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氧化固醇结合蛋白相关蛋白 1 变体具有与内溶酶体相反的胆固醇转运活性。

Oxysterol-binding protein-related protein 1 variants have opposing cholesterol transport activities from the endolysosomes.

机构信息

Departments of Pediatrics and Biochemistry & Molecular Biology, Dalhousie University, Halifax, NS B3H 4R2, Canada.

出版信息

Mol Biol Cell. 2020 Apr 1;31(8):793-802. doi: 10.1091/mbc.E19-12-0697. Epub 2020 Feb 5.

DOI:10.1091/mbc.E19-12-0697
PMID:32023146
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7185962/
Abstract

encodes the full-length oxysterol-binding protein-related protein ORP1L, which transports LDL-derived cholesterol at membrane contacts between the late endosomes/lysosomes (LEL) and the endoplasmic reticulum (ER). also encodes the truncated variant ORP1S that contains only the C-terminal lipid binding domain. HeLa cells in which both variants were knocked out (ORP1-null) were used to determine the functional relationship between ORP1L and ORP1S with respect to cellular cholesterol localization and regulation. ORP1-null cells accumulated cholesterol in LEL and had reduced plasma membrane (PM) cholesterol. PM cholesterol was restored by expression of wild-type ORP1S or a phosphatidylinositol phosphate-binding mutant but not by a sterol-binding mutant. Expression of ORP2, another truncated variant, also restored PM cholesterol in ORP1-null cells. Consistent with a LEL-to-PM cholesterol transport activity, a small fraction of ORP1S was detected on the PM. As a consequence of reduced delivery of cholesterol to the PM in ORP1-null cells, cholesterol was diverted to the ER resulting in normalization of de novo cholesterol synthesis. The deficiency in PM cholesterol also reduced ABCA1-dependent cholesterol efflux and LDL receptor activity in ORP1-null cells. We conclude that ORP1S, which lacks discrete membrane-targeting motifs, transports cholesterol from LEL to the PM.

摘要

编码全长的氧化固醇结合蛋白相关蛋白 ORP1L,该蛋白在晚期内体/溶酶体(LEL)和内质网(ER)之间的膜接触处运输 LDL 衍生的胆固醇。还编码仅包含 C 末端脂质结合结构域的截断变体 ORP1S。用敲除了这两种变体(ORP1 缺失)的 HeLa 细胞来确定 ORP1L 和 ORP1S 之间在细胞胆固醇定位和调节方面的功能关系。ORP1 缺失细胞在 LEL 中积累胆固醇,并且质膜(PM)胆固醇减少。通过表达野生型 ORP1S 或磷酸肌醇磷酸结合突变体,但不是固醇结合突变体,可以恢复 PM 胆固醇。另一种截断变体 ORP2 的表达也可以恢复 ORP1 缺失细胞中的 PM 胆固醇。与 LEL 到 PM 胆固醇转运活性一致,一小部分 ORP1S 被检测到在 PM 上。由于 ORP1 缺失细胞中胆固醇向 PM 的输送减少,胆固醇被分流到 ER,导致从头合成胆固醇正常化。PM 胆固醇的缺乏也降低了 ORP1 缺失细胞中 ABCA1 依赖性胆固醇外流和 LDL 受体活性。我们得出结论,ORP1S 缺乏离散的膜靶向基序,从 LEL 向 PM 转运胆固醇。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6245/7185962/2402699f7e11/mbc-31-793-g008.jpg
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