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Ligand-Specific Selection of MHC Class II-Restricted Thymocytes in Fetal Thymic Organ Culture

机译:胎儿胸腺器官培养物中MHC II类限制性胸腺细胞的配体特异性选择

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Positive and negative selection of thymocytes is determined by the specificity of the TCR and signaling through its associated molecules. We have studied selection of thymocytes bearing a MHC class II-restricted TCR using fetal thymic organ culture. This system allows the addition of peptides to the already diverse panoply of endogenous peptide ligands and is useful for analyzing ligand-specific negative selection of CD4 single positive (CD4SP) thymocytes. The data reveal that the ability of a given ligand to mediate negative selection is related to its dissociation rate from the TCR. We find that negative selection is very sensitive, and only the weakest ligand that we can identify fails to induce negative selection. None of the numerous peptides tested were able to induce an increase in CD4SP thymocytes. In addition, the ligands that induce negative selection of CD4SP thymocytes also cause an increase in numbers of CD8SP thymocytes bearing high levels of the class II-restricted TCR. Although these cells have a cell surface phenotype consistent with positive selection, they most likely represent cells in the process of negative selection. Further analysis reveals that these cells are not induced by these ligands in intact adult animals and that their induction is probably only revealed in the organ culture system.
机译:胸腺细胞的阳性和阴性选择取决于TCR的特异性和通过其相关分子发出的信号。我们已经研究了使用胎儿胸腺器官培养物选择携带MHC II类限制性TCR的胸腺细胞。该系统允许将肽添加到已经多样化的内源肽配体中,并且可用于分析CD4单阳性(CD4SP)胸腺细胞的配体特异性阴性选择。数据表明给定配体介导负选择的能力与其从TCR的解离速率有关。我们发现负选择非常敏感,只有我们能识别的最弱的配体不能诱导负选择。测试的众多肽中没有一个能够诱导CD4SP胸腺细胞增加。另外,诱导CD4SP胸腺细胞阴性选择的配体也引起携带高水平的II类限制性TCR的CD8SP胸腺细胞的数量增加。尽管这些细胞具有与阳性选择一致的细胞表面表型,但它们最有可能代表阴性选择过程中的细胞。进一步的分析表明,这些细胞在完整的成年动物中并未被这些配体诱导,并且它们的诱导可能仅在器官培养系统中被揭示。

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