I类和II类MHC基因产物对携带V β 5胸腺细胞的命运影响不同。

J Bill, O Kanagawa, J Linten, Y Utsunomiya, E Palmer
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引用次数: 0

摘要

我们之前的研究表明,携带V β 5+ T细胞受体(TCRs)的T细胞在B10 (H-2b)和B10中很常见。Q (H-2q)小鼠菌株,但在基因菌株B10中罕见。BR (H-2k)。此外,我们发现携带V β 5的T细胞似乎被排除在B10对I-Abm12的同种异体反应之外,尽管大多数其他携带V β的细胞都参与其中。为了进一步研究MHC对V β 5表达的影响,我们生成了两种V β 5特异性单克隆抗体,并在这里显示,表达V β 5的T细胞从表达II类,I-E分子的菌株中被克隆删除。此外,尽管在CD8+亚群中有大量的V β 5+ T细胞,但I-E-菌株产生的CD4+ V β 5+ T细胞很少。因此,携带V β 5的T细胞被I类MHC分子积极选择,被II类I- e分子克隆删除,被II类I- a分子不佳选择。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Class I and class II MHC gene products differentially affect the fate of V beta 5 bearing thymocytes.

We have previously shown that T cells bearing V beta 5+ T-cell receptors (TCRs) are frequent in B10 (H-2b) and B10.Q (H-2q) mouse strains but are rare in the congenic strain B10.BR (H-2k). Furthermore, we have found that V beta 5 bearing T cells appear to be excluded from the B10 alloresponse to I-Abm12 despite the participation of most other V beta bearing cells. To further study MHC effects on V beta 5 expression, we have generated two V beta 5 specific monoclonal antibodies and show here that V beta 5 expressing T cells are clonally deleted from strains expressing a class II, I-E molecule. Furthermore, I-E- strains generate few CD4+ V beta 5+ T cells despite significant numbers of V beta 5+ T cells in the CD8+ subset. Thus, V beta 5 bearing T cells are positively selected by class I MHC molecules, clonally deleted by class II I-E molecules, and poorly selected by class II I-A molecules.

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