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I型清道夫受体的二聚化:在不同细胞和组织中的形成、功能及定位

Dimerization of the scavenger receptor class B type I: formation, function, and localization in diverse cells and tissues.

作者信息

Reaven Eve, Cortez Yuan, Leers-Sucheta Susan, Nomoto Ann, Azhar Salman

机构信息

Geriatrics Research, Education, and Clinical Center, VA Palo Alto Health Care System, Palo Alto, CA, USA.

出版信息

J Lipid Res. 2004 Mar;45(3):513-28. doi: 10.1194/jlr.M300370-JLR200. Epub 2003 Dec 1.

DOI:10.1194/jlr.M300370-JLR200
PMID:14657200
Abstract

This study has examined the dimeric/oligomeric forms of scavenger receptor class B type I (SR-BI) and its alternatively spliced form, SR-BII, in a diverse group of cells and tissues: i.e., normal and hormonally altered tissues of mice and rats as well as tissues of transgenic animals and genetically altered steroidogenic and nonsteroidogenic cells overexpressing the SR-B proteins. Using both biochemical and morphological techniques, we have seen that these dimeric and higher order oligomeric forms of SR-BI expression are strongly associated with both functional and morphological expression of the selective HDL cholesteryl ester uptake pathway. Rats and mice show some species differences in expression of SR-BII dimeric forms; this difference does not extend to the use of SR-B cDNA types for transfection purposes. In a separate study, cotransfection of HEK293 cells with cMyc and V5 epitope-tagged SR-BI permitted coprecipitation and quantitative coimmunocytochemical measurements at the electron microscope level, suggesting that much of the newly expressed SR-BI protein in stimulated cells dimerizes and that the SR-BI dimers are localized to the cell surface and specifically to microvillar or double membraned intracellular channels. These combined data suggest that SR-BI self-association represents an integral step in the selective cholesteryl ester uptake process.

摘要

本研究检测了I型清道夫受体B类(SR-BI)及其可变剪接形式SR-BII在多种细胞和组织中的二聚体/寡聚体形式,这些细胞和组织包括:小鼠和大鼠的正常组织及激素改变后的组织、转基因动物的组织,以及过表达SR-B蛋白的基因改造的类固醇生成细胞和非类固醇生成细胞。运用生化和形态学技术,我们发现SR-BI表达的这些二聚体和高阶寡聚体形式与选择性高密度脂蛋白胆固醇酯摄取途径的功能和形态学表达密切相关。大鼠和小鼠在SR-BII二聚体形式的表达上存在一些物种差异;这种差异在用于转染目的的SR-B cDNA类型的使用上并未体现。在另一项研究中,将HEK293细胞与cMyc和V5表位标记的SR-BI共转染,可在电子显微镜水平进行共沉淀和定量共免疫细胞化学测量,这表明受刺激细胞中许多新表达的SR-BI蛋白会形成二聚体,且SR-BI二聚体定位于细胞表面,特别是微绒毛或双膜细胞内通道。这些综合数据表明,SR-BI的自我缔合是选择性胆固醇酯摄取过程中不可或缺的一步。

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