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Cutting Edge: Limiting Amounts of IL-7 Do Not Control Contraction of CD4+ T Cell Responses

机译:前沿:IL-7的限量不能控制CD4 + T细胞反应的收缩

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摘要

During the acute T cell response most effector T cells die while some survive and become memory T cells. Selective expression of CD127 (IL-7Rα) on effector T cells has been proposed to engender their survival into the memory pool. We assessed the role of IL-7 in effector T cell survival using MHC class II tetramers to track a CD4+ T cell response following infection with a recombinant vaccinia virus (rVV-2W1S). Exogenous IL-7 prevented the contraction of the 2W1S-specific CD4+ T cell response after rVV-2W1S infection. IL-7 increased proliferation of, and Bcl-2 expression within, 2W1S-specific T cells; the latter was required for IL-7-driven prevention of contraction. Conversely, in vivo neutralization of IL-7 or Bcl-2 did not exacerbate the contraction of 2W1S-specific CD4+ T cells. These data suggest that IL-7 administration may enhance the survival of effector T cells but that IL-7 is not the limiting factor during normal contraction of the response.
机译:在急性T细胞反应过程中,大多数效应T细胞死亡,而有些存活并变成记忆T细胞。已经提出在效应T细胞上选择性表达CD127(IL-7Rα)以使其存活进入记忆库。我们使用II类MHC四聚体追踪重组痘苗病毒(rVV-2W1S)感染后CD4 + T细胞应答,评估IL-7在效应T细胞存活中的作用。外源IL-7阻止rVV-2W1S感染后2W1S特异性CD4 + T细胞反应的收缩。 IL-7增加2W1S特异性T细胞的增殖和Bcl-2表达。后者是IL-7驱动的预防收缩所必需的。相反,体内中和IL-7或Bcl-2并不会加剧2W1S特异性CD4 + T细胞的收缩。这些数据表明,IL-7的给药可以提高效应T细胞的存活率,但IL-7并不是正常收缩反应的限制因素。

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