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小鼠胚胎干细胞自我更新中的转化生长因子-β超家族。

Transforming growth factor-beta superfamily in mouse embryonic stem cell self-renewal.

机构信息

Department of Pathology and Laboratory Medicine, Institute for Reproductive Health and Regenerative Medicine, University of Kansas Medical Center, Kansas City, USA.

出版信息

Vitam Horm. 2011;87:341-65. doi: 10.1016/B978-0-12-386015-6.00035-4.

Abstract

Embryonic stem (ES) cells are pluripotent cells that maintain the capability of undifferentiated self-renewal in culture. As mouse ES cells have the capacity to give rise to all the tissues of the body, they are an excellent developmental biology model system and a model for regenerative therapies. The extracellular cues and the intracellular signaling cascades that regulate ES cell self-renewal and cell-fate choices are complex and actively studied. Many developmental signaling pathways regulate the ES cell phenotype, and their intracellular programs interact to modulate the gene networks controlling ES cell pluripotency. This review focuses on the current understanding and outstanding questions of the roles of the transforming growth factor-beta-related signaling pathways in regulating pluripotency and differentiation of mouse ES cells. The complex dichotomic roles of bone morphogenetic protein signaling in maintaining the undifferentiated state and also inducing specific cell fates will be reviewed. The emerging roles of Nodal signaling in ES cell self-renewal will also be discussed.

摘要

胚胎干细胞(ES 细胞)是具有多能性的细胞,能够在培养中保持未分化的自我更新能力。由于小鼠 ES 细胞具有产生身体所有组织的能力,因此它们是优秀的发育生物学模型系统和再生治疗模型。调节 ES 细胞自我更新和细胞命运选择的细胞外线索和细胞内信号级联非常复杂,目前正在积极研究。许多发育信号通路调节 ES 细胞表型,其细胞内程序相互作用,调节控制 ES 细胞多能性的基因网络。本综述重点介绍转化生长因子-β相关信号通路在调节小鼠 ES 细胞多能性和分化中的作用的最新认识和悬而未决的问题。还将回顾骨形态发生蛋白信号在维持未分化状态和诱导特定细胞命运方面的复杂二分作用。还将讨论 Nodal 信号在 ES 细胞自我更新中的新兴作用。

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