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多态性DQα和DQβ相互作用决定了同种异体识别的HLA II类决定簇。

Polymorphic DQ alpha and DQ beta interactions dictate HLA class II determinants of allo-recognition.

作者信息

Kwok W W, Mickelson E, Masewicz S, Milner E C, Hansen J, Nepom G T

机构信息

Virginia Mason Research Center, Seattle, WA 98101.

出版信息

J Exp Med. 1990 Jan 1;171(1):85-95. doi: 10.1084/jem.171.1.85.

Abstract

18 transfected cell lines were generated that expressed distinct DQ molecules related to the serologically defined HLA-DQw3 specificity. These transfectants were constructed using site-directed mutagenesis to introduce nucleotide substitutions into DQ3.2 beta cDNA, followed by retrovirus-mediated gene expression of the mutagenized genes in human B cell lines with different endogenous DQ alpha chains. The capacity of particular class II dimers to stimulate alloreactive T cell clones was investigated. T cell activation was found to be dependent on both DQ alpha and DQ beta chains. In some cases, single amino acid substitutions at codons 13, 26, 45, or 57 of the DQ beta chain were sufficient to dramatically alter T cell reactivity; T cell recognition of these substitutions, however, was strongly influenced by the alpha chain polymorphisms present in the stimulatory class II dimer. Both gain and loss of major serologic and cellular specificities associated with specific DQw3+ alleles were observed with a limited array of site-directed substitutions.

摘要

产生了18个转染细胞系,它们表达与血清学定义的HLA - DQw3特异性相关的不同DQ分子。这些转染体是通过定点诱变构建的,将核苷酸取代引入DQ3.2β cDNA,然后通过逆转录病毒介导诱变基因在具有不同内源性DQα链的人B细胞系中的基因表达。研究了特定II类二聚体刺激同种异体反应性T细胞克隆的能力。发现T细胞活化依赖于DQα链和DQβ链。在某些情况下,DQβ链第13、26、45或57位密码子处的单个氨基酸取代足以显著改变T细胞反应性;然而,T细胞对这些取代的识别受到刺激II类二聚体中存在的α链多态性的强烈影响。通过有限的一系列定点取代观察到与特定DQw3 +等位基因相关的主要血清学和细胞特异性的获得和丧失。

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