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ATP binding cassette transporter G1 (ABCG1) is an intracellular sterol transporter

机译:ATP结合盒转运蛋白G1(ABCG1)是细胞内固醇转运蛋白

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摘要

Four members of the mammalian ATP binding cassette (ABC) transporter G subfamily are thought to be involved in transmembrane (TM) transport of sterols. The residues responsible for this transport are unknown. The mechanism of action of ABCG1 is controversial and it has been proposed to act at the plasma membrane to facilitate the efflux of cellular sterols to exogenous high-density lipoprotein (HDL). Here we show that ABCG1 function is dependent on localization to intracellular endosomes. Importantly, localization to the endosome pathway distinguishes ABCG1 and/or ABCG4 from all other mammalian members of this superfamily, including other sterol transporters. We have identified critical residues within the TM domains of ABCG1 that are both essential for sterol transport and conserved in some other members of the ABCG subfamily and/or the insulin-induced gene 2 (INSIG-2). Our conclusions are based on studies in which (i) biotinylation of peritoneal macrophages showed that endogenous ABCG1 is intracellular and undetectable at the cell surface, (ii) a chimeric protein containing the TM of ABCG1 and the cytoplasmic domains of the nonsterol transporter ABCG2 is both targeted to endosomes and functional, and (iii) ABCG1 colocalizes with multiple proteins that mark late endosomes and recycling endosomes. Mutagenesis studies identify critical residues in the TM domains that are important for ABCG1 to alter sterol efflux, induce sterol regulatory element binding protein-2 (SREBP-2) processing, and selectively attenuate the oxysterol-mediated repression of SREBP-2 processing. Our data demonstrate that ABCG1 is an intracellular sterol transporter that localizes to endocytic vesicles to facilitate the redistribution of specific intracellular sterols away from the endoplasmic reticulum (ER).
机译:哺乳动物ATP结合盒(ABC)转运蛋白G亚家族的四个成员被认为与甾醇的跨膜(TM)转运有关。负责这种运输的残留物是未知的。 ABCG1的作用机制是有争议的,有人提出它作用于质膜以促进细胞固醇向外源高密度脂蛋白(HDL)的流出。在这里,我们显示ABCG1功能取决于细胞内内体的定位。重要的是,定位于内体途径将ABCG1和/或ABCG4与该超家族的所有其他哺乳动物成员(包括其他固醇转运蛋白)区分开。我们已经确定了ABCG1 TM域内的关键残基,这些残基对于固醇转运至关重要,并且在ABCG亚家族的其他成员和/或胰岛素诱导的基因2(INSIG-2)中也保守。我们的结论基于以下研究:(i)腹膜巨噬细胞的生物素化显示内源性ABCG1在细胞内且在细胞表面不可检测;(ii)包含ABCG1 TM和非甾醇转运蛋白ABCG2胞质域的嵌合蛋白(iii)ABCG1与标记晚期内体和回收内体的多种蛋白质共定位。诱变研究发现TM域中的关键残基对于ABCG1改变固醇外排,诱导固醇调节元件结合蛋白2(SREBP-2)加工以及选择性地减弱氧固醇介导的SREBP-2加工的抑制至关重要。我们的数据表明,ABCG1是一种细胞内固醇转运蛋白,定位于内吞小泡,以促进特定细胞内固醇从内质网(ER)的重新分布。

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