Adis, a Wolters Kluwer Business, Auckland, New Zealand.
Pharmacoeconomics. 2010;28(3):231-54. doi: 10.2165/11204380-000000000-00000.
Varenicline (Chantix, Champix) is an orally administered alpha4beta2 nicotinic acetylcholine receptor partial agonist that is indicated as an aid to smoking cessation. Well designed clinical trials indicate that varenicline is an effective aid to smoking cessation. During the last 4 weeks of treatment, carbon monoxide-confirmed continuous abstinence rates were generally significantly higher with varenicline than with placebo, bupropion sustained release (SR) or nicotine replacement therapy. Varenicline also reduced cravings, the reinforcing effects of smoking and some withdrawal symptoms. Another well designed trial demonstrated that extending varenicline therapy by an additional 12 weeks helped maintain abstinence in individuals who had quit smoking. Varenicline was generally well tolerated in clinical trials; nausea, the most commonly occurring adverse event, diminished over time. More data are needed regarding the potential for neuropsychiatric events in varenicline recipients. Some of these events may be associated with nicotine withdrawal, rather than varenicline, although neuropsychiatric events have been observed in individuals who continued to smoke whilst receiving varenicline. In modelled cost-effectiveness analyses based on data from clinical trials in participants receiving smoking cessation therapy, 12 weeks' treatment with varenicline was predicted to be cost effective from a healthcare payer perspective in numerous countries. With regard to the incremental costs per QALY or life-year gained, 12 weeks' treatment with varenicline consistently dominated bupropion SR and nicotine replacement therapy and was dominant over or considered cost effective relative to unaided cessation, regular brief counselling or nortriptyline in analyses based on Markov models. In additional modelled analyses from a healthcare payer perspective, administering varenicline for an additional 12 weeks in participants who had successfully quit smoking was estimated to have acceptable incremental costs per QALY gained relative to varenicline for 12 weeks and to dominate other smoking cessation options. Moreover, in Swedish analyses that also included societal costs for production and consumption, the incremental cost per QALY gained for varenicline versus bupropion SR, and for an additional 12 weeks of varenicline therapy versus varenicline for 12 weeks only, was below commonly accepted thresholds of cost effectiveness. A US decision-analytic model from the perspective of various US health insurance plans demonstrated that, after 2 years, varenicline was predicted to dominate bupropion SR, in terms of the incremental cost per additional smoking cessation. Varenicline was also dominant or cost effective versus nicotine replacement therapy, and cost effective versus unaided cessation. Sensitivity analyses demonstrated that the results of cost-effectiveness studies were generally robust to plausible variations in key parameters. In conclusion, varenicline is an effective aid to smoking cessation. Varenicline was generally well tolerated in clinical trials, although more data are needed regarding the potential for neuropsychiatric events. The costs associated with varenicline are offset by direct savings associated with the reduction in smoking-related diseases. Despite their limitations, available pharmacoeconomic analyses from numerous countries support the use of varenicline for 12 or 24 weeks as a cost-effective treatment relative to other smoking cessation therapies in smokers who wish to quit smoking.
伐伦克林(Chantix,Champix)是一种口服给予的α4β2 烟碱型乙酰胆碱受体部分激动剂,被批准作为戒烟的辅助治疗药物。精心设计的临床试验表明,伐伦克林是一种有效的戒烟辅助治疗药物。在治疗的最后 4 周,与安慰剂、安非他酮缓释剂(bupropion sustained release,SR)或尼古丁替代疗法相比,使用伐伦克林治疗的患者,经一氧化碳证实的持续戒烟率通常显著更高。伐伦克林还可减轻烟瘾、吸烟的强化作用和一些戒断症状。另一项精心设计的试验表明,将伐伦克林治疗时间延长 12 周有助于维持已戒烟患者的戒烟状态。伐伦克林在临床试验中通常具有良好的耐受性;最常发生的不良反应是恶心,随着时间的推移会逐渐减轻。需要更多数据来评估接受伐伦克林治疗者出现神经精神事件的潜在风险。其中一些事件可能与尼古丁戒断有关,而不是与伐伦克林有关,尽管在继续吸烟的同时接受伐伦克林治疗的患者中观察到了神经精神事件。基于接受戒烟治疗的参与者临床试验数据进行的基于模型的成本效益分析预测,在许多国家,从医疗保健支付者的角度来看,12 周的伐伦克林治疗在成本效益方面具有优势。关于每增加一个质量调整生命年(quality-adjusted life-year,QALY)或生命年的增量成本,在基于马尔可夫模型的分析中,12 周的伐伦克林治疗始终优于安非他酮 SR 和尼古丁替代疗法,并且与未辅助戒烟、常规简短咨询或曲米帕明相比,具有优势或被认为具有成本效益。在基于医疗保健支付者视角的其他基于模型的分析中,在成功戒烟的参与者中再给予伐伦克林治疗 12 周,估计相对于 12 周的伐伦克林治疗和其他戒烟选择,每增加一个 QALY 的增量成本是可以接受的。此外,在包括生产和消费社会成本的瑞典分析中,与安非他酮 SR 相比,伐伦克林的增量成本每 QALY 获得,以及与仅接受 12 周伐伦克林治疗相比,接受 12 周伐伦克林治疗加 12 周治疗的增量成本,均低于通常可接受的成本效益阈值。来自各种美国健康保险计划的美国决策分析模型表明,在 2 年后,与安非他酮 SR 相比,预计伐伦克林在额外的戒烟方面具有成本效益优势。伐伦克林也优于或具有成本效益,优于尼古丁替代疗法和未辅助戒烟。敏感性分析表明,成本效益研究的结果通常对关键参数的合理变化具有稳健性。总之,伐伦克林是一种有效的戒烟辅助治疗药物。伐伦克林在临床试验中通常具有良好的耐受性,尽管需要更多数据来评估神经精神事件的潜在风险。与吸烟相关疾病减少相关的直接节省抵消了与伐伦克林相关的成本。尽管存在局限性,但来自许多国家的可用药物经济学分析支持在希望戒烟的吸烟者中,将伐伦克林治疗 12 周或 24 周作为一种比其他戒烟疗法更具成本效益的治疗方法。
