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CYP11A1的新活性及其潜在的生理意义。

Novel activities of CYP11A1 and their potential physiological significance.

作者信息

Slominski Andrzej T, Li Wei, Kim Tae-Kang, Semak Igor, Wang Jin, Zjawiony Jordan K, Tuckey Robert C

机构信息

Department of Pathology and Laboratory Medicine, University of Tennessee HSC, Memphis, TN, USA; Division of Rheumatology of the Department of Medicine, University of Tennessee HSC, Memphis, TN, USA.

Department of Pharmaceutical Sciences, University of Tennessee HSC, Memphis, TN, USA.

出版信息

J Steroid Biochem Mol Biol. 2015 Jul;151:25-37. doi: 10.1016/j.jsbmb.2014.11.010. Epub 2014 Nov 13.

Abstract

CYP11A1, found only in vertebrates, catalyzes the first step of steroidogenesis where cholesterol is converted to pregnenolone. The purified enzyme, also converts desmosterol and plant sterols including campesterol and β-sitosterol, to pregnenolone. Studies, initially with purified enzyme, reveal that 7-dehydrocholesterol (7DHC), ergosterol, lumisterol 3, and vitamins D3 and D2 also serve as substrates for CYP11A1, with 7DHC being better and vitamins D3 and D2 being poorer substrates than cholesterol. Adrenal glands, placenta, and epidermal keratinocytes can also carry out these conversions and 7-dehydropregnenolone has been detected in the epidermis, adrenal glands, and serum, and 20-hydroxyvitamin D3 was detected in human serum and the epidermis. Thus, this metabolism does appear to occur in vivo, although its quantitative importance and physiological role remain to be established. CYP11A1 action on 7DHC in vivo is further supported by detection of Δ(7)steroids in Smith-Lemli-Opitz syndrome patients. The activity of CYP11A1 is affected by the structure of the substrate with sterols having steroidal or Δ(7)-steroidal structures undergoing side chain cleavage following hydroxylations at C22 and C20. In contrast, metabolism of vitamin D involves sequential hydroxylations that start at C20 but do not lead to cleavage. Molecular modeling using the crystal structure of CYP11A1 predicts that other intermediates of cholesterol synthesis could also serve as substrates for CYP11A1. Finally, CYP11A1-derived secosteroidal hydroxy-derivatives and Δ(7)steroids are biologically active when administered in vitro in a manner dependent on the structure of the compound and the lineage of the target cells, suggesting physiological roles for these metabolites. This article is part of a special issue entitled 'SI: Steroid/Sterol signaling'.

摘要

CYP11A1仅在脊椎动物中发现,它催化类固醇生成的第一步,即将胆固醇转化为孕烯醇酮。纯化后的该酶还能将羊毛甾醇以及包括菜油甾醇和β-谷甾醇在内的植物甾醇转化为孕烯醇酮。最初对纯化酶进行的研究表明,7-脱氢胆固醇(7DHC)、麦角固醇、光甾醇3以及维生素D3和D2也可作为CYP11A1的底物,其中7DHC作为底物比胆固醇更佳,而维生素D3和D2作为底物则比胆固醇更差。肾上腺、胎盘和表皮角质形成细胞也能进行这些转化,并且在表皮、肾上腺和血清中检测到了7-脱氢孕烯醇酮,在人血清和表皮中检测到了20-羟基维生素D3。因此,尽管其定量重要性和生理作用仍有待确定,但这种代谢似乎确实在体内发生。史密斯-利姆利-奥皮茨综合征患者体内检测到Δ(7)类固醇,进一步支持了CYP11A1在体内对7DHC的作用。CYP11A1的活性受底物结构的影响,具有甾体或Δ(7)-甾体结构的甾醇在C22和C20羟基化后会发生侧链裂解。相比之下,维生素D的代谢涉及从C20开始的顺序羟基化,但不会导致裂解。使用CYP11A1晶体结构进行的分子建模预测,胆固醇合成的其他中间体也可能作为CYP11A1的底物。最后,CYP11A1衍生的甾类羟基衍生物和Δ(7)类固醇在体外给药时具有生物活性,其活性方式取决于化合物的结构和靶细胞的谱系,这表明这些代谢产物具有生理作用。本文是名为“SI:类固醇/甾醇信号传导”特刊的一部分。

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