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人类白细胞抗原-DR多态性影响其与CD4的相互作用。

HLA-DR polymorphism affects the interaction with CD4.

作者信息

Fleury S, Thibodeau J, Croteau G, Labrecque N, Aronson H E, Cantin C, Long E O, Sékaly R P

机构信息

Laboratoire d'Immunologie, Institut de Recherches Clinques de Montréal, Québec, Canada.

出版信息

J Exp Med. 1995 Sep 1;182(3):733-41. doi: 10.1084/jem.182.3.733.

Abstract

Major histocompatibility complex (MHC) class II molecules are highly polymorphic and bind peptides for presentation to CD4+ T cells. Functional and adhesion assays have shown that CD4 interacts with MHC class II molecules, leading to enhanced responses of CD4+ T cells after the activation of the CD4-associated tyrosine kinase p56lck. We have addressed the possible contribution of allelic polymorphism in the interaction between CD4 and MHC class II molecules. Using mouse DAP-3-transfected cells expressing different isotypes and allelic forms of the HLA-DR molecule, we have shown in a functional assay that a hierarchy exists in the ability of class II molecules to interact with CD4. Also, the study of DR4 subtypes minimized the potential contribution of polymorphic residues of the peptide-binding groove in the interaction with CD4. Chimeras between the DR4 or DR1 molecules, which interact efficiently with CD4, and DRw53, which interacts poorly, allowed the mapping of polymorphic residues between positions beta 180 and 189 that can exert a dramatic influence on the interaction with CD4.

摘要

主要组织相容性复合体(MHC)II类分子具有高度多态性,能结合肽段并呈递给CD4+ T细胞。功能和黏附分析表明,CD4与MHC II类分子相互作用,在与CD4相关的酪氨酸激酶p56lck激活后,会导致CD4+ T细胞反应增强。我们探讨了等位基因多态性在CD4与MHC II类分子相互作用中的可能作用。利用表达不同同种型和HLA-DR分子等位基因形式的小鼠DAP-3转染细胞,我们在功能分析中表明,II类分子与CD4相互作用的能力存在等级差异。此外,对DR4亚型的研究将肽结合槽多态性残基在与CD4相互作用中的潜在作用降至最低。能与CD4有效相互作用的DR4或DR1分子与几乎不与CD4相互作用的DRw53之间的嵌合体,使得能够定位β180至189位之间的多态性残基,这些残基可对与CD4的相互作用产生显著影响。

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