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Brain neurotransmitter transporter/receptor genomics and efavirenz central nervous system adverse events

机译:脑神经递质转运蛋白/受体基因组学和efavirenz中枢神经系统不良事件

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ObjectiveWe characterized associations between central nervous system (CNS) adverse events and brain neurotransmitter transporter/receptor genomics among participants randomized to efavirenz-containing regimens in AIDS Clinical Trials Group studies in the USA.Participants and methodsFour clinical trials randomly assigned treatment-naive participants to efavirenz-containing regimens. Genome-wide genotype and PrediXcan were used to infer gene expression levels in tissues including 10 brain regions. Multivariable regression models stratified by race/ethnicity were adjusted for CYP2B6/CYP2A6 genotypes that predict plasma efavirenz exposure, age, and sex. Combined analyses also adjusted for genetic ancestry.ResultsAnalyses included 167 cases with grade 2 or greater efavirenz-consistent CNS adverse events within 48 weeks of study entry, and 653 efavirenz-tolerant controls. CYP2B6/CYP2A6 genotype level was independently associated with CNS adverse events (odds ratio: 1.07; P=0.044). Predicted expression of six genes postulated to mediate efavirenz CNS side effects (SLC6A2, SLC6A3, PGR, HTR2A, HTR2B, HTR6) were not associated with CNS adverse events after correcting for multiple testing, the lowest P value being for PGR in hippocampus (P=0.012), nor were polymorphisms in these genes or AR and HTR2C, the lowest P value being for rs12393326 in HTR2C (P=6.7x10(-4)). As a positive control, baseline plasma bilirubin concentration was associated with predicted liver UGT1A1 expression level (P=1.9x10(-27)).ConclusionEfavirenz-related CNS adverse events were not associated with predicted neurotransmitter transporter/receptor gene expression levels in brain or with polymorphisms in these genes. Variable susceptibility to efavirenz-related CNS adverse events may not be explained by brain neurotransmitter transporter/receptor genomics.
机译:目标中枢神经系统(CNS)不良事件和脑神经递质转运蛋白和脑神经递质转运蛋白/受体基因组学之间的特征在美国艾滋病临床试验组研究中的参与者中的脑神经递质转运蛋白/受体基因组学。晚上试验临床试验随机分配给efavirenz的治疗 - 天真的参与者 - 统一的方案。基因组基因型和预先用来推断出包括10个脑区的组织中的基因表达水平。通过种族/种族分层分层的多变量回归模型针对CYP2B6 / CYP2A6基因型进行调整,预测血浆EFAVIRENZ暴露,年龄和性别。结合分析还调整了遗传血统。遗传素包括167例,患者在48周内患有2级或更高的EFAVIRENZ-一致的CNS不良事件,以及653种EFAVIRENZ耐受控制。 CYP2B6 / CYP2A6基因型水平独立与CNS不良事件相关(差距:1.07; P = 0.044)。预测六种基因的表达出假设到介导EFAVIREVENCNS副作用(SLC6A2,SLC6A3,PGR,HTR2A,HTR2B,HTR6)没有与校正多次测试后的CNS不良事件相关联,在海马中PGR的最低P值(P = 0.012),在这些基因或Ar和HTR2C中也不是多态性,最低P值为HTR2C中的RS12393326(P = 6.7x10(-4))。作为阳性对照,基线等离子体胆红素浓度与预测的肝脏UGT1A1表达水平有关(P = 1.9×10(-27))。结案相关的相关的CNS不良事件与脑或脑中的预测神经递质转运蛋白/受体基因表达水平无关这些基因中的多态性。脑神经递质转运蛋白/受体基因组学可能不解释对Efavirenz相关的CNS不良事件的可变易感性。

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