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小分子 GTP 酶 Cdc42 与尼曼-匹克 C1 样蛋白 1(NPC1L1)相互作用,并以胆固醇依赖的方式控制 NPC1L1 从内体再循环隔室到质膜的运动。

The small GTPase Cdc42 interacts with Niemann-Pick C1-like 1 (NPC1L1) and controls its movement from endocytic recycling compartment to plasma membrane in a cholesterol-dependent manner.

机构信息

The State Key Laboratory of Molecular Biology, Institute of Biochemistry and Cell Biology, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, 320 Yue-Yang Road, Shanghai 200031, China.

The State Key Laboratory of Molecular Biology, Institute of Biochemistry and Cell Biology, Shanghai Institutes for Biological Sciences, Chinese Academy of Sciences, 320 Yue-Yang Road, Shanghai 200031, China.

出版信息

J Biol Chem. 2011 Oct 14;286(41):35933-35942. doi: 10.1074/jbc.M111.270199. Epub 2011 Aug 15.

DOI:10.1074/jbc.M111.270199
PMID:21844200
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3195612/
Abstract

Niemann-Pick C1-like 1 (NPC1L1) is a multi-transmembrane protein that mediates the absorption of dietary and biliary cholesterol through vesicular endocytosis. The subcellular localization of NPC1L1 is regulated by cholesterol. Cholesterol depletion induces the transport of NPC1L1 to plasma membrane (PM) from endocytic recycling compartment that requires MyoVb·Rab11a·Rab11-FIP2 triple complex, and cholesterol-replenishment renders the internalization of NPC1L1 together with cholesterol. Here, we find that GTP-bound Cdc42 interacts with NPC1L1. Cholesterol depletion regulates the activation of Cdc42 and enhances NPC1L1-Cdc42 interaction. Overexpression of constitutive GTP-bound Cdc42 mutant form or knockdown of Cdc42 inhibits the transport of NPC1L1 to the PM and disturbs the cholesterol-regulated binding of NPC1L1 to Rab11a, MyoVb, and actin. Knockdown of Cdc42 downstream effectors N-WASP or Arp3 also leads to the similar results. In liver-specific Cdc42 knock-out (Cdc42 LKO) mice, NPC1L1 fails to localize to bile canaliculi, and the biliary cholesterol cannot be efficiently reabsorbed. These results indicate that Cdc42 controls the cholesterol-regulated transport and localization of NPC1L1, and plays a role in cholesterol absorption.

摘要

尼曼-匹克 C1 样蛋白 1(NPC1L1)是一种多跨膜蛋白,通过囊泡内吞作用介导膳食和胆汁胆固醇的吸收。NPC1L1 的亚细胞定位受胆固醇调节。胆固醇耗竭诱导 NPC1L1 从内体再循环隔室转运到质膜(PM),这需要 MyoVb·Rab11a·Rab11-FIP2 三聚体,胆固醇补充使 NPC1L1 与胆固醇一起内化。在这里,我们发现 GTP 结合的 Cdc42 与 NPC1L1 相互作用。胆固醇耗竭调节 Cdc42 的激活,并增强 NPC1L1-Cdc42 相互作用。组成型 GTP 结合的 Cdc42 突变体形式的过表达或 Cdc42 的敲低抑制 NPC1L1 向 PM 的转运,并扰乱 NPC1L1 与 Rab11a、MyoVb 和肌动蛋白的胆固醇调节结合。Cdc42 下游效应物 N-WASP 或 Arp3 的敲低也导致类似的结果。在肝特异性 Cdc42 敲除(Cdc42 LKO)小鼠中,NPC1L1 无法定位到胆小管,胆汁胆固醇不能被有效重吸收。这些结果表明 Cdc42 控制 NPC1L1 的胆固醇调节运输和定位,并在胆固醇吸收中发挥作用。

