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孕烷X受体的天然蛋白变体,其对CYP3A4的反式激活活性发生改变。

Natural protein variants of pregnane X receptor with altered transactivation activity toward CYP3A4.

作者信息

Hustert E, Zibat A, Presecan-Siedel E, Eiselt R, Mueller R, Fuss C, Brehm I, Brinkmann U, Eichelbaum M, Wojnowski L, Burk O

机构信息

EPIDAUROS Biotechnologie AG, Bernried, Germany.

出版信息

Drug Metab Dispos. 2001 Nov;29(11):1454-9.

Abstract

Between 45 and 60% of all drugs currently used are metabolized by the CYP3A4 protein. CYP3A4 expression in liver varies up to 60-fold in the general population, which can lead to ineffective drug therapy (high CYP3A4) or, on the other hand, to harmful drug reactions (low CYP3A4). Most of this variability has been attributed to genetic factors, but to date their identity remains unknown. Recently, it was shown that CYP3A expression is largely controlled by the pregnane X receptor (PXR). We, therefore, hypothesized that polymorphisms in PXR may contribute to CYP3A4 variability. The presence of PXR variants was investigated in two ethnic groups, Caucasians and Africans. Six missense mutations leading to variant PXR proteins were identified, and their consequences on CYP3A4 expression were analyzed. Expressed in LS174T cells, three protein variants, V140M, D163G, and A370T, exhibited altered basal and/or induced transactivation of CYP3A promoter reporter genes. Thus, these natural PXR protein variants may play a role in the observed interindividual variability of CYP3A4 expression and may be involved in rare, atypical responses to drugs or altered sensitivities to carcinogens.

摘要

目前使用的所有药物中,有45%至60%是由CYP3A4蛋白代谢的。在普通人群中,肝脏中CYP3A4的表达差异高达60倍,这可能导致药物治疗无效(CYP3A4水平高),或者另一方面,导致有害的药物反应(CYP3A4水平低)。这种变异性大多归因于遗传因素,但迄今为止,其具体情况仍不清楚。最近的研究表明,CYP3A的表达在很大程度上受孕烷X受体(PXR)的控制。因此,我们推测PXR基因多态性可能导致CYP3A4的变异性。我们在白种人和非洲人这两个人种群体中研究了PXR变体的存在情况。鉴定出六个导致PXR变体蛋白的错义突变,并分析了它们对CYP3A4表达的影响。在LS174T细胞中表达时,三种蛋白变体V140M、D163G和A370T表现出CYP3A启动子报告基因的基础和/或诱导反式激活的改变。因此,这些天然的PXR蛋白变体可能在观察到的CYP3A4表达个体间变异性中发挥作用,并且可能与罕见的、非典型的药物反应或对致癌物的敏感性改变有关。

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