烟 6 个月或更长时间的戒烟率。也没有明确的证据支持或反驳在 PLWH 中使用系统层面的干预措施,如热交线,以增加烟草使用戒烟或接受戒烟干预的可能性。然而,必须考虑到纳入研究的数量较少。伐伦克林可能有助于 PLWH 在 6 个月或更长时间内戒烟。我们没有发现伐伦克林和安慰剂之间在 SAE 率方面的差异,尽管证据的确定性较低。
