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肽与 MHC Ⅰ类和Ⅱ类蛋白的结合:新方法带来的新途径。

Peptide binding to MHC class I and II proteins: new avenues from new methods.

机构信息

Biochemistry and Cell Biology, Jacobs University Bremen, Campus Ring 1, 28759 Bremen, Germany.

出版信息

Mol Immunol. 2010 Jan;47(4):649-57. doi: 10.1016/j.molimm.2009.10.008. Epub 2009 Nov 11.

Abstract

Major histocompatibility complex (MHC) class I and II proteins have been in the focus of interest for immunologists, biochemists, cell biologists, and structural biologists for decades. With dozens of entries in the Protein Data Bank, their crystal structures are now sufficiently well understood, while their dynamic properties such as peptide binding and intracellular trafficking and their immunological (as well as non-immunological) functions are still being intensely investigated. In recent years, new methods and technologies have emerged to detect and characterize the conformational changes and intermediate states that accompany peptide binding and exchange by MHC proteins. These techniques have delivered more detailed information and allowed us to compare the molecular mechanisms of peptide selection between MHC class I and II proteins, suggesting both similarities and differences. Here, we review these recent achievements and suggest avenues for further work.

摘要

主要组织相容性复合体(MHC)I 类和 II 类蛋白几十年来一直是免疫学家、生物化学家、细胞生物学家和结构生物学家关注的焦点。目前,它们的晶体结构已经得到了充分的理解,有数十个条目收录在蛋白质数据库中,而它们的动态特性,如肽结合和细胞内运输,以及它们的免疫(和非免疫)功能仍在被深入研究。近年来,出现了新的方法和技术来检测和描述 MHC 蛋白结合和交换肽时伴随的构象变化和中间状态。这些技术提供了更详细的信息,并使我们能够比较 MHC 类 I 和 II 蛋白之间的肽选择的分子机制,表明存在相似之处和差异。在这里,我们回顾这些最新的研究成果,并提出进一步研究的途径。

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