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首页> 外文期刊>Journal of Structural Biology >A new drug binding subsite on human serum albumin and drug-drug interaction studied by X-ray crystallography
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A new drug binding subsite on human serum albumin and drug-drug interaction studied by X-ray crystallography

机译:X射线晶体学研究人血清白蛋白与药物相互作用的新药物结合位点

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3'-Azido-3'-deoxythymidine (AZT) is the first clinically effective drug for the treatment of human immunodeficiency virus infection. The drug interaction with human serum albumin (HSA) has been an important component in understanding its mechanism of action, especially in drug distribution and in drug-drug interaction on HSA in the case of multi-drug therapy. We present here crystal structures of a ternary HSA-Myr-AZT complex and a quaternary HSA-Myr-AZT-SAL complex (Myr, myristate; SAL, salicylic acid). From this study, a new drug binding subsite on HSA Sudlow site I was identified. The presence of fatty acid is needed for the creation of this subsite due to fatty acid induced conformational changes of HSA. Thus, the Sudlow site I of HSA can be divided into three non-overlapped subsites: a SAL subsite, an indomethacin subsite and an AZT subsite. Binding of a drug to HSA often influences simultaneous binding of other drugs. From the HSA-Myr-AZT-SAL complex structure, we observed the coexistence of two drugs (AZT and SAL) in Sudlow site I and the competition between these two drugs in subdomain IB. These results provide new structural information on HSA-drug interaction and drug-drug interaction on HSA.
机译:3'-Azido-3'-脱氧胸苷(AZT)是第一种可有效治疗人类免疫缺陷病毒感染的临床药物。与人血清白蛋白(HSA)的药物相互作用一直是了解其作用机理的重要组成部分,尤其是在药物分布以及在多种药物治疗的情况下,药物与HSA的药物相互作用。我们在这里介绍三元HSA-Myr-AZT复合物和四元HSA-Myr-AZT-SAL复合物(Myr,肉豆蔻酸盐; SAL,水杨酸)的晶体结构。通过这项研究,在HSA Sudlow位点I上​​确定了一个新的药物结合亚位点。由于脂肪酸诱导的HSA构象变化,脂肪酸的存在对于创建该亚位点是必需的。因此,HSA的Sudlow站点I可以分为三个不重叠的子站点:SAL子站点,消炎痛子站点和AZT子站点。药物与HSA的结合通常会影响其他药物的同时结合。从HSA-Myr-AZT-SAL复杂结构中,我们观察到Sudlow位点I中两种药物(AZT和SAL)的共存以及在亚域IB中这两种药物之间的竞争。这些结果提供了关于HSA-药物相互作用和HSA上的药物-药物相互作用的新结构信息。

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