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一条划分胸腺细胞发育过程中两波克隆清除和Foxp3上调的时间线。

A timeline demarcating two waves of clonal deletion and Foxp3 upregulation during thymocyte development.

作者信息

Hu Daniel Y, Yap Jin Y, Wirasinha Rushika C, Howard Debbie R, Goodnow Christopher C, Daley Stephen R

机构信息

Immunology Department, The John Curtin School of Medical Research, The Australian National University, Canberra, Australian Capital Territory, Australia.

出版信息

Immunol Cell Biol. 2016 Apr;94(4):357-66. doi: 10.1038/icb.2015.95. Epub 2015 Oct 29.

Abstract

Thymocytes that bind strongly to self-antigens are prevented from becoming naive T cells by several mechanisms. They undergo clonal deletion at two stages of development; wave 1 in immature thymocytes lacking the medulla-homing chemokine receptor, CCR7, or wave 2 in more mature CCR7(+) thymocytes. Alternatively, self-reactive thymocytes upregulate Foxp3 to become T-regulatory cells. Here, we describe the differential timing of the two waves of deletion and Foxp3 upregulation relative to the immature proliferating stage. Proliferating thymocytes were pulse-labeled in normal C57BL/6 mice with 5-ethynyl-2'-deoxyuridine (EdU). Thymocytes progressed into wave 1 (CCR7(-)) and wave 2 (CCR7(+)) of clonal deletion ~2 and 5 days after proliferation, respectively. Foxp3 upregulation occurred between 4 and 8 days after proliferation, predominantly in thymocytes with a Helios(+) CCR7(+) phenotype. These findings establish a timeline that suggests that wave 1 of clonal deletion occurs in the thymic cortex, whereas wave 2 and Foxp3 upregulation both occur in the thymic medulla.

摘要

通过几种机制,与自身抗原强烈结合的胸腺细胞无法发育成为初始T细胞。它们在两个发育阶段经历克隆清除:一是在缺乏髓质归巢趋化因子受体CCR7的未成熟胸腺细胞中的第1波,二是在更成熟的CCR7(+)胸腺细胞中的第2波。另外,自身反应性胸腺细胞会上调Foxp3以成为调节性T细胞。在此,我们描述了相对于未成熟增殖阶段,两波克隆清除和Foxp3上调的不同时间。在正常C57BL/6小鼠中,用5-乙炔基-2'-脱氧尿苷(EdU)对增殖的胸腺细胞进行脉冲标记。增殖后约2天和5天,胸腺细胞分别进入克隆清除的第1波(CCR7(-))和第2波(CCR7(+))。Foxp3上调发生在增殖后4至8天,主要发生在具有Helios(+) CCR7(+)表型的胸腺细胞中。这些发现建立了一个时间轴,表明克隆清除的第1波发生在胸腺皮质,而第2波和Foxp3上调都发生在胸腺髓质。

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