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Cytochrome P450 metabolism of the post-lanosterol intermediates explains enigmas of cholesterol synthesis

机译:细胞色素P450后Lanterol醇中间体的代谢解释了胆固醇合成的谜团

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摘要

Cholesterol synthesis is among the oldest metabolic pathways, consisting of the Bloch and Kandutch-Russell branches. Following lanosterol, sterols of both branches are proposed to be dedicated to cholesterol. We challenge this dogma by mathematical modeling and with experimental evidence. It was not possible to explain the sterol profile of testis in cAMP responsive element modulator tau (Crem?τ) knockout mice with mathematical models based on textbook pathways of cholesterol synthesis. Our model differs in the inclusion of virtual sterol metabolizing enzymes branching from the pathway. We tested the hypothesis that enzymes from the cytochrome P450 (CYP) superfamily can participate in the catalysis of non-classical reactions. We show that CYP enzymes can metabolize multiple sterols in vitro, establishing novel branching points of cholesterol synthesis. In conclusion, sterols of cholesterol synthesis can be oxidized further to metabolites not dedicated to production of cholesterol. Additionally, CYP7A1, CYP11A1, CYP27A1, and CYP46A1 are parts of a broader cholesterol synthesis network.
机译:胆固醇合成是最古老的代谢途径,由Bloch和Kandutd-Russell分支组成。在Lanterols之后,提出了两个分支的甾醇致力于胆固醇。我们通过数学建模和实验证据挑战这条教条。在CAMP响应元素调制器TAU(CREM?τ)敲除小鼠中无法解释睾丸的甾醇谱,基于胆固醇合成教科书途径的数学模型。我们的模型与从途径分支的虚拟甾醇代谢酶含有含量。我们测试了来自细胞色素P450(CYP)超家族的酶的假设可以参与非经典反应的催化。我们表明CYP酶可以在体外代谢多种甾醇,建立胆固醇合成的新分支点。总之,胆固醇合成的甾醇可以进一步氧化,以致力于生产胆固醇的代谢物。另外,CYP7A1,CYP11A1,CYP27A1和CYP46A1是更广泛胆固醇合成网络的一部分。

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