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小鼠细胞毒性T淋巴细胞的一个亚群在其他H-2 I类分子的背景下识别同种异体H-2 I类抗原。

A subpopulation of mouse cytotoxic T lymphocytes recognizes allogeneic H-2 class I antigens in the context of other H-2 class I molecules.

作者信息

Kievits F, Ivanyi P

机构信息

Central Laboratory of The Netherlands Red Cross Blood Transfusion Service, Amsterdam.

出版信息

J Exp Med. 1991 Jul 1;174(1):15-9. doi: 10.1084/jem.174.1.15.

Abstract

Recently, independent lines of evidence strongly suggested that peptides derived from one foreign major histocompatibility complex (MHC) molecule bound to another MHC molecule can give rise to multiple composite MHC complexes that are able to stimulate allo-(xeno)-reactive T cells. In this study, we describe that in vivo immunization of mice with cells mismatched with the recipient for a single class I antigen results in the induction of CD8+ cytotoxic T lymphocytes (CTL) specific for allogeneic class I locus products (Dd, Kd, Dq) in the context of other class I molecules (Ks, Kd, Kk) present on stimulator cells. Evidently, the target antigen for these class I-restricted alloreactive CTL is not the native class I molecule but peptides derived from endogenous processing of allogeneic class I products presented by class I molecules. Using a combination of limiting dilution and split-well analyses, we estimated for Kk-restricted Dq-specific alloreactive CTL a precursor frequency (CTLpf) that was approximately 10 times lower than the CTLpf for "classical" nonrestricted Dq-specific alloreactive CTL. These data suggest that H-2 class I peptides presented by intact H-2 class I molecules are allostimulatory, supporting the concept that the capacity for presentation of MHC peptides by MHC molecules constitutes a part of the allogeneic immune response.

摘要

最近,多条独立的证据有力地表明,源自一种外来主要组织相容性复合体(MHC)分子并与另一种MHC分子结合的肽能够产生多种复合MHC复合体,这些复合体能够刺激同种(异种)反应性T细胞。在本研究中,我们描述了用与受体在单个I类抗原上不匹配的细胞对小鼠进行体内免疫,会导致在刺激细胞上存在的其他I类分子(Ks、Kd、Kk)的背景下,诱导出针对同种异体I类基因座产物(Dd、Kd、Dq)的CD8+细胞毒性T淋巴细胞(CTL)。显然,这些I类限制性同种异体反应性CTL的靶抗原不是天然的I类分子,而是由I类分子呈递的同种异体I类产物内源性加工产生的肽。通过结合有限稀释和分孔分析,我们估计Kk限制性Dq特异性同种异体反应性CTL的前体频率(CTLpf)比“经典”非限制性Dq特异性同种异体反应性CTL的CTLpf低约10倍。这些数据表明,完整的H-2 I类分子呈递的H-2 I类肽具有同种异体刺激作用,支持了MHC分子呈递MHC肽的能力构成同种异体免疫反应一部分的概念。

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