Genome-wide association study of varenicline-aided smoking cessation.

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

Nicotine & Tobacco Research Pub Date : 2025-01-10 DOI:10.1093/ntr/ntaf009

Kayesha Coley, Qingning Wang, Richard Packer, Catherine John, Erik Abner, Kadri Reis, Khaled F Bedair, Sundararajan Srinivasan, Sara Paciga, Craig Hyde, Robert C Free, Nicola F Reeve, David J Shepherd, Tõnu Esko, Colin Palmer, Ewan Pearson, Anders Malarstig, Martin D Tobin, Chiara Batini

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引用次数: 0

Abstract

Introduction: Varenicline is an α4β2 nicotinic acetylcholine receptor partial agonist with the highest therapeutic efficacy of any pharmacological smoking cessation aid and a 12-month cessation rate of 26%. Genetic variation may be associated with varenicline response, but to date no genome-wide association studies of varenicline response have been published.

Methods: In this study, we investigated the genetic contribution to varenicline effectiveness using two electronic health record-derived phenotypes. We defined short-term varenicline effectiveness (SVE) and long-term varenicline effectiveness (LVE) by assessing smoking status at 3 and 12 months, respectively, after initiating varenicline treatment. In Stage 1, comprising five European cohort studies, we tested genome-wide associations with SVE (1,405 cases, 2,074 controls) and LVE (1,576 cases, 2,555 controls), defining sentinel variants (the most strongly associated variant within 1 megabase) with p-value <5×10-6 to follow up in Stage 2. In Stage 2, we tested association between sentinel variants and comparable smoking cessation endpoints in varenicline randomised controlled trials. We subsequently meta-analysed Stages 1 and 2.

Results: No variants reached genome-wide significance in the meta-analysis. In Stage 1, 10 sentinel variants were associated with SVE and five with LVE at a suggestive significance threshold (p-value <5×10-6); none of these sentinels were previously implicated in varenicline-aided smoking cessation or in genetic studies of smoking behaviour.

Conclusions: We provide initial insights into the biological underpinnings of varenicline-aided smoking cessation, through implicating genes involved in various processes, including gene expression, cilium assembly and early-stage development.

Implications: Leveraging electronic health records, we undertook the largest genetic study of varenicline-aided smoking cessation to date, and the only such study to test genome-wide associations. We showed distinct genetic variants associated (p-value <5×10-6) with varenicline-aided smoking cessation which implicate diverse cellular functions, including transcriptional regulation, RNA modification and cilium assembly. These provide insights which, if independently corroborated, will improve understanding of varenicline response. The growing availability of biobank resources with genetic and varenicline response data will provide future opportunities for larger studies using the approach we developed.

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伐尼克林辅助戒烟的全基因组关联研究。

Varenicline是一种α4β2烟碱乙酰胆碱受体部分激动剂，在所有药物戒烟辅助药物中疗效最高，12个月戒烟率为26%。遗传变异可能与伐尼克兰反应有关，但迄今为止还没有发表有关伐尼克兰反应的全基因组关联研究。方法：在本研究中，我们利用两种电子健康记录衍生的表型研究了基因对伐尼克兰有效性的影响。我们通过在开始伐尼克兰治疗后3个月和12个月评估吸烟状况来定义伐尼克兰的短期有效性（SVE）和长期有效性（LVE）。在第一阶段，包括五项欧洲队列研究，我们测试了SVE（1,405例，2,074例对照）和LVE（1,576例，2,555例对照）与全基因组的关联，用p值结果定义了哨点变异（1兆碱基内相关性最强的变异）：meta分析中没有变异达到全基因组的显著性。在第一阶段，10个前哨变异与SVE相关，5个与LVE相关，具有提示性的显著阈值（p值）。结论：我们通过涉及基因表达、纤毛组装和早期发育等各种过程的相关基因，初步了解了伐尼克林辅助戒烟的生物学基础。意义：利用电子健康记录，我们进行了迄今为止最大规模的伐尼克林辅助戒烟的遗传研究，也是唯一一项测试全基因组相关性的研究。我们发现明显的遗传变异与（p值）相关

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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.