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甾醇调节的糖脂分选发生在尼曼-皮克C1晚期内体中。

Sterol-modulated glycolipid sorting occurs in niemann-pick C1 late endosomes.

作者信息

Zhang M, Dwyer N K, Neufeld E B, Love D C, Cooney A, Comly M, Patel S, Watari H, Strauss J F, Pentchev P G, Hanover J A, Blanchette-Mackie E J

机构信息

Lipid Cell Biology Section and Cell Biochemistry Section, Laboratory of Cell Biochemistry and Biology, NIDDK, National Institutes of Health, Bethesda, Maryland 20892, USA.

出版信息

J Biol Chem. 2001 Feb 2;276(5):3417-25. doi: 10.1074/jbc.M005393200. Epub 2000 Oct 13.

DOI:10.1074/jbc.M005393200
PMID:11032830
Abstract

The Niemann-Pick C1 (NPC1) protein and endocytosed low density lipoprotein (LDL)-derived cholesterol were shown to enrich separate subsets of vesicles containing lysosomal associated membrane protein 2. Localization of Rab7 in the NPC1-containing vesicles and enrichment of lysosomal hydrolases in the cholesterol-containing vesicles confirmed that these organelles were late endosomes and lysosomes, respectively. Lysobisphosphatidic acid, a lipid marker of the late endosomal pathway, was found in the cholesterol-enriched lysosomes. Recruitment of NPC1 to Rab7 compartments was stimulated by cellular uptake of cholesterol. The NPC1 compartment was shown to be enriched in glycolipids, and internalization of GalNAcbeta1-4[NeuAcalpha2-3]Galbeta1-4Glcbeta1-1'-ceramide (G(M2)) into endocytic vesicles depends on the presence of NPC1 protein. The glycolipid profiles of the NPC1 compartment could be modulated by LDL uptake and accumulation of lysosomal cholesterol. Expression in cells of biologically active NPC1 protein fused to green fluorescent protein revealed rapidly moving and flexible tubular extensions emanating from the NPC1-containing vesicles. We conclude that the NPC1 compartment is a dynamic, sterol-modulated sorting organelle involved in the trafficking of plasma membrane-derived glycolipids as well as plasma membrane and endocytosed LDL cholesterol.

摘要

已证实,尼曼-皮克C1(NPC1)蛋白和经内吞作用摄取的低密度脂蛋白(LDL)衍生的胆固醇分别富集于含有溶酶体相关膜蛋白2的不同囊泡亚群中。Rab7在含NPC1的囊泡中的定位以及溶酶体水解酶在含胆固醇囊泡中的富集证实,这些细胞器分别是晚期内体和溶酶体。在富含胆固醇的溶酶体中发现了晚期内体途径的脂质标志物——溶血双磷脂酸。细胞摄取胆固醇可刺激NPC1向Rab7区室的募集。已表明NPC1区室富含糖脂,并且N-乙酰半乳糖胺β1-4[唾液酸α2-3]半乳糖β1-4葡萄糖β1-1'-神经酰胺(GM2)内化到内吞囊泡中依赖于NPC1蛋白的存在。NPC1区室的糖脂谱可通过LDL摄取和溶酶体胆固醇的积累进行调节。与绿色荧光蛋白融合的具有生物活性的NPC1蛋白在细胞中的表达显示,从含NPC1的囊泡发出快速移动且灵活的管状延伸。我们得出结论,NPC1区室是一个动态的、受固醇调节的分选细胞器,参与源自质膜的糖脂以及质膜和经内吞作用摄取的LDL胆固醇的运输。

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