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功能性早期内体是人类B淋巴母细胞中主要组织相容性复合体II类分子成熟所必需的。

Functional early endosomes are required for maturation of major histocompatibility complex class II molecules in human B lymphoblastoid cells.

作者信息

Pond L, Watts C

机构信息

Department of Biochemistry, Wellcome Trust Building, University of Dundee, Dundee DD1 4HN, United Kingdom.

出版信息

J Biol Chem. 1999 Jun 18;274(25):18049-54. doi: 10.1074/jbc.274.25.18049.

DOI:10.1074/jbc.274.25.18049
PMID:10364256
Abstract

Major histocompatibility complex (MHC) class II molecules are targeted together with their invariant chain (Ii) chaperone from the secretory pathway to the endocytic pathway. Within the endosome/lysosome system, Ii must be degraded to enable peptide capture by MHC class II molecules. It remains controversial exactly which route or routes MHC class II/Ii complexes take to reach the sites of Ii processing and peptide loading. We have asked whether early endosomes are required for successful maturation of MHC class II molecules by using an in situ peroxidase/diaminobenzidine compartment ablation technique. Cells whose early endosomes were selectively ablated using transferrin-horseradish peroxidase conjugates fail to mature their newly synthesized MHC class II molecules. We show that whereas transport of secretory Ig through the secretory pathway is virtually normal in the ablated cells, newly synthesized MHC class II/Ii complexes never reach compartments capable of processing Ii. These results strongly suggest that the transport of the bulk of newly synthesized MHC class II molecules through early endosomes is obligatory and that direct input into later endosomes/lysosomes does not take place.

摘要

主要组织相容性复合体(MHC)II类分子与其恒定链(Ii)伴侣一起从分泌途径靶向至内吞途径。在内体/溶酶体系统中,Ii必须被降解,以使MHC II类分子能够捕获肽段。MHC II类/Ii复合物究竟通过哪条或哪些途径到达Ii加工和肽段装载位点仍存在争议。我们通过原位过氧化物酶/二氨基联苯胺区室消融技术,研究了早期内体对于MHC II类分子成功成熟是否是必需的。使用转铁蛋白-辣根过氧化物酶偶联物选择性消融早期内体的细胞,无法使其新合成的MHC II类分子成熟。我们发现,虽然分泌型Ig通过分泌途径的运输在消融细胞中基本正常,但新合成的MHC II类/Ii复合物从未到达能够加工Ii的区室。这些结果强烈表明,大部分新合成的MHC II类分子通过早期内体的运输是必需的,且不会直接进入晚期内体/溶酶体。

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