Department of Behavioral Science, University of Texas MD Anderson Cancer Center, Houston.
Center for Clinical Research and Evidence-Based Medicine, Department of Pediatrics, University of Texas at Houston Health Sciences Center, Houston.
JAMA. 2024 May 28;331(20):1722-1731. doi: 10.1001/jama.2024.4183.
Most people who smoke do not quit on their initial attempt.
To determine the best subsequent strategy for nonabstinence following initial treatment with varenicline or combined nicotine replacement therapy (CNRT).
DESIGN, SETTING, AND PARTICIPANTS: Using a double-blind, placebo-controlled, sequential multiple assignment randomized trial, 490 volunteers were randomized to receive 6 weeks of varenicline or CNRT. After 6 weeks, nonabstainers were rerandomized to continue, switch, or increase medication dosage for 6 additional weeks. The study was conducted from June 2015 through October 2019 in a Texas tobacco treatment clinic.
The initial treatment was 2 mg/d of varenicline or the combined replacement therapy of a 21-mg patch plus 2-mg lozenge. The rerandomized participants either continued with their initial therapies, switched between varenicline and CNRT, or increased dosages either to 3-mg or more of varenicline or to a 42-mg patch and lozenges. All received weekly brief counseling.
Biochemically verified 7-day point prevalence abstinence at the end of treatment at 12 weeks.
The 490 randomized participants (210 female [43%], 287 non-Hispanic White [58%], mean age, 48.1 years) smoked an average of 20 cigarettes per day. After the first phase, 54 participants in the CNRT group were abstinent and continued their therapy; of the 191 who were not abstinent, 151 were rerandomized, and the 40 who did not return for rerandomization were assigned to continue their initial CNRT condition in phase 2. The end-of-treatment abstinence rate for the 191 phase 1 nonabstainers was 8% (95% credible interval [CrI], 6% to 10%) for the 90 (47%) who continued at the dosage condition, 14% (CrI, 10% to 18%) for the 50 (33%) who increased their dosage, and 14% (95% CrI, 10% to 18%) for the 51 (34%) who switched to varenicline (absolute risk difference [RD], 6%; 95% CrI, 6% to 11%) with more than 99% posterior probability that either strategy conferred benefit over continuing the initial dosage. After the first phase, 88 participants in the varenicline group were abstinent and continued their therapy; of the 157 who were not abstinent, 122 were rerandomized and 35 who did not return for rerandomization were assigned to continue with the varenicline condition. The end-of-treatment abstinence rate for the 157 phase 1 nonabstainers was 20% (95% CrI, 16% to 26%) for the 39 (32%) who increased their varenicline dosage, 0 (95% CrI, 0 to 0) for the 41 (34%) who switched CNRT, and 3% (95% CrI, 1% to 4%) for the 77 (49%) who were assigned to the continued varenicline condition (absolute RD, -3%; 95% CrI, -4% to -1%) with more than 99% posterior probability that continuing varenicline at the initial dosage was worse than switching to a higher dosage. Furthermore, increasing the varenicline dosage had an absolute RD of 18% (95% CrI, 13% to 24%) and a more than 99% posterior probability of conferring benefit. The secondary outcome of continuous abstinence at 6 months indicated that only increased dosages of the CNRT and varenicline provided benefit over continuation of the initial treatment dosages.
For individuals who smoked but did not achieve abstinence after treatment with varenicline, increasing the dosage enhanced abstinence vs continuing, whereas for nonabstainers initially treated with CNRT, a dosage increase or switch to varenicline enhanced abstinence and may be viable rescue strategies.
ClinicalTrials.gov Identifier: NCT02271919.
大多数尝试初始治疗的吸烟者并未戒烟。
确定在使用伐尼克兰或联合尼古丁替代疗法(CNRT)初始治疗后非戒断的最佳后续策略。
设计、设置和参与者:使用双盲、安慰剂对照、连续多次分配随机试验,490 名志愿者被随机分配接受 6 周的伐尼克兰或 CNRT 治疗。6 周后,非戒烟者被重新随机分配继续、转换或增加 6 周的药物剂量。该研究于 2015 年 6 月至 2019 年 10 月在德克萨斯州的一家烟草治疗诊所进行。
初始治疗为 2 毫克/天的伐尼克兰或 21 毫克贴片加 2 毫克含片的联合替代治疗。重新随机的参与者要么继续他们的初始治疗,要么在伐尼克兰和 CNRT 之间切换,要么增加剂量至 3 毫克或更多的伐尼克兰或 42 毫克贴片和含片。所有患者每周接受一次简短的咨询。
治疗结束时(12 周),通过生物化学验证的 7 天点患病率(即 12 周)。
490 名随机参与者(210 名女性[43%],287 名非西班牙裔白人[58%],平均年龄 48.1 岁)平均每天吸烟 20 支。在第一阶段后,CNRT 组中有 54 名参与者戒烟并继续治疗;在 191 名未戒烟者中,有 151 人被重新随机分配,而未返回重新随机分配的 40 人被分配在第二阶段继续接受他们的初始 CNRT 治疗。在 191 名第一阶段未戒烟者中,90 名(47%)继续按剂量治疗者的戒烟率为 8%(95%可信区间[CrI],6%至 10%),50 名(33%)增加剂量者为 14%(CrI,10%至 18%),51 名(34%)转换为伐尼克兰者为 14%(95%CrI,10%至 18%)(绝对风险差异[RD],6%;95%CrI,6%至 11%),超过 99%的后验概率表明这两种策略均优于继续初始剂量。在第一阶段后,88 名伐尼克兰组参与者戒烟并继续治疗;在 157 名未戒烟者中,有 122 人被重新随机分配,35 人未返回重新随机分配被分配继续接受伐尼克兰治疗。在 157 名第一阶段非戒烟者中,39 名(32%)增加伐尼克兰剂量者的戒烟率为 20%(95%CrI,16%至 26%),41 名(34%)转换为 CNRT 者为 0(95%CrI,0 至 0),77 名(49%)继续接受伐尼克兰治疗者为 3%(95%CrI,1%至 4%)(绝对 RD,-3%;95%CrI,-4%至-1%),超过 99%的后验概率表明继续初始剂量的伐尼克兰治疗比转换为更高剂量的伐尼克兰治疗更差。此外,增加伐尼克兰剂量的绝对 RD 为 18%(95%CrI,13%至 24%),并且超过 99%的后验概率表明有获益。次要结局为 6 个月时的连续戒烟,表明仅增加 CNRT 和伐尼克兰的剂量可提供比继续初始治疗剂量更好的效果。
对于使用伐尼克兰治疗后未戒烟的吸烟者,增加剂量可提高戒烟率,而对于初始接受 CNRT 治疗的非戒烟者,增加剂量或转换为伐尼克兰可提高戒烟率,可能是可行的挽救策略。
ClinicalTrials.gov 标识符:NCT02271919。
