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衔接蛋白ARH将巨蛋白护送至内体并穿过内体。

The adaptor protein ARH escorts megalin to and through endosomes.

作者信息

Nagai Masaaki, Meerloo Timo, Takeda Tetsuro, Farquhar Marilyn Gist

机构信息

Department of Cellular and Molecular Medicine, University of California, San Diego, La Jolla, California 92093, USA.

出版信息

Mol Biol Cell. 2003 Dec;14(12):4984-96. doi: 10.1091/mbc.e03-06-0385. Epub 2003 Oct 3.

Abstract

Megalin is an endocytic receptor that binds multiple ligands and is essential for many physiological processes such as brain development and uptake of proteins by the kidney tubule, yolk sac, and thyroid. The cytoplasmic tail of megalin contains two FXNPXY motifs. Autosomal recessive hypercholesterolemia (ARH) is an adaptor protein that binds to the FXNPXY motif of the low-density lipoprotein receptor as well as clathrin and AP-2. We found that ARH also binds to the first FXNPXY motif of megalin in two-hybrid, pull-down and coimmunoprecipitation assays. ARH colocalizes with megalin in clathrin coated pits and in recycling endosomes in the Golgi region. When cells are treated with nocodazole, the recycling endosomes containing megalin and ARH disperse. On internalization of megalin, ARH and megalin are first seen in clathrin coated pits followed by sequential localization in early endosomes and tubular recycling endosomes in the pericentriolar region followed by their reappearance at the cell surface. Expression of ARH in Madin-Darby canine kidney cells expressing megalin mini-receptors enhances megalin-mediated uptake of 125I-lactoferrin, a megalin ligand. These results show that ARH facilitates endocytosis of megalin, escorts megalin along its endocytic route and raise the possibility that transport through the endosomal system is selective and requires interaction with specific adaptor proteins.

摘要

巨蛋白是一种内吞受体,可结合多种配体,对许多生理过程至关重要,如大脑发育以及肾小管、卵黄囊和甲状腺对蛋白质的摄取。巨蛋白的胞质尾含有两个FXNPXY基序。常染色体隐性高胆固醇血症(ARH)是一种衔接蛋白,可与低密度脂蛋白受体的FXNPXY基序以及网格蛋白和AP-2结合。我们发现在双杂交、下拉和共免疫沉淀实验中,ARH也能与巨蛋白的第一个FXNPXY基序结合。ARH与巨蛋白在网格蛋白包被小窝以及高尔基体区域的循环内体中共定位。当用诺考达唑处理细胞时,含有巨蛋白和ARH的循环内体分散。在巨蛋白内化时,首先在网格蛋白包被小窝中观察到ARH和巨蛋白,随后依次定位于中心粒周围区域的早期内体和管状循环内体,之后它们再次出现在细胞表面。在表达巨蛋白微型受体的Madin-Darby犬肾细胞中表达ARH可增强巨蛋白介导的125I-乳铁蛋白(一种巨蛋白配体)的摄取。这些结果表明,ARH促进巨蛋白的内吞作用,在其内吞途径中护送巨蛋白,并增加了通过内体系统的运输具有选择性且需要与特定衔接蛋白相互作用的可能性。

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