首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Mapping of the Allosteric Site in Cholesterol Hydroxylase CYP46A1 for Efavirenz a Drug That Stimulates Enzyme Activity
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Mapping of the Allosteric Site in Cholesterol Hydroxylase CYP46A1 for Efavirenz a Drug That Stimulates Enzyme Activity

机译:依法韦仑胆固醇羟化酶CYP46A1的变构位点的映射一种刺激酶活性的药物。

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摘要

Cytochrome P450 46A1 (CYP46A1) is a microsomal enzyme and cholesterol 24-hydroxylase that controls cholesterol elimination from the brain. This P450 is also a potential target for Alzheimer disease because it can be activated pharmacologically by some marketed drugs, as exemplified by efavirenz, the anti-HIV medication. Previously, we suggested that pharmaceuticals activate CYP46A1 allosterically through binding to a site on the cytosolic protein surface, which is different from the enzyme active site facing the membrane. Here we identified this allosteric site for efavirenz on CYP46A1 by using a combination of hydrogen-deuterium exchange coupled to MS, computational modeling, site-directed mutagenesis, and analysis of the CYP46A1 crystal structure. We also mapped the binding region for the CYP46A1 redox partner oxidoreductase and found that the allosteric and redox partner binding sites share a common border. On the basis of the data obtained, we propose the mechanism of CYP46A1 allostery and the pathway for the signal transmission from the P450 allosteric site to the active site.
机译:细胞色素P450 46A1(CYP46A1)是微粒体酶和胆固醇24羟化酶,可控制大脑中胆固醇的清除。该P450也是阿尔茨海默氏病的潜在靶标,因为它可以被某些市售药物在药理上激活,例如抗HIV药物efavirenz。以前,我们建议药物通过与胞质蛋白表面上的位点结合来变构地激活CYP46A1,该位点与面向膜的酶活性位点不同。在这里,我们通过结合使用氢-氘交换联用MS,计算模型,定点诱变和CYP46A1晶体结构分析,确定了CYP46A1上依非韦伦的这个变构位点。我们还绘制了CYP46A1氧化还原伴侣氧化还原酶的结合区域,并发现变构和氧化还原伴侣结合位点具有相同的边界。根据获得的数据,我们提出了CYP46A1变构的机理和信号从P450变构位点向活性位点的传递途径。

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