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首页> 外文期刊>The journal of immunology >Cutting Edge: CXCR4 Is Critical for CD8+ Memory T Cell Homeostatic Self-Renewal but Not Rechallenge Self-Renewal
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Cutting Edge: CXCR4 Is Critical for CD8+ Memory T Cell Homeostatic Self-Renewal but Not Rechallenge Self-Renewal

机译:前沿:CXCR4对于CD8 +记忆T细胞稳态自我更新至关重要,但对挑战自我更新而言却不重要

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Central memory (CM) CD8+ T cells “remember” prior encounters because they maintain themselves through cell division in the absence of ongoing challenge (homeostatic self-renewal), as well as reproduce the CM fate while manufacturing effector cells during secondary Ag encounters (rechallenge self-renewal). We tested the consequence of conditional deletion of the bone marrow homing receptor CXCR4 on antiviral T cell responses. CXCR4-deficient CD8+ T cells have impaired memory cell maintenance due to defective homeostatic proliferation. Upon rechallenge, however, CXCR4-deficient T cells can re-expand and renew the CM pool while producing secondary effector cells. The critical bone marrow–derived signals essential for CD8+ T cell homeostatic self-renewal appear to be dispensable to yield self-renewing, functionally asymmetric cell fates during rechallenge.
机译:中央记忆(CM)CD8 + T细胞可以“记住”先前的遭遇,因为它们在不存在持续挑战(稳态自我更新)的情况下通过细胞分裂来维持自身状态,并在二次Ag遭遇期间制造效应细胞时重现CM命运(挑战自我更新)。我们测试了在抗病毒T细胞反应中条件性删除骨髓归巢受体CXCR4的后果。缺乏CXCR4的CD8 + T细胞由于体内稳态增殖缺陷而损害了存储单元的维护。然而,一旦受到挑战,缺乏CXCR4的T细胞可以重新扩增和更新CM库,同时产生次级效应细胞。 CD8 + T细胞体内自我更新所必需的关键性骨髓来源信号似乎在再挑战过程中可产生自我更新,功能不对称的细胞命运。

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