首页> 外文期刊>The Journal of Experomental Medicine >Delayed maturation of CD4- CD8- Fc gamma RII/III+ T and natural killer cell precursors in Fc epsilon RI gamma transgenic mice.
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Delayed maturation of CD4- CD8- Fc gamma RII/III+ T and natural killer cell precursors in Fc epsilon RI gamma transgenic mice.

机译:CD4-CD8-FCγRII/ III + T和自然杀伤细胞前体的延迟成熟和FcεrIγ转基因小鼠的延迟成熟。

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摘要

Fc epsilon RI gamma (gamma) is a member of a group of related proteins (the zeta-family dimers) that function as signal-transducing components of both Fc receptors and the T cell antigen receptor (TCR). Analysis of gamma expression during fetal thymus ontogeny revealed that it is expressed in early thymocytes, before the initiation of clonotypic TCR-alpha and TCR-beta gene rearrangement but is down-regulated in most adult thymocytes. To explore a possible role for gamma in thymocyte development, we generated transgenic mice in which this protein was overexpressed at all stages of ontogeny. Overexpression of gamma inhibited the maturation of T cells as well as natural killer (NK) cells. The developmental effects were transgene dose related and correlated with markedly delayed maturation of fetal CD4-CD8- FcRII/III+ thymocytes, cells thought to include the progenitors of both T and NK cells. These results suggest that the zeta and gamma chains serve distinctive functions in thymocyte development and indicate that Fc receptor(s) may play an important role in regulating the differentiation of early progenitor cells within the thymus.
机译:FcεiLγ(γ)是一组相关蛋白质(Zeta类二聚体)的成员,其用作Fc受体和T细胞抗原受体(TCR)的信号转换组分。胎儿胸腺炎γ表达的分析表明,在最早的胸腺细胞中表达,在Clonotypic TCR-α和TCR-Beta基因重排开始之前在大多数成年胸腺细胞中下调。为了探讨γ在胸腺细节发育中的可能作用,我们产生的转基因小鼠,其中该蛋白在组来的所有阶段过表达。 γ的过度表达抑制了T细胞的成熟以及天然杀伤(NK)细胞的成熟。发育效果是转基因剂量相关和与胎儿CD4-CD8-FCRII / III +胸腺细胞的明显延迟成熟相关,细胞认为包括T和NK细胞的祖细胞。这些结果表明,Zeta和γ链在胸腺细节发育中提供了独特的功能,并表明Fc受体可能在调节胸腺内的早期祖细胞的分化方面发挥重要作用。

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