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Differential requirement of the cytoplasmic subregions of γc chain in T cell development and function

机译:γc链胞质亚区对T细胞发育和功能的差异性要求

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摘要

The common cytokine receptor γ chain (γc), a shared component of the receptors for IL-2, IL-4, IL-7, IL-9, and IL-15, is critical for the development and function of lymphocytes. The cytoplasmic domain of γc consists of 85 aa, in which the carboxyl-terminal 48 aa are essential for its interaction with and activation of the Janus kinase, Jak3. Evidence has been provided that Jak3-independent signals might be transmitted via the residual membrane-proximal region; however, its role in vivo remains totally unknown. In the present study, we expressed mutant forms of γc, which lack either most of the cytoplasmic domain or only the membrane-distal Jak3-binding region, on a γc null background. We demonstrate that, unlike γc or Jak3 null mice, expression of the latter, but not the former mutant, restores T lymphopoiesis in vivo, accompanied by strong expression of Bcl-2. On the other hand, the in vitro functions of the restored T cells still remained impaired. These results not only reveal the hitherto unknown role of the γc membrane-proximal region, but also suggest the differential requirement of the cytoplasmic subregions of γc in T cell development and function.
机译:共同的细胞因子受体γ链(γc)是IL-2,IL-4,IL-7,IL-9和IL-15受体的共享成分,对淋巴细胞的发育和功能至关重要。 γc的胞质域由85个氨基酸组成,其中羧基末端48个氨基酸对于其与Janus激酶Jak3的相互作用和激活至关重要。有证据表明,与Jak3无关的信号可能会通过残留的膜近端区域传播。然而,其在体内的作用仍然完全未知。在本研究中,我们在γc无效背景上表达了γc的突变体形式,该突变体要么缺少大部分的胞质域,要么仅缺少膜远端Jak3结合区。我们证明,与γc或Jak3 null小鼠不同,后者的表达但不是前者突变体在体内恢复T淋巴细胞生成,并伴有Bcl-2的强表达。另一方面,恢复的T细胞的体外功能仍然受损。这些结果不仅揭示了迄今未知的γc膜近端区域的作用,而且还暗示了γc的胞质亚区在T细胞发育和功能上的不同需求。

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