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A pathway for the metabolism of vitamin D3: Unique hydroxylated metabolites formed during catalysis with cytochrome P450scc (CYP11A1)

机译:维生素D3的代谢途径:细胞色素P450scc(CYP11A1)催化过程中形成的独特羟基化代谢物

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摘要

Metabolites of vitamin D3 (D3) (cholecalciferol) are recognized as enzymatically formed chemicals in humans that can influence a wide variety of reactions that regulate a large number of cellular functions. The metabolism of D3 has been extensively studied, and a role for three different mitochondrial cytochrome P450s (CYP24A, CYP27A, and CYP27B1) has been described that catalyze the formation of the 24(OH), 25(OH), and 1(OH) metabolites of D3, respectively. The hormone 1,25-dihydroxyvitamin D3 has been most extensively studied and is widely recognized as a regulator of calcium and phosphorous metabolism. Hydroxylated metabolites of D3 interact with the nuclear receptor and thereby influence growth, cellular differentiation, and proliferation. In this article, we describe in vitro experiments using purified mitochondrial cytochrome P450scc (CYP11A1) reconstituted with the iron-sulfer protein, adrenodoxin, and the flavoprotein, adrenodoxin reductase, and show the NADPH and time-dependent formation of two major metabolites of D3 (i.e., 20-hydroxyvitamin D3 and 20,22-dihydroxyvitamin D3) plus two unknown minor metabolites. In addition, we describe the metabolism of 7-dehydrocholesterol by CYP11A1 to a single product identified as 7-dehydropregnenolone. Although the physiological importance of these hydroxylated metabolites of D3 and their in vivo formation and mode of action remain to be determined, the rate with which they are formed by CYP11A1 in vitro suggests an important role.
机译:维生素D3(D3)(胆钙化固醇)的代谢产物被认为是人体内酶促形成的化学物质,可影响调节多种细胞功能的多种反应。 D3的代谢已被广泛研究,并且已经描述了三种不同的线粒体细胞色素P450(CYP24A,CYP27A和CYP27B1)的作用,它们催化24(OH),25(OH)和1(OH)的形成D3的代谢产物。 1,25-二羟基维生素D3激素已得到最广泛的研究,被广泛认为是钙和磷代谢的调节剂。 D3的羟基代谢产物与核受体相互作用,从而影响生长,细胞分化和增殖。在本文中,我们描述了使用纯化的线粒体细胞色素P450scc(CYP11A1)与铁硫蛋白肾上腺素毒素和黄素蛋白,肾上腺素毒素还原酶重构的体外实验,并显示了NADPH和D3两种主要代谢物的时间依赖性形成(即20-羟基维生素D3和20,22-二羟基维生素D3)加上两个未知的次要代谢物。此外,我们描述了由CYP11A1代谢为7-脱氢孕烯醇酮的单一产品的7-脱氢胆固醇。尽管这些D3羟基化代谢物的生理重要性及其在体内的形成和作用方式尚待确定,但在体外由CYP11A1形成的速率表明了重要的作用。

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