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T细胞受体与I类重链的相互作用影响T细胞选择。

T cell receptor interactions with class I heavy-chain influence T cell selection.

作者信息

Kuhns S T, Tallquist M D, Johnson A J, Mendez-Fernandez Y, Pease L R

机构信息

Departments of Biochemistry and Molecular Biology, Mayo Clinic/Foundation, Rochester, MN 55905, USA.

出版信息

Proc Natl Acad Sci U S A. 2000 Jan 18;97(2):756-60. doi: 10.1073/pnas.97.2.756.

Abstract

The interaction of the T cell receptor (TCR) with peptide in the binding site of the major histocompatibility complex molecule provides the basis for T cell recognition during immune surveillance, repertoire development, and tolerance. Little is known about the extent to which repertoire selection is influenced directly by variation of the structure of the class I heavy chain. We find that the 2C TCR, normally positively selected in the context of the K(b) molecule, is minimally selected into the CD8 lineage in the absence of antigen-processing genes. This finding underscores the importance of peptides in determining the positive-selecting class I ligands in the thymus. In contrast, K(bm3), a variant class I molecule that normally exerts a negative selection pressure on 2C-bearing T cells, positively selects 2C transgenic T cells into the CD8 lineage in an antigen-processing gene-deficient environment. These findings indicate that structural changes in the heavy chain can have direct influence in T cell recognition, from which we conclude that the nature of TCR interaction with class I heavy chain influences the array of TCRs selected during development of the functional adult repertoire.

摘要

T细胞受体(TCR)与主要组织相容性复合体分子结合位点中的肽相互作用,为免疫监视、库发育和耐受性过程中的T细胞识别提供了基础。关于I类重链结构变异直接影响库选择的程度,目前所知甚少。我们发现,通常在K(b)分子背景下被阳性选择的2C TCR,在缺乏抗原加工基因的情况下,极少被选择进入CD8谱系。这一发现强调了肽在胸腺中确定阳性选择的I类配体方面的重要性。相反,K(bm3)是一种变异的I类分子,通常对携带2C的T细胞施加阴性选择压力,但在抗原加工基因缺陷的环境中,它能将2C转基因T细胞阳性选择进入CD8谱系。这些发现表明,重链的结构变化可直接影响T细胞识别,由此我们得出结论,TCR与I类重链相互作用的性质会影响功能性成年库发育过程中所选择的TCR阵列。

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