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祖源基因分型在激素避孕药物基因组学研究中的适用性。

Applicability of ancestral genotyping in pharmacogenomic research with hormonal contraception.

机构信息

Division of Family Planning, Department of Obstetrics and Gynecology, University of Colorado Anschutz Medical Campus, Aurora, Colorado, USA.

Skaggs School of Pharmacy and Pharmaceutical Sciences, Department of Pharmaceutical Sciences, University of Colorado Anschutz Medical Campus, Aurora, Colorado, USA.

出版信息

Clin Transl Sci. 2021 Sep;14(5):1713-1718. doi: 10.1111/cts.13014. Epub 2021 May 2.

Abstract

To compare etonogestrel pharmacokinetic and pharmacodynamic outcomes by both self-reported race/ethnicity and genetically determined ancestry among contraceptive implant users. We conducted a secondary analysis of our parent pharmacogenomic study of 350 implant users. We genotyped these reproductive-aged (18-45 years) women for 88 ancestry-informative single nucleotide polymorphisms. We then assigned each participant a proportion value for African (AFR), European (EUR), and Indigenous American (AMR) ancestry based on reference population data. We correlated genetic ancestry with self-reported race/ethnicity and utilized genetic ancestry proportion values as variables for previously performed association analyses with serum etonogestrel concentrations and progestin-related side effects (e.g., bothersome bleeding and subjective weight gain). We successfully estimated genetically determined ancestry for 332 participants. EUR, AFR, and AMR ancestry were each highly correlated with self-reported White/non-Hispanic race (r = 0.64, p = 4.14 × 10 ), Black/African American race (r = 0.88, p = 1.36 × 10 ), and Hispanic/Latina ethnicity (r = 0.68, p = 4.03 × 10 ), respectively. Neither genetically determined ancestry nor self-reported race/ethnicity were significantly associated with serum etonogestrel concentrations. AFR ancestry and self-reported Black race had similar associations with reporting monthly periods (odds ratio [OR] 2.18, p = 0.09 vs. OR 2.22, p = 0.02) and having received treatment for bothersome bleeding (OR 5.19, p = 0.005 vs. OR 4.73, p = 2.0 × 10 ). In multivariable logistic regression for subjective weight gain, AMR ancestry dropped out of the model in preference for self-reported Hispanic/Latina ethnicity. We found no new associations between genetically determined ancestry and contraceptive implant pharmacodynamics/pharmacokinetics. Self-reported race/ethnicity were strong surrogates for genetically determined ancestry among this population of contraceptive implant users. Our data suggest that self-reported race/ethnicity, capturing societal and cultural aspects, remain important to the investigation of progestin-related side effects.

摘要

比较使用避孕植入物的人群中自我报告的种族/民族和遗传确定的祖先对依托孕烯药代动力学和药效学结果的影响。我们对我们的父母药物基因组学研究中的 350 名植入物使用者进行了二次分析。我们对这些育龄(18-45 岁)女性进行了 88 个与祖先相关的单核苷酸多态性基因分型。然后,我们根据参考人群数据为每位参与者分配了非洲裔(AFR)、欧洲裔(EUR)和美洲原住民(AMR)祖先的比例值。我们将遗传祖先与自我报告的种族/民族相关联,并利用遗传祖先比例值作为先前与血清依托孕烯浓度和孕激素相关副作用(如令人烦恼的出血和主观体重增加)进行关联分析的变量。我们成功地为 332 名参与者估计了遗传决定的祖先。EUR、AFR 和 AMR 祖先与自我报告的白人/非西班牙裔种族(r=0.64,p=4.14×10-4)、黑人/非裔美国人种族(r=0.88,p=1.36×10-8)和西班牙裔/拉丁裔种族(r=0.68,p=4.03×10-4)分别高度相关。遗传确定的祖先和自我报告的种族/民族与血清依托孕烯浓度均无显著相关性。AFR 祖先和自我报告的黑人种族与报告每月经期(比值比[OR]2.18,p=0.09 与 OR 2.22,p=0.02)和接受治疗以缓解出血问题(OR 5.19,p=0.005 与 OR 4.73,p=2.0×10-4)具有相似的相关性。在多变量逻辑回归中,对于主观体重增加,AMR 祖先被自我报告的西班牙裔/拉丁裔种族所取代。我们在避孕植入物药代动力学/药效学的遗传决定的祖先之间没有发现新的关联。在这群避孕植入物使用者中,自我报告的种族/民族是遗传决定的祖先的有力替代品。我们的数据表明,自我报告的种族/民族,捕捉社会和文化方面,仍然是孕激素相关副作用研究的重要因素。

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