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肝G2细胞中固醇27-羟化酶对氧甾醇7-酮胆固醇的代谢作用

Metabolism of an oxysterol, 7-ketocholesterol, by sterol 27-hydroxylase in HepG2 cells.

作者信息

Lyons M A, Brown A J

机构信息

Cell Biology Group, Heart Research Institute, Sydney, New South Wales, Australia.

出版信息

Lipids. 2001 Jul;36(7):701-11. doi: 10.1007/s11745-001-0775-8.

Abstract

7-Ketocholesterol (7K) is a quantitatively important oxysterol in both atherosclerotic lesions and macrophage foam cells. We reported recently that radiolabeled 7K delivered to rodents in a modified lipoprotein or chylomicron remnant-like emulsion, both cleared predominantly by the liver, was rapidly excreted into the intestine as water-soluble products, presumably bile acids. Herein, we aimed to elucidate the early or initial reactions in 7K metabolism. The hypothesis was tested that sterol 27-hydroxylase, a mitochondrial cytochrome P450 and the first enzyme of the acidic bile acid pathway, is responsible for the initial metabolism of 7K by HepG2 cells, a human hepatoblastoma cell-line. The 27-hydroxylated product of 7K (27OH-7K) was shown to be the initial, lipid-soluble product of 7K metabolism. It was produced in mitochondrial incubations and whole cells and was readily released into the media from cells. Intact cells generated metabolites of 7K that had undergone conversion from lipid-soluble precursors to water-soluble products rapidly and extensively. Their production was ablated with cyclosporin A, a sterol 27-hydroxylase inhibitor. Furthermore, we demonstrated the effectiveness of two novel selective inhibitors of this enzyme, GW273297X and GI268267X. These inhibitors also ablated the production of water-soluble products by cells; and the inhibitor of choice, GW273297X, decreased the production of 27OH-7K in mitochondrial preparations. This is the first study to demonstrate that sterol 27-hydroxylase plays an important role in the metabolism of oxysterols such as 7K in liver cells.

摘要

7-酮胆固醇(7K)是动脉粥样硬化病变和巨噬细胞泡沫细胞中一种数量上重要的氧化甾醇。我们最近报道,以修饰脂蛋白或乳糜微粒残粒样乳剂形式给予啮齿动物的放射性标记7K,主要由肝脏清除,会迅速以水溶性产物(可能是胆汁酸)的形式排泄到肠道中。在此,我们旨在阐明7K代谢的早期或初始反应。我们检验了这样一个假设:甾醇27-羟化酶,一种线粒体细胞色素P450和酸性胆汁酸途径的首个酶,负责HepG2细胞(一种人肝癌细胞系)对7K的初始代谢。7K的27-羟基化产物(27OH-7K)被证明是7K代谢的初始脂溶性产物。它在线粒体孵育体系和完整细胞中产生,并很容易从细胞释放到培养基中。完整细胞能迅速且广泛地产生从脂溶性前体转化为水溶性产物的7K代谢物。它们的产生被环孢素A(一种甾醇27-羟化酶抑制剂)所消除。此外,我们证明了该酶的两种新型选择性抑制剂GW273297X和GI268267X的有效性。这些抑制剂也消除了细胞对水溶性产物的产生;而首选抑制剂GW273297X降低了线粒体制剂中27OH-7K的产生。这是第一项证明甾醇27-羟化酶在肝细胞中7K等氧化甾醇代谢中起重要作用的研究。

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