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Notch与Wnt信号通路在造血干细胞维持中的整合

Integration of Notch and Wnt signaling in hematopoietic stem cell maintenance.

作者信息

Duncan Andrew W, Rattis Frédérique M, DiMascio Leah N, Congdon Kendra L, Pazianos Gregory, Zhao Chen, Yoon Keejung, Cook J Michael, Willert Karl, Gaiano Nicholas, Reya Tannishtha

机构信息

Department of Pharmacology and Cancer Biology, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

Nat Immunol. 2005 Mar;6(3):314-22. doi: 10.1038/ni1164. Epub 2005 Jan 23.

Abstract

A fundamental question in hematopoietic stem cell (HSC) biology is how self-renewal is controlled. Here we show that the molecular regulation of two critical elements of self-renewal, inhibition of differentiation and induction of proliferation, can be uncoupled, and we identify Notch signaling as a key factor in inhibiting differentiation. Using transgenic Notch reporter mice, we found that Notch signaling was active in HSCs in vivo and downregulated as HSCs differentiated. Inhibition of Notch signaling led to accelerated differentiation of HSCs in vitro and depletion of HSCs in vivo. Finally, intact Notch signaling was required for Wnt-mediated maintenance of undifferentiated HSCs but not for survival or entry into the cell cycle in vitro. These data suggest that Notch signaling has a dominant function in inhibiting differentiation and provide a model for how HSCs may integrate multiple signals to maintain the stem cell state.

摘要

造血干细胞(HSC)生物学中的一个基本问题是自我更新如何受到调控。在此我们表明,自我更新的两个关键要素(抑制分化和诱导增殖)的分子调控可以被分开,并且我们确定Notch信号是抑制分化的关键因素。利用转基因Notch报告基因小鼠,我们发现Notch信号在体内的造血干细胞中是活跃的,并且随着造血干细胞的分化而被下调。抑制Notch信号会导致造血干细胞在体外加速分化以及在体内耗竭。最后,完整的Notch信号是Wnt介导的未分化造血干细胞维持所必需的,但不是体外存活或进入细胞周期所必需的。这些数据表明Notch信号在抑制分化中具有主导作用,并为造血干细胞如何整合多种信号以维持干细胞状态提供了一个模型。

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