Can We Predict Who Will Experience Adverse Events While Using Smoking Cessation Pharmacotherapy? A Secondary Analysis of the EAGLES Clinical Trial.

IF 3 2区医学 Q2 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH

Nicotine & Tobacco Research Pub Date : 2024-12-10 DOI:10.1093/ntr/ntae290

Bethany J Wolf, Kevin M Gray, Jennifer R Dahne, Daniel Hashemi, Rachel L Tomko

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引用次数: 0

Abstract

Introduction: Concerns about potential side effects remain a barrier to uptake of Food and Drug Administration (FDA)-approved smoking cessation pharmacotherapy [i.e., varenicline, bupropion, nicotine replacement therapy (NRT)]. However, use of pharmacotherapy can double the odds of successful quitting. Knowledge of an individual's likelihood of side effects while taking smoking cessation pharmacotherapy could influence treatment planning discussions and monitoring.

Methods: We conducted a secondary, post-hoc analysis to predict an individual's likelihood of adverse events (AEs) using the Evaluating Adverse Events in a Global Smoking Cessation Study (EAGLES) data from 4,209 adults in the United States who smoked. Participants were randomized to receive 12 weeks of treatment with varenicline, bupropion, NRT patch, or placebo. Our models predicted the likelihood of moderate to severe psychiatric and non-psychiatric AEs during treatment.

Results: Using pre-treatment demographic and clinical data, multivariable logistic regression models yielded acceptable areas under the receiver operating characteristic curve for an individual's likelihood of moderate to severe 1) psychiatric AEs for bupropion and NRT and 2) non-psychiatric AEs for varenicline and bupropion. Once we adjusted for demographic and baseline characteristics, medication was not associated with psychiatric AEs. Varenicline differed from placebo with regards to non-psychiatric AEs.

Conclusions: It is possible to predict person-specific likelihood of moderate to severe psychiatric and non-psychiatric AEs during smoking cessation treatment, though the probability of psychiatric AEs did not differ by medication. Future work should consider factors related to implementation in clinical settings, including determining whether lower burden assessment protocols can be equally accurate for AE prediction.

Implications: Using data from a large dataset people who smoke in the U.S., it is possible to predict an individual's likelihood of psychiatric and non-psychiatric adverse events during smoking cessation treatment prior to initiating treatment. These predictive models provide a starting point for future work addressing how best to modify and integrate such clinical decision support algorithms into treatment for smoking cessation.

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我们能预测哪些人在使用戒烟药物治疗时会出现不良事件吗？eagle临床试验的二次分析。

对潜在副作用的担忧仍然是美国食品和药物管理局（FDA）批准的戒烟药物治疗的障碍[即，伐尼克兰，安非他酮，尼古丁替代疗法（NRT）]。然而，使用药物疗法可以使成功戒烟的几率加倍。在接受戒烟药物治疗时，了解个人可能出现的副作用会影响治疗计划、讨论和监测。方法：我们使用来自美国4,209名吸烟成人的不良事件评估全球戒烟研究（EAGLES）数据进行了二次事后分析，以预测个人不良事件（ae）的可能性。参与者被随机分配接受为期12周的伐尼克兰、安非他酮、NRT贴片或安慰剂治疗。我们的模型预测了治疗期间出现中度至重度精神和非精神不良事件的可能性。结果：使用治疗前的人口学和临床数据，多变量logistic回归模型在受试者工作特征曲线下产生了可接受区域，用于个体中度至重度的可能性：1)安非他酮和NRT的精神性不良事件；2)伐尼克兰和安非他酮的非精神性不良事件。一旦我们调整了人口统计学和基线特征，药物治疗与精神病学不良事件无关。伐尼克兰与安慰剂在非精神不良事件方面有所不同。结论：有可能预测戒烟治疗期间发生中度至重度精神和非精神不良事件的个体特异性可能性，尽管精神不良事件的概率没有因药物而异。未来的工作应考虑与临床环境实施相关的因素，包括确定较低负担评估方案是否同样准确地预测AE。含义：利用来自美国吸烟者的大型数据集的数据，可以在开始治疗之前预测个体在戒烟治疗期间出现精神和非精神不良事件的可能性。这些预测模型为未来的工作提供了一个起点，解决如何最好地修改和整合这些临床决策支持算法到戒烟治疗中。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Nicotine & Tobacco Research 医学-公共卫生、环境卫生与职业卫生

CiteScore

8.10

自引率

10.60%

发文量

268

审稿时长

3-8 weeks

期刊介绍： Nicotine & Tobacco Research is one of the world''s few peer-reviewed journals devoted exclusively to the study of nicotine and tobacco. It aims to provide a forum for empirical findings, critical reviews, and conceptual papers on the many aspects of nicotine and tobacco, including research from the biobehavioral, neurobiological, molecular biologic, epidemiological, prevention, and treatment arenas. Along with manuscripts from each of the areas mentioned above, the editors encourage submissions that are integrative in nature and that cross traditional disciplinary boundaries. The journal is sponsored by the Society for Research on Nicotine and Tobacco (SRNT). It publishes twelve times a year.