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多态性HLA - DRβ链残基在向T细胞呈递病毒抗原中的作用。

The role of polymorphic HLA-DR beta chain residues in presentation of viral antigens to T cells.

作者信息

Karr R W, Yu W, Watts R, Evans K S, Celis E

机构信息

Department of Veterans Affairs Medical Center, University of Iowa College of Medicine, Iowa City 52242.

出版信息

J Exp Med. 1990 Jul 1;172(1):273-83. doi: 10.1084/jem.172.1.273.

Abstract

The relative importance of 11 polymorphic positions in the HLA-DR7 beta 1 chain in T cell recognition of foreign antigens was investigated using transfectants expressing mutant DR7 beta 1 chains as APC for five rabies virus-specific T cell clones. The results indicate that multiple amino acids, located in both the beta-strands and alpha-helix of DR7 beta 1 in the model of a class II molecule, are involved in DR7-restricted T cell recognition of these antigens. Many of the substitutions appeared to reduce the affinity of an antigenic peptide for the mutant DR7 molecules but did not prevent binding. The heterogeneity of responses of the three G-specific T cell clones to presentation of the G11.3 peptide by several of the mutant DR7 molecules indicates that the T cell receptor (TCR) of each these clones requires a different view of the G11.3/DR7 complex and raises the possibility that the G11.3 peptide may bind to the DR7 molecule in more than one conformation.

摘要

利用表达突变型DR7β1链的转染细胞作为抗原呈递细胞(APC),针对五个狂犬病病毒特异性T细胞克隆,研究了HLA - DR7β1链中11个多态性位点在T细胞识别外来抗原中的相对重要性。结果表明,在II类分子模型中,位于DR7β1的β链和α螺旋中的多个氨基酸参与了DR7限制性T细胞对这些抗原的识别。许多替换似乎降低了抗原肽与突变型DR7分子的亲和力,但并未阻止结合。三个G特异性T细胞克隆对几种突变型DR7分子呈递G11.3肽的反应异质性表明,这些克隆中的每一个的T细胞受体(TCR)需要对G11.3/DR7复合物有不同的视角,并增加了G11.3肽可能以不止一种构象与DR7分子结合的可能性。

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Molecular diversity of HLA-DR4 haplotypes.HLA-DR4单倍型的分子多样性。
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