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首页> 外文期刊>The Journal of Experomental Medicine >Xenogeneic human anti-mouse T cell responses are due to the activity of the same functional T cell subsets responsible for allospecific and major histocompatibility complex-restricted responses.
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Xenogeneic human anti-mouse T cell responses are due to the activity of the same functional T cell subsets responsible for allospecific and major histocompatibility complex-restricted responses.

机译:异种人类抗小鼠T细胞反应是由于负责异源特异性和主要组织相容性复合物限制性反应的相同功能性T细胞亚群的活性所致。

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摘要

Human T cells respond strongly to mouse major histocompatibility complex (MHC) antigens. The response is directed predominantly to the polymorphic determinants of the MHC antigens and there is little or no response to the nonpolymorphic determinants or to non-MHC antigens. Human cytotoxic T lymphocytes (CTL) are generated specific for the mouse class I MHC antigens and the CTL effectors are blocked by anti-Leu-2a antisera. Human interleukin 2-producing T cells are generated specific for mouse class II antigens and their induction is blocked by anti-Leu-3a antisera. These and other considerations lead us to propose a model for the T cell receptor that provides an explanation for several of the features of T cell recognition. In this model, the recognition of the "class" (I or II) of MHC antigen is separate from the recognition of the polymorphic determinants. We suggest that the initial recognition of the conserved "class" determinants positions another domain of the receptor so that it can only engage with the part of the MHC molecule carrying the polymorphic determinants.
机译:人T细胞对小鼠主要组织相容性复合体(MHC)抗原产生强烈反应。该反应主要针对MHC抗原的多态决定簇,而对非多态决定簇或对非MHC抗原几乎没有响应。产生针对小鼠I类MHC抗原的人类细胞毒性T淋巴细胞(CTL),并且CTL效应子被抗Leu-2a抗血清阻断。产生产生人白介素2的T细胞对小鼠II类抗原具有特异性,并且其诱导被抗Leu-3a抗血清阻断。这些和其他考虑因素使我们提出了T细胞受体模型,该模型为T细胞识别的几个特征提供了解释。在该模型中,MHC抗原“ I”或“ II”类的识别与多态决定簇的识别是分开的。我们建议对保守的“类”决定簇的初始识别将定位受体的另一个结构域,以使其只能与携带多态决定簇的MHC分子的一部分结合。

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