Fink P J, Blair M J, Matis L A, Hedrick S M
Department of Immunology, Research Institute of Scripps Clinic, La Jolla, California 92037.
J Exp Med. 1990 Jul 1;172(1):139-50. doi: 10.1084/jem.172.1.139.
Immunization of both B10.A and B10.S(9R) mice with pigeon cytochrome c (pcc) elicits T cells capable of proliferating to pcc presented on I-E major histocompatibility complex (MHC) molecules. The T cell receptor (TCR) repertoire used by pcc-specific T cells from these two strains is markedly different, even for T cells recognizing very similar antigen/MHC complexes. Our current studies have been directed toward explaining this differential expression between MHC congenic strains of TCR gene elements capable of recognizing similar ligands. Analysis of the TCR repertoire of pcc-specific T cells from F1[B10.A x B10.S (9R)]----parent radiation chimeras has demonstrated that much of this difference is a result of the positive selection of T cells for MHC restriction specificity. Further analysis of T cell lines from F1 mice and from radiation chimeras stimulated in vitro with pcc on both B10.A and B10.S(9R) antigen-presenting cells has provided clear-cut examples of the influence of positive selection, tolerance induction and of both in vivo and in vitro antigen presentation on the shaping of the TCR repertoire for a protein antigen. This is the first molecular analysis of how positive selection, tolerance induction, and antigen presentation can combine to mold the TCR repertoire.
用鸽细胞色素c(pcc)对B10.A和B10.S(9R)小鼠进行免疫,可引发能够增殖以应对I-E主要组织相容性复合体(MHC)分子呈递的pcc的T细胞。来自这两个品系的pcc特异性T细胞所使用的T细胞受体(TCR)库明显不同,即使对于识别非常相似的抗原/MHC复合体的T细胞也是如此。我们目前的研究旨在解释能够识别相似配体的TCR基因元件在MHC同基因品系之间的这种差异表达。对来自F1[B10.A×B10.S(9R)]-亲本辐射嵌合体的pcc特异性T细胞的TCR库分析表明,这种差异很大程度上是T细胞针对MHC限制特异性进行阳性选择的结果。对来自F1小鼠和辐射嵌合体的T细胞系进行进一步分析,这些细胞系在体外由B10.A和B10.S(9R)抗原呈递细胞用pcc刺激,这为阳性选择、耐受诱导以及体内和体外抗原呈递对蛋白质抗原TCR库形成的影响提供了明确的例子。这是对阳性选择、耐受诱导和抗原呈递如何共同塑造TCR库的首次分子分析。
