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HLA A03 超型和几种物种主要组织相容性复合体 I 类 A 同种异型共享 F 口袋中结合正电荷残基的偏好:对控制逆转录病毒感染的影响。

The HLA A03 Supertype and Several Species Major Histocompatibility Complex Class I A Allotypes Share a Preference for Binding Positively Charged Residues in the F Pocket: Implications for Controlling Retroviral Infections.

机构信息

Comparative Genetics and Refinement, Biomedical Primate Research Centre, Rijswijk, The Netherlands

Comparative Genetics and Refinement, Biomedical Primate Research Centre, Rijswijk, The Netherlands.

出版信息

J Virol. 2020 Apr 16;94(9). doi: 10.1128/JVI.01960-19.

DOI:10.1128/JVI.01960-19
PMID:32075930
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7163143/
Abstract

The major histocompatibility complex (MHC) class I region of humans, chimpanzees (), and bonobos () is highly similar, and orthologues of , -, and - are present in both species. Based on functional characteristics, the different HLA-A allotypes are classified into different supertypes. One of them, the HLA A03 supertype, is widely distributed among different human populations. All contemporary known chimpanzee and bonobo MHC class I A allotypes cluster genetically into one of the six families, the family. We report here that the peptide-binding motif of the Patr-A*05:01 allotype, which is commonly present in a cohort of western African chimpanzees, has a strong preference for binding peptides with basic amino acids at the carboxyl terminus. This phenomenon is shared with the family members of the HLA A03 supertype. Based on the chemical similarities in the peptide-binding pocket, we inferred that the preference for binding peptides with basic amino acids at the carboxyl terminus is widely present among the human, chimpanzee, and bonobo MHC-A allotypes. Subsequent peptide-binding predictions illustrated that these allotypes have the capacity to target conserved parts of the proteome of human immunodeficiency virus type 1 (HIV-1) and the simian immunodeficiency virus SIVcpz. Most experimentally infected chimpanzees seem to control an HIV-1 infection and are therefore considered to be relatively resistant to developing AIDS. Contemporary free-ranging chimpanzees may carry SIVcpz, and there is evidence for AIDS-like symptoms in these free-ranging animals, whereas SIV infections in bonobos appear to be absent. In humans, the natural control of an HIV-1 infection is strongly associated with the presence of particular HLA class I allotypes. The ancestor of the contemporary living chimpanzees and bonobos survived a selective sweep targeting the MHC class I repertoire. We have put forward a hypothesis that this may have been caused by an ancestral retroviral infection similar to SIVcpz. Characterization of the relevant MHC allotypes may contribute to understanding the shaping of their immune repertoire. The abundant presence of MHC-A allotypes that prefer peptides with basic amino acids at the C termini suggests that these molecules may contribute to the control of retroviral infections in humans, chimpanzees, and bonobos.

摘要

人类、黑猩猩()和倭黑猩猩()的主要组织相容性复合体(MHC)I 类区域高度相似,并且在这两个物种中都存在、-和-的直系同源物。根据功能特征,不同的 HLA-A 同种异型分为不同的超型。其中之一,HLA A03 超型广泛分布于不同的人类群体中。所有当代已知的黑猩猩和倭黑猩猩 MHC I 类 A 同种异型在遗传上都聚类为六个家族之一,即家族。我们在此报告,在一组西部非洲黑猩猩中常见的 Patr-A*05:01 同种异型的肽结合基序对羧基末端具有碱性氨基酸的肽具有强烈的结合偏好。这种现象与 HLA A03 超型的家族成员共享。基于肽结合口袋中的化学相似性,我们推断出对羧基末端具有碱性氨基酸的肽的结合偏好广泛存在于人类、黑猩猩和倭黑猩猩 MHC-A 同种异型中。随后的肽结合预测表明,这些同种异型具有靶向人类免疫缺陷病毒 1(HIV-1)和猿猴免疫缺陷病毒 SIVcpz 的蛋白质组保守部分的能力。大多数实验感染的黑猩猩似乎控制了 HIV-1 感染,因此被认为相对不易发展为艾滋病。当代自由放养的黑猩猩可能携带 SIVcpz,并且在这些自由放养的动物中存在类似于艾滋病的症状的证据,而在倭黑猩猩中 SIV 感染似乎不存在。在人类中,对 HIV-1 感染的自然控制与特定 HLA 类 I 同种异型的存在强烈相关。当代存活的黑猩猩和倭黑猩猩的祖先经历了针对 MHC I 类库的选择性清除。我们提出了一个假设,即这可能是由类似于 SIVcpz 的祖先逆转录病毒感染引起的。相关 MHC 同种异型的特征描述可能有助于了解其免疫库的形成。大量存在的 C 末端具有碱性氨基酸的 MHC-A 同种异型表明,这些分子可能有助于控制人类、黑猩猩和倭黑猩猩中的逆转录病毒感染。