从大规模 MHC I 类配体分析中获得的 MHC I 类抗原加工的见解。
Insights into MHC class I antigen processing gained from large-scale analysis of class I ligands.
机构信息
Institute for Cell Biology, Department of Immunology, Eberhard Karls University Tübingen, Tübingen, Germany.
出版信息
Cell Mol Life Sci. 2011 May;68(9):1521-32. doi: 10.1007/s00018-011-0659-9. Epub 2011 Mar 9.
Abstract
Short peptides derived from intracellular proteins and presented on MHC class I molecules on the cell surface serve as a showcase for the immune system to detect pathogenic or malignant alterations inside the cell, and the sequencing and analysis of the presented peptide pool has received considerable attention over the last two decades. In this review, we give a comprehensive presentation of the methods employed for the large-scale qualitative and quantitative analysis of the MHC class I ligandome. Furthermore, we focus on insights gained into the underlying processing pathway, especially involving the roles of the proteasome, the TAP complex, and the peptide specificities and motifs of MHC molecules. The identification of post-translational modifications in MHC ligands and their implications for processing are also considered. Finally, we review the correlations of the ligandome to the proteome and the transcriptome.
摘要
从细胞内蛋白质衍生而来并呈现在细胞表面 MHC I 类分子上的短肽,作为免疫系统检测细胞内病原体或恶性改变的展示架,过去二十年来,对呈递肽库的测序和分析受到了相当大的关注。在这篇综述中,我们全面介绍了用于大规模定性和定量分析 MHC I 类配体组的方法。此外,我们还重点介绍了对潜在加工途径的深入了解,特别是涉及蛋白酶体、TAP 复合物以及 MHC 分子的肽特异性和基序的作用。还考虑了 MHC 配体中翻译后修饰的鉴定及其对加工的影响。最后,我们回顾了配体组与蛋白质组和转录组的相关性。
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