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高密度脂蛋白受体SR-BI的过表达会改变血浆高密度脂蛋白和胆汁胆固醇水平。

Overexpression of the HDL receptor SR-BI alters plasma HDL and bile cholesterol levels.

作者信息

Kozarsky K F, Donahee M H, Rigotti A, Iqbal S N, Edelman E R, Krieger M

机构信息

Institute for Human Gene Therapy, University of Pennsylvania Medical Center, Philadelphia 19104, USA.

出版信息

Nature. 1997 May 22;387(6631):414-7. doi: 10.1038/387414a0.

Abstract

The risk of atherosclerosis, a leading cause of cardiovascular disease and death, is inversely related to plasma levels of high-density lipoprotein (HDL) cholesterol, although the mechanism of this protective effect is unclear. The class B scavenger receptor, SR-BI, is the first HDL receptor to be well defined at a molecular level and is a mediator of selective cholesterol uptake in vitro. It is expressed most abundantly in steroidogenic tissues, where it is coordinately regulated with steroidogenesis by adrenocorticotropic hormone (ACTH), human chorionic gonadotropin (hCG) and oestrogen, and in the liver, where its expression in rats is suppressed by oestrogen. Here we show that adenovirus-mediated, hepatic overexpression of SR-BI in mice on both sinusoidal and canalicular surfaces of hepatocytes results in the virtual disappearance of plasma HDL and a substantial increase in biliary cholesterol. SR-BI may directly mediate these effects by increasing hepatic HDL cholesterol uptake or by increasing cholesterol secretion into bile, or both. These results indicate that SR-BI may be important in hepatic HDL metabolism, in determining plasma HDL concentrations, and in controlling cholesterol concentrations in bile, and thus may influence the development and progression of atherosclerosis and gallstone disease.

摘要

动脉粥样硬化是心血管疾病和死亡的主要原因,其风险与血浆高密度脂蛋白(HDL)胆固醇水平呈负相关,尽管这种保护作用的机制尚不清楚。B类清道夫受体SR-BI是第一个在分子水平上得到明确界定的HDL受体,是体外选择性胆固醇摄取的介质。它在类固醇生成组织中表达最为丰富,在那里它与促肾上腺皮质激素(ACTH)、人绒毛膜促性腺激素(hCG)和雌激素对类固醇生成的调节相互协调;在肝脏中,雌激素可抑制其在大鼠体内的表达。在此我们表明,腺病毒介导的肝细胞窦状隙和胆小管表面SR-BI在小鼠肝脏中的过表达导致血浆HDL几乎消失,胆汁胆固醇大幅增加。SR-BI可能通过增加肝脏对HDL胆固醇的摄取或增加胆固醇向胆汁中的分泌,或两者兼而有之,直接介导这些效应。这些结果表明,SR-BI可能在肝脏HDL代谢、决定血浆HDL浓度以及控制胆汁中胆固醇浓度方面发挥重要作用,从而可能影响动脉粥样硬化和胆结石疾病的发生和发展。

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