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HLA转基因小鼠中病毒抗原的HLA限制识别。

HLA-restricted recognition of viral antigens in HLA transgenic mice.

作者信息

Kievits F, Ivanyi P, Krimpenfort P, Berns A, Ploegh H L

机构信息

Central Laboratory of the Netherlands Red Cross Blood Transfusion Service, Department of Immunochematology, University of Amsterdam, The Netherlands.

出版信息

Nature. 1987;329(6138):447-9. doi: 10.1038/329447a0.

Abstract

Cytotoxic T lymphocytes (CTL) recognize antigen in the context of the class-I products of the major histocompatibility complex (MHC). The extensive polymorphism of class-I molecules is thought to be linked to their capacity to present a large variety of foreign antigens. Whether a single T-cell receptor (TCR) recognizes two separate epitopes (the foreign antigen and an epitope on MHC molecules), or a single epitope resulting from the combination of a foreign antigen and an MHC molecule, has not yet been resolved. In view of the differences between species in primary structure of histocompatibility antigens, it might be predicted that the TCR repertoire would evolve in concert with the diversity of MHC antigens. The mouse and human TCR repertoire would be optimally adapted to engage in productive interactions only with mouse (H-2) and human (HLA) MHC antigens respectively, especially if the more conserved features of histocompatibility antigens, in addition to foreign antigen, were seen by the TCR. Alternatively, only the most variable segments of MHC antigens might be engaged in antigen presentation and thus in interaction with the TCR. In that case, interaction between MHC plus antigen and the TCR might not necessarily be limited by species-specific features. By analysis of the T-cell response against virus-infected cells in HLA-B27/human beta 2-microglobulin double transgenic mice, we report here that the mouse T-cell repertoire is perfectly capable of using the human HLA-B27 antigen as a restriction element.

摘要

细胞毒性T淋巴细胞(CTL)在主要组织相容性复合体(MHC)的I类产物背景下识别抗原。I类分子的广泛多态性被认为与其呈递多种外来抗原的能力有关。单个T细胞受体(TCR)是识别两个独立的表位(外来抗原和MHC分子上的一个表位),还是识别由外来抗原和MHC分子组合产生的单个表位,目前尚未得到解决。鉴于组织相容性抗原一级结构在物种间存在差异,可以预测TCR库将与MHC抗原的多样性协同进化。小鼠和人类的TCR库可能分别仅与小鼠(H-2)和人类(HLA)MHC抗原进行最佳适配以进行有效的相互作用,特别是如果TCR除了能识别外来抗原外,还能识别组织相容性抗原中更保守的特征。或者,只有MHC抗原中最可变的片段可能参与抗原呈递,从而与TCR相互作用。在这种情况下,MHC加抗原与TCR之间的相互作用不一定受物种特异性特征的限制。通过分析HLA-B27/人β2-微球蛋白双转基因小鼠对病毒感染细胞的T细胞反应,我们在此报告,小鼠的T细胞库完全能够将人类HLA-B27抗原用作限制元件。

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