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与H-2Kb结合的肽段中P2和P3残基的特性决定小鼠Ly49C的识别。

Identities of P2 and P3 Residues of H-2Kb-Bound Peptides Determine Mouse Ly49C Recognition.

作者信息

Marquez Elsa A, Kane Kevin P

机构信息

Medical Microbiology and Immunology, University of Alberta, Edmonton, Alberta, Canada.

出版信息

PLoS One. 2015 Jul 6;10(7):e0131308. doi: 10.1371/journal.pone.0131308. eCollection 2015.

Abstract

Ly49 receptors can be peptide selective in their recognition of MHC-I-peptide complexes, affording them a level of discrimination beyond detecting the presence or absence of specific MHC-I allele products. Despite this ability, little is understood regarding the properties that enable some peptides, when bound to MHC-I molecules, to support Ly49 recognition, but not others. Using RMA-S target cells expressing MHC-I molecules loaded with individual peptides and effector cells expressing the ectodomain of the inhibitory Ly49C receptor, we found that two adjacent amino acid residues, P2 and P3, both buried in the peptide binding groove of H-2Kb, determine mouse Ly49C specificity. If both are aliphatic residues, this is supportive. Whereas, small amino acids at P2 and aromatic amino acids at the P3 auxiliary anchor residue are detrimental to Ly49C recognition. These results resemble those with a rat Ly49 where the identity of a peptide anchor residue determines recognition, suggesting that dependence on specific peptide residues buried in the MHC-I peptide-binding groove may be fundamental to Ly49 peptide selectivity and recognition.

摘要

Ly49受体在识别MHC-I-肽复合物时具有肽选择性,这使它们具有一定的辨别能力,不仅仅是检测特定MHC-I等位基因产物的存在与否。尽管有这种能力,但对于某些肽与MHC-I分子结合时能够支持Ly49识别而其他肽则不能的特性,人们了解甚少。利用表达加载有单个肽的MHC-I分子的RMA-S靶细胞和表达抑制性Ly49C受体胞外域的效应细胞,我们发现两个相邻的氨基酸残基P2和P3(均埋藏在H-2Kb的肽结合槽中)决定了小鼠Ly49C的特异性。如果两者都是脂肪族残基,则具有支持作用。而P2处的小氨基酸和P3辅助锚定残基处的芳香族氨基酸对Ly49C识别不利。这些结果与大鼠Ly49的情况相似,即肽锚定残基的特性决定识别,这表明依赖埋藏在MHC-I肽结合槽中的特定肽残基可能是Ly49肽选择性和识别的基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8e20/4493100/dd7d0854019d/pone.0131308.g001.jpg

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