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A pharmacokinetic and pharmacogenetic evaluation of contraceptive implants and antiretroviral therapy among women in Kenya and Uganda

机译:肯尼亚和乌干达妇女避孕药植入物和抗逆转录病毒治疗的药代动力学和药代理评价

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Objectives: To evaluate pharmacokinetics and pharmacogenetics of contraceptive implant progestin concentrations in HIV-positive women initiating efavirenz (EFV)-containing or nevirapine (NVP)-containing antiretroviral therapy (ART). Design: We analyzed stored samples from women self-reporting implant use in the Partners PrEP Study. Methods: Plasma samples collected every 6 months were analyzed for levonorgestrel and etonogestrel concentrations. Progestin concentrations from samples collected after ART initiation were compared with pre-ART concentrations for intraindividual comparisons. We used adjusted linear mixed models to compare hormone concentrations between individuals on EFV and NVP to a no ART group. We then evaluated whether possessing certain alleles with known or possible influences on EFV, NVP, or progestin metabolism were associated with changes in progestin concentrations or modified the association between ART use and progestin concentrations. Results: Our analysis included 11 women who initiated EFV, 13 who initiated NVP, and 36 who remained ART-naive. In the EFV group, the adjusted geometric mean ratio (aGMR) of levonorgestrel was 0.39 [90% confidence intervals (0.31, 0.49); P < 0.001] and the etonogestrel aGMR was 0.51 (0.34, 0.76; P = 0.006) compared with the control group. No difference was observed in the NVP group compared with controls [levonorgestrel 0.93 (0.74, 1.18); P = 0.64; etonogestrel 1.07 (0.77, 1.50); P = 0.73]. Possession of four allele variants were found to result in further reductions in progestin concentrations among those receiving EFV. Conclusion: Concomitant use of EFV significantly reduces levonorgestrel or etonogestrel concentrations by 61 and 49%, respectively, compared with no ART use. We also report allelic variants in hepatic enzymes that influenced the extent of the observed drug-interaction between progestins and EFV.
机译:目的:评估艾滋病毒阳性妇女的避孕植入孕激素浓度的药代动力学和药物发生,发起EFAVIRENZ(EFV) - 甲基(NVP)抗逆转录病毒治疗(ART)。设计:我们分析了在合作伙伴准备研究中的女性自我报告植入物使用的储存样本。方法:针对左旋林和Etonogestrel浓度分析每6个月收集每6个月的血浆样品。与艺术启动后收集的样品的孕激素浓度与术前浓度进行比较,以便在闭合性比较。我们使用调整的线性混合模型将eFV和NVP上的个体之间的激素浓度与NO艺术组进行比较。然后,我们评估是否具有关于EFV,NVP或孕激素代谢的某些具有已知或可能影响的等位基因与孕激素浓度的变化或改性艺术使用和孕激素浓度之间的变化相关。结果:我们的分析包括11名启动EFV,13岁的妇女,谁启动了NVP,36岁仍然是艺术天真的。在EFV组中,左旋酮的调节几何平均比(AGMR)为0.39 [90%置信区间(0.31,0.49);与对照组相比,P <0.001]和Etonogestrel AGMR为0.51(0.34,0.76; p = 0.006)。与对照组相比,NVP组中没有观察到差异[左炔诺孕烯0.93(0.74,118); p = 0.64; Etonogestrel 1.07(0.77,1.50); p = 0.73]。发现有四种等位基因变体的占有导致孕激素浓度进一步减少接受EFV的浓度。结论:除了没有艺术用途的情况下,伴随EFV的使用显着降低了61%和49%的左旋组织或Etonegestrel浓度。我们还报告肝酶中的等位基因变体,影响了孕激素和EFV之间观察到的药物相互作用的程度。

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