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CD1分子的来龙去脉:让脂质接受免疫监测。

The ins and outs of CD1 molecules: bringing lipids under immunological surveillance.

作者信息

Gumperz Jenny E

机构信息

Department of Medical Microbiology and Immunology, University of Wisconsin Medical School, Madison, 53706, USA,

出版信息

Traffic. 2006 Jan;7(1):2-13. doi: 10.1111/j.1600-0854.2005.00364.x.

Abstract

An emerging area of investigation is the role of lipids as immunological antigens. CD1 glycoproteins comprise a family of molecules that are specialized for presenting lipids, glycolipids and lipopeptides to T lymphocytes. Variations in the cytoplasmic tail sequences of CD1 isoforms lead to differential association with adaptor proteins and consequently divergent routes of intracellular trafficking, resulting in surveillance of distinct cellular sites for binding lipid antigens. CD1 molecules efficiently gain access to lipids from intracellular microbial pathogens in endosomal compartments, and the trafficking and lipid-binding specialization of CD1 isoforms may correlate with the endosomal segregation of structurally distinct lipids. Endosomal trafficking is also critical for CD1d molecules to load antigenic self-lipids that are presented to autoreactive CD1d-restricted natural killer (NK)T cells and is required for the positive selection of these unique T cells. Recent studies reveal a key role for accessory proteins that facilitate the uptake of lipid antigens by CD1 molecules. These include lysosomal lipid-transfer proteins, such as the saposins, and apolipoprotein E, the major serum factor that binds and delivers extracellular lipids to antigen-presenting cells. These advances in understanding the CD1 lipid antigen presentation system raise new considerations about the role of the immune response in lipid-related diseases.

摘要

一个新兴的研究领域是脂质作为免疫抗原的作用。CD1糖蛋白构成了一类专门将脂质、糖脂和脂肽呈递给T淋巴细胞的分子家族。CD1亚型的胞质尾序列变异导致与衔接蛋白的差异结合,进而导致细胞内运输途径不同,从而对不同的细胞位点进行脂质抗原结合监测。CD1分子能有效地从内体区室中的细胞内微生物病原体获取脂质,且CD1亚型的运输和脂质结合特异性可能与结构不同的脂质在内体中的分离有关。内体运输对于CD1d分子加载呈递给自身反应性CD1d限制性自然杀伤(NK)T细胞的抗原性自身脂质也至关重要,并且是这些独特T细胞阳性选择所必需的。最近的研究揭示了辅助蛋白在促进CD1分子摄取脂质抗原方面的关键作用。这些辅助蛋白包括溶酶体脂质转移蛋白,如鞘脂激活蛋白,以及载脂蛋白E,后者是将细胞外脂质结合并递送至抗原呈递细胞的主要血清因子。在理解CD1脂质抗原呈递系统方面的这些进展引发了关于免疫反应在脂质相关疾病中的作用的新思考。

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