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单体 HLA-G 的结构和稳定性受结合肽的性质影响。

The structure and stability of the monomorphic HLA-G are influenced by the nature of the bound peptide.

机构信息

The Protein Crystallography Unit, Department of Biochemistry and Molecular Biology, School of Biomedical Sciences, Monash University, Clayton, Victoria 3800, Australia.

出版信息

J Mol Biol. 2010 Mar 26;397(2):467-80. doi: 10.1016/j.jmb.2010.01.052. Epub 2010 Feb 1.

DOI:10.1016/j.jmb.2010.01.052
PMID:20122941
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2905647/
Abstract

The highly polymorphic major histocompatibility complex class Ia (MHC-Ia) molecules present a broad array of peptides to the clonotypically diverse alphabeta T-cell receptors. In contrast, MHC-Ib molecules exhibit limited polymorphism and bind a more restricted peptide repertoire, in keeping with their major role in innate immunity. Nevertheless, some MHC-Ib molecules do play a role in adaptive immunity. While human leukocyte antigen E (HLA-E), the MHC-Ib molecule, binds a very restricted repertoire of peptides, the peptide binding preferences of HLA-G, the class Ib molecule, are less stringent, although the basis by which HLA-G can bind various peptides is unclear. To investigate how HLA-G can accommodate different peptides, we compared the structure of HLA-G bound to three naturally abundant self-peptides (RIIPRHLQL, KGPPAALTL and KLPQAFYIL) and their thermal stabilities. The conformation of HLA-G(KGPPAALTL) was very similar to that of the HLA-G(RIIPRHLQL) structure. However, the structure of HLA-G(KLPQAFYIL) not only differed in the conformation of the bound peptide but also caused a small shift in the alpha2 helix of HLA-G. Furthermore, the relative stability of HLA-G was observed to be dependent on the nature of the bound peptide. These peptide-dependent effects on the substructure of the monomorphic HLA-G are likely to impact on its recognition by receptors of both innate and adaptive immune systems.

摘要

高度多态的主要组织相容性复合体 I 类 (MHC-I) 分子向克隆型多样化的αβ T 细胞受体呈递广泛的肽。相比之下,MHC-Ib 分子表现出有限的多态性,结合更有限的肽库,与其在先天免疫中的主要作用一致。然而,一些 MHC-Ib 分子确实在适应性免疫中发挥作用。虽然人类白细胞抗原 E (HLA-E) 是 MHC-Ib 分子,结合非常有限的肽库,但 MHC-Ib 分子 HLA-G 的肽结合偏好不太严格,尽管 HLA-G 可以结合各种肽的基础尚不清楚。为了研究 HLA-G 如何容纳不同的肽,我们比较了结合三种天然丰富的自身肽 (RIIPRHLQL、KGPPAALTL 和 KLPQAFYIL) 的 HLA-G 的结构及其热稳定性。HLA-G (KGPPAALTL) 的构象与 HLA-G (RIIPRHLQL) 结构非常相似。然而,HLA-G (KLPQAFYIL) 的结构不仅在结合肽的构象上有所不同,而且还导致 HLA-G 的α2 螺旋发生小位移。此外,观察到 HLA-G 的相对稳定性取决于结合肽的性质。这些肽依赖性效应对单态 HLA-G 的亚结构可能会影响其被先天和适应性免疫系统受体的识别。

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