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恒河猴 FcγR2A 和 FcγR3A 常见同种异型与人类和恒河猴 IgG 亚类的功能相互作用。

Functional Interactions of Common Allotypes of Rhesus Macaque FcγR2A and FcγR3A with Human and Macaque IgG Subclasses.

机构信息

Department of Pathology and Laboratory Medicine, University of Wisconsin-Madison, Madison, WI 53705; and.

Wisconsin National Primate Research Center, University of Wisconsin-Madison, Madison, WI 53715.

出版信息

J Immunol. 2020 Dec 15;205(12):3319-3332. doi: 10.4049/jimmunol.2000501. Epub 2020 Nov 18.

DOI:10.4049/jimmunol.2000501
PMID:33208458
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7725946/
Abstract

The rhesus macaque is an important animal model for AIDS and other infectious diseases. However, the investigation of Fc-mediated Ab responses in macaques is complicated by species-specific differences in FcγRs and IgG subclasses relative to humans. To assess the effects of these differences on FcγR-IgG interactions, reporter cell lines expressing common allotypes of human and rhesus macaque FcγR2A and FcγR3A were established. FcγR-mediated responses to B cells were measured in the presence of serial dilutions of anti-CD20 Abs with Fc domains corresponding to each of the four subclasses of human and rhesus IgG and with Fc variants of IgG1 that enhance binding to FcγR2A or FcγR3A. All of the FcγRs were functional and preferentially recognized either IgG1 or IgG2. Whereas allotypes of rhesus FcγR2A were identified with responses similar to variants of human FcγR2A with higher (H131) and lower (R131) affinity for IgG, all of the rhesus FcγR3A allotypes exhibited responses most similar to the higher affinity V158 variant of human FcγR3A. Unlike responses to human IgGs, there was little variation in FcγR-mediated responses to different subclasses of rhesus IgG. Phylogenetic comparisons suggest that this reflects limited sequence variation of macaque IgGs as a result of their relatively recent diversification from a common gene since humans and macaques last shared a common ancestor. These findings reveal species-specific differences in FcγR-IgG interactions with important implications for investigating Ab effector functions in macaques.

摘要

食蟹猴是艾滋病和其他传染病的重要动物模型。然而,由于食蟹猴与人类FcγR 和 IgG 亚类在种属上存在特异性差异,因此对 Fc 介导的 Ab 反应的研究较为复杂。为了评估这些差异对 FcγR-IgG 相互作用的影响,我们建立了表达常见同种型的人源和食蟹猴 FcγR2A 和 FcγR3A 的报告细胞系。在存在对应于人源和食蟹猴 IgG 的四个亚类的 Fc 结构域的抗 CD20 Ab 的系列稀释液的情况下,测量了 FcγR 介导的对 B 细胞的反应,并且还测量了 Fc 变体 IgG1 与 FcγR2A 或 FcγR3A 结合增强的情况下对 FcγR 的反应。所有的 FcγR 均具有功能,并且优先识别 IgG1 或 IgG2。尽管鉴定出了食蟹猴 FcγR2A 的同种型,但其与对 IgG 具有更高(H131)和更低(R131)亲和力的人源 FcγR2A 变体的反应相似,但是所有的食蟹猴 FcγR3A 同种型均表现出与对人源 FcγR3A 的高亲和力 V158 变体最相似的反应。与对人源 IgGs 的反应不同,对食蟹猴不同 IgG 亚类的 FcγR 介导的反应变化不大。系统发育比较表明,这反映了由于人类和食蟹猴最近从一个共同的基因分化而来,因此食蟹猴 IgGs 的序列变化有限。这些发现揭示了 FcγR-IgG 相互作用中的种属特异性差异,这对研究食蟹猴 Ab 效应功能具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1761/7725946/a01f6c49de31/nihms-1640338-f0006.jpg
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https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1761/7725946/dac231014268/nihms-1640338-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1761/7725946/d658fe9c9f45/nihms-1640338-f0002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1761/7725946/25bf6253ff32/nihms-1640338-f0003.jpg
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