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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Cutting Edge: a thymocyte-thymic epithelial cell cross-talk dynamically regulates intrathymic IL-7 expression in vivo.
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Cutting Edge: a thymocyte-thymic epithelial cell cross-talk dynamically regulates intrathymic IL-7 expression in vivo.

机译:前沿:胸腺细胞-胸腺上皮细胞的串扰在体内动态调节胸腺内IL-7的表达。

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摘要

Thymic epithelial cells (TECs) are the predominant intrathymic source of the essential thymopoietin IL-7. Whether thymocyte-TEC interactions have a role in the regulation of IL-7 expression is not known. By exploiting IL-7 reporter mice in which yellow fluorescent protein expression identifies TECs expressing high levels of IL-7 (Il7(+) TECs), we show that Il7(+) TECs segregate from emerging medullary TECs during thymic organogenesis. Although Il7(+) TECs normally diminish with age, we found that Il7(+) TECs are markedly retained in alymphoid Rag2(-/-)Il2rg(-/-) IL-7 reporter mice that manifest a profound thymopoietic arrest. Transfer of Tcra(-/-) or wild-type (but not Rag2(-/-)) hematopoietic progenitors to alymphoid IL-7 reporter recipients normalizes the frequency of Il7(+) TECs and re-establishes cortical TEC/medullary TEC segregation. Although thymocyte-derived signals are often considered stimulatory for TEC maturation, our findings identify a negative feedback mechanism in which signals derived from TCRbeta-selected thymocytes modulate TEC-dependent IL-7 expression.
机译:胸腺上皮细胞(TECs)是必需胸腺生成素IL-7的主要胸腺内来源。胸腺细胞-TEC相互作用是否在IL-7表达的调节中起作用尚不清楚。通过利用其中黄色荧光蛋白表达可识别表达高水平IL-7的TEC(IL17(+)TECs)的IL-7报告基因小鼠,我们显示,Il7(+)TECs在胸腺器官发生过程中与新兴的髓质TEC分离。虽然Il7(+)TECs通常会随着年龄的增长而减少,但我们发现Il7(+)TECs明显保留在Alymphoid Rag2(-/-)Il2rg(-/-)IL-7报告基因小鼠中,表现出深深的胸腺细胞性逮捕。 Tcra(-/-)或野生型(但不是Rag2(-/-))造血祖细胞转移至Amphmphoid IL-7报告受体,可正常化Il7(+)TECs的频率并重新建立皮质TEC /髓质TEC隔离。尽管胸腺细胞衍生的信号通常被认为是TEC成熟的刺激因素,但我们的发现确定了一种负反馈机制,其中从TCRbeta选择的胸腺细胞衍生的信号调节TEC依赖性IL-7表达。

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