Kinjyo Ichiko, Qin Jim, Tan Sioh-Yang, Wellard Cameron J, Mrass Paulus, Ritchie William, Doi Atsushi, Cavanagh Lois L, Tomura Michio, Sakaue-Sawano Asako, Kanagawa Osami, Miyawaki Atsushi, Hodgkin Philip D, Weninger Wolfgang
Immune Imaging Program, Centenary Institute for Cancer Medicine and Cell Biology, Newtown, New South Wales 2042, Australia.
1] Division of Immunology, Walter and Eliza Hall Institute of Medical Research, Parkville, Victoria 3052, Australia [2] Department of Medical Biology, University of Melbourne, Melbourne, Victoria 3052, Australia.
Nat Commun. 2015 Feb 24;6:6301. doi: 10.1038/ncomms7301.
The precise pathways of memory T-cell differentiation are incompletely understood. Here we exploit transgenic mice expressing fluorescent cell cycle indicators to longitudinally track the division dynamics of individual CD8(+) T cells. During influenza virus infection in vivo, naive T cells enter a CD62L(intermediate) state of fast proliferation, which continues for at least nine generations. At the peak of the anti-viral immune response, a subpopulation of these cells markedly reduces their cycling speed and acquires a CD62L(hi) central memory cell phenotype. Construction of T-cell family division trees in vitro reveals two patterns of proliferation dynamics. While cells initially divide rapidly with moderate stochastic variations of cycling times after each generation, a slow-cycling subpopulation displaying a CD62L(hi) memory phenotype appears after eight divisions. Phenotype and cell cycle duration are inherited by the progeny of slow cyclers. We propose that memory precursors cell-intrinsically modulate their proliferative activity to diversify differentiation pathways.
记忆性T细胞分化的确切途径尚未完全明确。在此,我们利用表达荧光细胞周期指示剂的转基因小鼠来纵向追踪单个CD8(+) T细胞的分裂动态。在体内感染流感病毒期间,初始T细胞进入快速增殖的CD62L(中间)状态,这种状态持续至少九代。在抗病毒免疫反应的高峰期,这些细胞的一个亚群显著降低其循环速度,并获得CD62L(高)中央记忆细胞表型。体外构建T细胞家族分裂树揭示了两种增殖动态模式。虽然细胞最初快速分裂,每一代后的循环时间有适度的随机变化,但在八次分裂后出现了显示CD62L(高)记忆表型的慢循环亚群。慢循环细胞的后代继承了表型和细胞周期持续时间。我们提出,记忆前体细胞内在地调节其增殖活性以使分化途径多样化。
Zotero 插件