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The small GTPase Cdc42 interacts with Niemann-Pick C1-like 1 (NPC1L1) and controls its movement from endocytic recycling compartment to plasma membrane in a cholesterol-dependent manner.小分子 GTP 酶 Cdc42 与尼曼-匹克 C1 样蛋白 1(NPC1L1)相互作用,并以胆固醇依赖的方式控制 NPC1L1 从内体再循环隔室到质膜的运动。
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本文引用的文献

1
The N-terminal domain of NPC1L1 protein binds cholesterol and plays essential roles in cholesterol uptake.NPC1L1 蛋白的 N 端结构域与胆固醇结合,并在胆固醇摄取中发挥重要作用。
J Biol Chem. 2011 Jul 15;286(28):25088-97. doi: 10.1074/jbc.M111.244475. Epub 2011 May 20.
2
Molecular characterization of the NPC1L1 variants identified from cholesterol low absorbers.胆固醇吸收不良者中 NPC1L1 变异体的分子特征。
J Biol Chem. 2011 Mar 4;286(9):7397-408. doi: 10.1074/jbc.M110.178368. Epub 2010 Dec 28.
3
Flotillins play an essential role in Niemann-Pick C1-like 1-mediated cholesterol uptake. flotillins 在尼曼-匹克 C1 样蛋白 1 介导的胆固醇摄取中发挥重要作用。
Proc Natl Acad Sci U S A. 2011 Jan 11;108(2):551-6. doi: 10.1073/pnas.1014434108. Epub 2010 Dec 27.
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Cdc42 and vesicle trafficking in polarized cells.Cdc42 与极化细胞中的小泡运输。
Traffic. 2010 Oct;11(10):1272-9. doi: 10.1111/j.1600-0854.2010.01102.x.
5
Cyclodextrin overcomes the transport defect in nearly every organ of NPC1 mice leading to excretion of sequestered cholesterol as bile acid.环糊精克服了 NPC1 小鼠几乎所有器官的转运缺陷,导致被隔离的胆固醇作为胆汁酸排出。
J Lipid Res. 2010 May;51(5):933-44. doi: 10.1194/jlr.M000257. Epub 2009 Nov 18.
6
In-vitro characterization of the six clustered variants of NPC1L1 observed in cholesterol low absorbers.胆固醇吸收不良者中观察到的 NPC1L1 的六个聚集变体的体外特征。
Pharmacogenet Genomics. 2009 Nov;19(11):884-92. doi: 10.1097/FPC.0b013e3283327925.
7
Requirement of myosin Vb.Rab11a.Rab11-FIP2 complex in cholesterol-regulated translocation of NPC1L1 to the cell surface.肌球蛋白Vb.Rab11a.Rab11-FIP2复合物在胆固醇调节的NPC1L1向细胞表面转运中的作用
J Biol Chem. 2009 Aug 14;284(33):22481-22490. doi: 10.1074/jbc.M109.034355. Epub 2009 Jun 19.
8
Hepatocyte-specific deletion of Cdc42 results in delayed liver regeneration after partial hepatectomy in mice.在小鼠中,肝细胞特异性缺失Cdc42会导致部分肝切除术后肝脏再生延迟。
Hepatology. 2009 Jan;49(1):240-9. doi: 10.1002/hep.22610.
9
The cholesterol absorption inhibitor ezetimibe acts by blocking the sterol-induced internalization of NPC1L1.胆固醇吸收抑制剂依折麦布通过阻断固醇诱导的NPC1L1内化发挥作用。
Cell Metab. 2008 Jun;7(6):508-19. doi: 10.1016/j.cmet.2008.04.001.
10
Functional characterization of genetic variants in NPC1L1 supports the sequencing extremes strategy to identify complex trait genes.NPC1L1基因变异的功能特征支持通过测序极端个体策略来鉴定复杂性状基因。
Hum Mol Genet. 2008 Jul 15;17(14):2101-7. doi: 10.1093/hmg/ddn108. Epub 2008 Apr 15.