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转基因小鼠中携带CD8的T淋巴细胞上抗原受体的选择性表达。

Selective expression of an antigen receptor on CD8-bearing T lymphocytes in transgenic mice.

作者信息

Sha W C, Nelson C A, Newberry R D, Kranz D M, Russell J H, Loh D Y

机构信息

Department of Medicine, Howard Hughes Medical Institute, Washington University School of Medicine, St Louis, Missouri 63110.

出版信息

Nature. 1988 Sep 15;335(6187):271-4. doi: 10.1038/335271a0.

Abstract

The major problem in the study of T-cell development is that of tracking thymocytes of a given specificity. Recent studies have exploited natural correlations between the expression of a particular V beta gene segment and T-cell receptor (TCR) specificity. We and others (refs 5, 6 and M. Davis, personal communication) have taken an alternative approach. We have generated transgenic mice expressing the alpha beta antigen receptor from the cytotoxic T-lymphocyte clone 2C (ref. 7). In transgenic mice of the same haplotype as the 2C clone, the 2C TCR was expressed on 20-95% of peripheral T cells. Very few of these T cells carried the CD4 antigen; the vast majority were CD4-CD8+ and were able to lyse targets with the same specificity as the original 2C clone. These results indicate that the alpha beta heterodimer transfers specificity to recipient cells as expected from earlier studies, and that receptor specificity in T-cell repertoire selection is determined by both alpha beta heterodimer and CD4 or CD8 accessory molecules.

摘要

T细胞发育研究中的主要问题是追踪具有特定特异性的胸腺细胞。最近的研究利用了特定Vβ基因片段的表达与T细胞受体(TCR)特异性之间的天然关联。我们和其他人(参考文献5、6以及M. 戴维斯的个人交流)采用了另一种方法。我们构建了表达来自细胞毒性T淋巴细胞克隆2C的αβ抗原受体的转基因小鼠(参考文献7)。在与2C克隆相同单倍型的转基因小鼠中,2C TCR在20%至95%的外周T细胞上表达。这些T细胞中很少携带CD4抗原;绝大多数是CD4-CD8+,并且能够以与原始2C克隆相同的特异性裂解靶细胞。这些结果表明,αβ异二聚体如早期研究所预期的那样将特异性传递给受体细胞,并且T细胞库选择中的受体特异性由αβ异二聚体和CD4或CD8辅助分子共同决定。

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