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首页> 外文期刊>Current HIV research >Genetic variants of drug metabolizing enzymes and drug transporter (ABCB1) as possible biomarkers for adverse drug reactions in an HIV/AIDS cohort in Zimbabwe.
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Genetic variants of drug metabolizing enzymes and drug transporter (ABCB1) as possible biomarkers for adverse drug reactions in an HIV/AIDS cohort in Zimbabwe.

机译:药物代谢酶和药物转运蛋白(ABCB1)的遗传变异在津巴布韦艾滋病毒/艾滋病队列中的药物反应可能的生物标志物。

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摘要

A study was conducted in an HIV/AIDS Zimbabwean cohort to assess possible associations of pharmacogenetic variants with common adverse drug reactions (ADRs) during anti-retroviral treatment (ART) and/or tuberculosis (TB) treatment. Genotype and allele frequencies for CYP2B6 G516T, CYP2B6 T983C, CYP2A6*17, ABCB1 rs10276036 C>T, NAT2*5 and NAT2*14 were similar to those reported in literature for other African populations. The CYP2B6 516TT genotype and male gender were significantly associated with occurrence of Efavirenz induced central nervous system disorders (OR 20.58, p=0.004) and the ABCB1 rs10276036TT genotype with Nevirapine induced skin hypersensitivity (OR 4.01, p=0.04). For Stavudine, time on treatment was the main factor in development of lipodystrophy (OR 1.06, p<0.0001). For isoniazid, increasing patient age was associated with peripheral neuropathy (OR 1.05, p=0.001). Although genetic polymorphisms may play a role in predicting occurrence of ADRs, this study also indicates that other factors (gender, age, treatment time) are crucial in predicting drug-induced adverse effects.
机译:在艾滋病毒/艾滋病津巴布韦群组中进行了一项研究,以评估药物发生变体在抗逆转录病毒治疗(ART)和/或结核病(TB)治疗期间具有常见不利药物反应(ADRS)的可能组织。 CYP2B6 G516T的基因型和等位基因频率,CYP2B6 T983C,CYP2A6 * 17,ABCB1 RS10276036 C> T,NAT2 * 5和NAT2 * 14类似于其他非洲人群的文献中报告的那些。 CYP2B6 516TT基因型和男性性别与Efavirenz诱导的中枢神经系统疾病(或20.58,P = 0.004)和ABCB1 RS10276036TT基因型与Nevirapine诱导的皮肤超敏反应(或4.01,P = 0.04)显着相关。对于史莱达汀,治疗时间是唇脂萎缩的主要因素(或1.06,P <0.0001)。对于异烟肼,增加患者年龄与周围神经病变(或1.05,p = 0.001)有关。虽然遗传多态性可能在预测ADR的发生时发挥作用,但该研究还表明其他因素(性别,年龄,治疗时间)对于预测药物诱导的不良反应至关重要。

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