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组织干细胞动态中的Runx家族基因

Runx Family Genes in Tissue Stem Cell Dynamics.

作者信息

Wang Chelsia Qiuxia, Mok Michelle Meng Huang, Yokomizo Tomomasa, Tergaonkar Vinay, Osato Motomi

机构信息

Cancer Science Institute of Singapore, National University of Singapore, Singapore, Singapore.

Institute of Molecular and Cell Biology, A*STAR, Singapore, Singapore.

出版信息

Adv Exp Med Biol. 2017;962:117-138. doi: 10.1007/978-981-10-3233-2_9.

Abstract

The Runx family genes play important roles in development and cancer, largely via their regulation of tissue stem cell behavior. Their involvement in two organs, blood and skin, is well documented. This review summarizes currently known Runx functions in the stem cells of these tissues. The fundamental core mechanism(s) mediated by Runx proteins has been sought; however, it appears that there does not exist one single common machinery that governs both tissue stem cells. Instead, Runx family genes employ multiple spatiotemporal mechanisms in regulating individual tissue stem cell populations. Such specific Runx requirements have been unveiled by a series of cell type-, developmental stage- or age-specific gene targeting studies in mice. Observations from these experiments revealed that the regulation of stem cells by Runx family genes turned out to be far more complex than previously thought. For instance, although it has been reported that Runx1 is required for the endothelial-to-hematopoietic cell transition (EHT) but not thereafter, recent studies clearly demonstrated that Runx1 is also needed during the period subsequent to EHT, namely at perinatal stage. In addition, Runx1 ablation in the embryonic skin mesenchyme eventually leads to complete loss of hair follicle stem cells (HFSCs) in the adult epithelium, suggesting that Runx1 facilitates the specification of skin epithelial stem cells in a cell extrinsic manner. Further in-depth investigation into how Runx family genes are involved in stem cell regulation is warranted.

摘要

Runx家族基因在发育和癌症中发挥着重要作用,主要是通过对组织干细胞行为的调控来实现。它们在血液和皮肤这两个器官中的作用已有充分记载。本综述总结了目前已知的Runx在这些组织干细胞中的功能。人们一直在探寻由Runx蛋白介导的基本核心机制;然而,似乎并不存在一种单一的共同机制来调控这两种组织干细胞。相反,Runx家族基因在调节各个组织干细胞群体时采用了多种时空机制。通过一系列针对小鼠的细胞类型、发育阶段或年龄特异性基因敲除研究,已经揭示了Runx的这些特定需求。这些实验的观察结果表明,Runx家族基因对干细胞的调控远比之前认为的要复杂得多。例如,虽然已有报道称Runx1是内皮细胞向造血细胞转变(EHT)所必需的,但在此之后并非如此,然而最近的研究清楚地表明,Runx1在EHT之后的时期,即在围产期也同样需要。此外,胚胎皮肤间充质中Runx1的缺失最终会导致成年上皮中毛囊干细胞(HFSC)完全丧失,这表明Runx1以细胞外的方式促进皮肤上皮干细胞的特化。有必要对Runx家族基因如何参与干细胞调控进行进一步深入研究。

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