Department of Pharmaceutics, University of Washington, Seattle, WA.
Research Department, Southcentral Foundation, Anchorage, AK.
Nicotine Tob Res. 2020 May 26;22(6):910-918. doi: 10.1093/ntr/ntz105.
Alaska Native and American Indian (AN/AI) populations have higher tobacco use prevalence than other ethnic/racial groups. Pharmacogenetic testing to tailor tobacco cessation treatment may improve cessation rates. This study characterized polymorphic variations among AN/AI people in genes associated with metabolism of nicotine and drugs used for tobacco cessation.
Recruitment of AN/AI individuals represented six subgroups, five geographic subgroups throughout Alaska and a subgroup comprised of AIs from the lower 48 states living in Alaska. We sequenced the CYP2A6 and CYP2B6 genes to identify known and novel gain, reduced, and loss-of-function alleles, including structural variation (eg, gene deletions, duplications, and hybridizations).
Variant allele frequencies differed substantially between AN/AI subgroups. The gene deletion CYP2A64 and reduced function CYP2A69 alleles were found at high frequency in Northern/Western subgroups and in Lower 48/Interior subgroups, respectively. The reduced function CYP2B6*6 allele was observed in all subgroups and a novel, predicted reduced function CYP2B6 variant was found at relatively high frequency in the Southeastern subgroup.
Diverse CYP2A6 and CYP2B6 variation among the subgroups highlight the need for comprehensive pharmacogenetic testing to guide tobacco cessation therapy for AN/AI populations.
Nicotine metabolism is largely determined by CYP2A6 genotype, and variation in CYP2A6 activity has altered the treatment success in other populations. These findings suggest pharmacogenetic-guided smoking cessation drug treatment could provide benefit to this unique population seeking tobacco cessation therapy.
阿拉斯加原住民和美洲印第安人(AN/AI)的烟草使用流行率高于其他族裔/种族群体。针对代谢尼古丁和用于戒烟的药物的基因进行遗传药理学测试可能会提高戒烟率。本研究描述了与尼古丁代谢和用于戒烟的药物相关的基因中存在于 AN/AI 人群中的多态性变异。
招募的 AN/AI 个体代表六个亚组,五个分布在整个阿拉斯加的地理亚组和一个由居住在阿拉斯加的来自下 48 个州的美洲印第安人组成的亚组。我们对 CYP2A6 和 CYP2B6 基因进行测序,以确定已知和新的获得、减少和功能丧失等位基因,包括结构变异(例如基因缺失、重复和杂交)。
AN/AI 亚组之间的变异等位基因频率差异很大。Northern/Western 亚组和 Lower 48/Interior 亚组分别存在 CYP2A64 基因缺失和 CYP2A69 功能降低等位基因。所有亚组都观察到降低功能的 CYP2B6*6 等位基因,并且在 Southeastern 亚组中发现了一种新型的、预测降低功能的 CYP2B6 变体,其频率相对较高。
亚组之间 CYP2A6 和 CYP2B6 的多样性变异突出表明,需要进行全面的遗传药理学测试,以指导 AN/AI 人群的戒烟治疗。
尼古丁代谢在很大程度上取决于 CYP2A6 基因型,CYP2A6 活性的变异改变了其他人群的治疗成功率。这些发现表明,基于遗传药理学的戒烟药物治疗可能会为寻求戒烟治疗的这一独特人群带来益处。
