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单细胞衍生免疫能力的连续传递揭示了 CD8(+)中央记忆 T 细胞的干细胞特性。

Serial transfer of single-cell-derived immunocompetence reveals stemness of CD8(+) central memory T cells.

机构信息

Institute for Medical Microbiology, Immunology and Hygiene, Technische Universität München (TUM), Munich 81675, Germany.

Institute for Medical Microbiology, Immunology and Hygiene, Technische Universität München (TUM), Munich 81675, Germany; Focus Group "Clinical Cell Processing and Purification," Institute for Advanced Study, TUM, Munich 81675, Germany.

出版信息

Immunity. 2014 Jul 17;41(1):116-26. doi: 10.1016/j.immuni.2014.05.018.

Abstract

Maintenance of immunological memory has been proposed to rely on stem-cell-like lymphocytes. However, data supporting this hypothesis are focused on the developmental potential of lymphocyte populations and are thus insufficient to establish the functional hallmarks of stemness. Here, we investigated self-renewal capacity and multipotency of individual memory lymphocytes by in vivo fate mapping of CD8(+) T cells and their descendants across three generations of serial single-cell adoptive transfer and infection-driven re-expansion. We found that immune responses derived from single naive T (Tn) cells, single primary, and single secondary central memory T (Tcm) cells reached similar size and phenotypic diversity, were subjected to comparable stochastic variation, and could ultimately reconstitute immunocompetence against an otherwise lethal infection with the bacterial pathogen Listeria monocytogenes. These observations establish that adult tissue stem cells reside within the CD62L(+) Tcm cell compartment and highlight the promising therapeutic potential of this immune cell subset.

摘要

免疫记忆的维持被认为依赖于干细胞样淋巴细胞。然而,支持这一假设的数据集中在淋巴细胞群体的发育潜力上,因此不足以确定干细胞特性的功能特征。在这里,我们通过 CD8(+)T 细胞及其后代在三代连续单细胞过继转移和感染驱动的再扩增中的体内命运图谱,研究了单个记忆淋巴细胞的自我更新能力和多能性。我们发现,来自单个幼稚 T(Tn)细胞、单个初级和单个次级中央记忆 T(Tcm)细胞的免疫反应达到了相似的大小和表型多样性,受到可比较的随机变化的影响,并且最终可以重建对李斯特菌属细菌病原体李斯特菌单核细胞增生症的致命感染的免疫能力。这些观察结果确立了成年组织干细胞存在于 CD62L(+)Tcm 细胞区室中,并强调了这种免疫细胞亚群有希望的治疗潜力。

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