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胸腺细胞和成熟 T 细胞增殖对差异 geminin 的需求。

Differential geminin requirement for proliferation of thymocytes and mature T cells.

机构信息

Department of Pharmacology, Medical Research Council/National Institute for Medical Research, The Ridgeway, London NW7 1AA, United Kingdom.

出版信息

J Immunol. 2010 Mar 1;184(5):2432-41. doi: 10.4049/jimmunol.0901983. Epub 2010 Jan 27.

DOI:10.4049/jimmunol.0901983
PMID:20107189
Abstract

Stem/progenitor cells coordinate proliferation and differentiation, giving rise to appropriate cell numbers of functionally specialized cells during organogenesis. In different experimental systems, Geminin was shown to maintain progenitor cells and participate in fate determination decisions and organogenesis. Although the exact mechanisms are unclear, Geminin has been postulated to influence proliferation versus differentiation decisions. To gain insight into the in vivo role of Geminin in progenitor cell division and differentiation, we have generated mice that specifically lack Geminin in cells of lymphoid lineage through Cre-mediated recombination. T cells lacking Geminin expression upregulate early activation markers efficiently upon TCR stimulation in vitro and are able to enter the S phase of cell cycle, but show a marked defect in completing the cycle, leading to a large proportion of T cells accumulating in S/G2/M phases. Accordingly, T cells deficient in Geminin show a reduced ability to repopulate lymphopenic hosts in vivo. Contrary to expectations, Geminin deficiency does not alter development and differentiation of T cells in vivo. Our data suggest that Geminin is required for the proliferation events taking place either in vitro upon TCR receptor activation or during homeostatic expansion, but appears to be redundant for the proliferation and differentiation of the majority of progenitor T cell populations.

摘要

干细胞/祖细胞协调增殖和分化,在器官发生过程中产生适当数量的功能特化细胞。在不同的实验系统中,Geminin 被证明可以维持祖细胞,并参与命运决定决策和器官发生。尽管确切的机制尚不清楚,但有人推测 Geminin 会影响增殖与分化决策。为了深入了解 Geminin 在祖细胞分裂和分化中的体内作用,我们通过 Cre 介导的重组生成了专门在淋巴细胞系细胞中缺乏 Geminin 的小鼠。缺乏 Geminin 表达的 T 细胞在体外 TCR 刺激下能够有效地上调早期激活标志物,并能够进入细胞周期的 S 期,但在完成周期方面存在明显缺陷,导致大量 T 细胞积累在 S/G2/M 期。因此,缺乏 Geminin 的 T 细胞在体内重新定植淋巴减少宿主的能力降低。与预期相反,Geminin 缺乏并不改变体内 T 细胞的发育和分化。我们的数据表明,Geminin 是 T 细胞受体激活后体外发生的增殖事件或在体内稳态扩张期间所必需的,但对于大多数祖 T 细胞群体的增殖和分化似乎是冗余的。

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Differential geminin requirement for proliferation of thymocytes and mature T cells.胸腺细胞和成熟 T 细胞增殖对差异 geminin 的需求。
J Immunol. 2010 Mar 1;184(5):2432-41. doi: 10.4049/jimmunol.0901983. Epub 2010 Jan 27.
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E2F1 and E2F2 are differentially required for homeostasis-driven and antigen-induced T cell proliferation in vivo.在体内,稳态驱动的和抗原诱导的T细胞增殖对E2F1和E2F2的需求存在差异。
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FoxM1, a forkhead transcription factor is a master cell cycle regulator for mouse mature T cells but not double positive thymocytes.FoxM1 是一个叉头转录因子,是调控成熟 T 细胞细胞周期的主控因子,但不是双阳性胸腺细胞的主控因子。
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J Immunol. 2006 Apr 1;176(7):4029-41. doi: 10.4049/jimmunol.176.7.4029.

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