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编码区多态性对人TCR Vβ基因外周表达的影响。

Influence of coding region polymorphism on the peripheral expression of a human TCR V beta gene.

作者信息

Vissinga C S, Charmley P, Concannon P

机构信息

Virginia Mason Research Center, Seattle, WA 98101.

出版信息

J Immunol. 1994 Feb 1;152(3):1222-7.

PMID:8301127
Abstract

A number of human TCR V beta gene segments are reported to be polymorphic, with alleles differing by one or a small number of amino acid substitutions. In the absence of detailed structural information regarding the interaction of specific positions in the TCR with Ag or MHC, the significance of such variation is difficult to assess. In this report the relative use of the two common alleles of the human V beta 6.7 gene, 6.7a and 6.7b, which differ by two non-conservative amino acid substitutions, and the use of two common alleles of the V beta 12.2 gene, which differ by only silent substitutions, were measured in PBL derived from individuals heterozygous for these alleles. Equal use of V beta 12.2 alleles was observed, consistent with the inability of selection mechanisms to discriminate between the products of these alleles that are indistinguishable at the amino acid level. However, statistically significant skewing in the use of V beta 6.7 alleles was observed in 15 of 16 individuals studied. Expression levels for each allele ranged from 16 to 84% of the total V beta 6.7 signal in heterozygous individuals, with either the 6.7a or the 6.7b allele predominant in different individuals. Based on segregation studies in families, it seems unlikely that other unidentified polymorphism in the TCR beta locus, such as in the V beta 6.7 promoter, was responsible for the differential allele expression. Family studies provided no evidence for an association between specific HLA haplotypes and V beta 6.7 allele use. These results indicate that even modest allelic variation in human TCR V beta coding regions can have a significant impact on the expression of human V beta genes in the peripheral repertoire.

摘要

据报道,一些人类TCR Vβ基因片段具有多态性,其等位基因之间存在一个或少数几个氨基酸替换的差异。由于缺乏关于TCR中特定位置与抗原或MHC相互作用的详细结构信息,这种变异的意义难以评估。在本报告中,对人类Vβ6.7基因的两个常见等位基因6.7a和6.7b(它们有两个非保守氨基酸替换的差异)以及Vβ12.2基因的两个常见等位基因(它们仅有沉默替换的差异)的相对使用情况,在来自这些等位基因杂合个体的外周血淋巴细胞(PBL)中进行了测定。观察到Vβ12.2等位基因的使用情况相同,这与选择机制无法区分这些在氨基酸水平上无法区分的等位基因产物一致。然而,在16名研究个体中的15名中观察到Vβ6.7等位基因使用存在统计学上显著的偏差。在杂合个体中,每个等位基因的表达水平占Vβ6.7总信号的16%至84%,在不同个体中,6.7a或6.7b等位基因占主导。基于家族中的分离研究,TCRβ基因座中其他未确定的多态性(如Vβ6.7启动子中的多态性)似乎不太可能是等位基因差异表达的原因。家族研究没有提供证据表明特定的HLA单倍型与Vβ6.7等位基因使用之间存在关联。这些结果表明,即使人类TCR Vβ编码区中等位基因的微小变异也可能对外周库中人类Vβ基因的表达产生重大影响。

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