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Cellular cholesterol delivery intracellular processing and utilization for biosynthesis of steroid hormones

机译:细胞内胆固醇的输送细胞内加工和甾类激素的生物合成利用

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摘要

Steroid hormones regulate diverse physiological functions such as reproduction, blood salt balance, maintenance of secondary sexual characteristics, response to stress, neuronal function and various metabolic processes. They are synthesized from cholesterol mainly in the adrenal gland and gonads in response to tissue-specific tropic hormones. These steroidogenic tissues are unique in that they require cholesterol not only for membrane biogenesis, maintenance of membrane fluidity and cell signaling, but also as the starting material for the biosynthesis of steroid hormones. It is not surprising, then, that cells of steroidogenic tissues have evolved with multiple pathways to assure the constant supply of cholesterol needed to maintain optimum steroid synthesis. The cholesterol utilized for steroidogenesis is derived from a combination of sources: 1) de novo synthesis in the endoplasmic reticulum (ER); 2) the mobilization of cholesteryl esters (CEs) stored in lipid droplets through cholesteryl ester hydrolase; 3) plasma lipoprotein-derived CEs obtained by either LDL receptor-mediated endocytic and/or SR-BI-mediated selective uptake; and 4) in some cultured cell systems from plasma membrane-associated free cholesterol. Here, we focus on recent insights into the molecules and cellular processes that mediate the uptake of plasma lipoprotein-derived cholesterol, events connected with the intracellular cholesterol processing and the role of crucial proteins that mediate cholesterol transport to mitochondria for its utilization for steroid hormone production. In particular, we discuss the structure and function of SR-BI, the importance of the selective cholesterol transport pathway in providing cholesterol substrate for steroid biosynthesis and the role of two key proteins, StAR and PBR/TSO in facilitating cholesterol delivery to inner mitochondrial membrane sites, where P450scc (CYP11A) is localized and where the conversion of cholesterol to pregnenolone (the common steroid precursor) takes place.
机译:类固醇激素调节多种生理功能,例如生殖,血盐平衡,维持第二性征,对压力的反应,神经元功能和各种代谢过程。它们是由胆固醇生成的,主要是响应组织特异性的热带激素而在肾上腺和性腺中合成的。这些类固醇生成组织的独特之处在于,它们不仅需要胆固醇来促进膜生物发生,维持膜流动性和细胞信号传导,而且还需要胆固醇作为生物合成类固醇激素的原料。因此,毫不奇怪的是,类固醇生成组织的细胞已通过多种途径进化,以确保维持最佳类固醇合成所需的恒定胆固醇供应。用于类固醇生成的胆固醇源自多种来源:1)内质网(ER)的从头合成; 2)通过胆固醇酯水解酶动员脂质滴中储存的胆固醇酯(CE); 3)通过LDL受体介导的内吞和/或SR-BI介导的选择性摄取获得血浆脂蛋白衍生的CE; 4)在某些培养的细胞系统中,血浆膜相关的游离胆固醇。在这里,我们重点介绍介导血浆脂蛋白衍生的胆固醇摄取的分子和细胞过程的最新见解,与细胞内胆固醇加工有关的事件以及介导胆固醇转运至线粒体以利用其产生类固醇激素的关键蛋白的作用。特别是,我们讨论了SR-BI的结构和功能,选择性胆固醇转运途径在为类固醇生物合成提供胆固醇底物方面的重要性以及两种关键蛋白StAR和PBR / TSO在促进胆固醇向线粒体内膜传递中的作用。 P450scc(CYP11A)位于本地,胆固醇向孕烯醇酮(普通甾体前体)的转化。

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