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Twists in views on RB functions in cellular signaling metabolism and stem cells

机译:在蜂窝信号新陈代谢和干细胞的RB功能的视图中曲折

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摘要

One‐quarter of a century ago, identification of the human retinoblastoma gene (RB) loci proved Knudson's ‘two‐hit theory’ that tumor suppressor genes exist. Since then, numerous works delineated crucial roles for the RB protein (pRB)‐E2F transcription factor complex in G1‐S phase transition. In addition, discovering the relationship between pRB and tissue‐specific transcription factors enabled a better understanding of how cell cycle exit and terminal differentiation are coupled. Recent works provoked many exciting twists in views on pRB functions during cancer initiation and progression beyond its previously well‐appreciated roles. Various mitogenic and cytostatic cellular signals appeared to modulate pRB functions and thus affect a wide variety of effector molecules. In addition, genetic studies in mice as well as other creatures incessantly force us to revise our views on pRB functions. This review will focus particularly on the roles of pRB in regulating intracellular signaling, cell metabolism, chromatin function, stem cells and cancer stem cells. (Cancer Sci 2012; 103: 1182–1188)
机译:四分之一世纪以前,鉴定人视网膜母细胞瘤基因(RB)基因座,证明了Knudson的“双击理论”存在肿瘤抑制基因。从那时起,众多作品划定了G1-S期转变中的RB蛋白(PRB)-E2F转录因子复合物的关键作用。此外,发现PRB和组织特异性转录因子之间的关系使得能够更好地理解细胞周期出口和终端分化如何耦合。最近的作品激发了许多令人兴奋的曲折在癌症启动期间对PRB功能的看法,超出其先前受到欣赏的角色。各种丝肠和细胞抑制性细胞信号似乎调节PRB功能,从而影响各种效应分子。此外,小鼠的遗传学研究以及其他生物不断强迫我们对PRB职能进行修改。本综述特别是对PRB在调节细胞内信号,细胞代谢,染色质功能,干细胞和癌症干细胞中的作用。 (癌症SCI 2012; 103:1182-1188)

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