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Sox9: A Master Regulator of the Pancreatic Program

机译:Sox9:胰腺程序的主要调节者

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Over the last decade, it has been discovered that the transcription factor Sox9 plays several critical roles in governing the development of the embryonic pancreas and the homeostasis of the mature organ. While analysis of pancreata from patients affected by the Sox9 haploinsufficiency syndrome campomelic dysplasia initially alluded to a functional role of Sox9 in pancreatic morphogenesis, transgenic mouse models have been instrumental in mechanistically dissecting such roles. Although initially defined as a marker and maintenance factor for pancreatic progenitors, Sox9 is now considered to fulfill additional indispensable functions during pancreogenesis and in the postnatal organ through its interactions with other transcription factors and signaling pathways such as Fgf and Notch. In addition to maintaining both multipotent and bipotent pancreatic progenitors, Sox9 is also required for initiating endocrine differentiation and maintaining pancreatic ductal identity, and it has recently been unveiled as a key player in the initiation of pancreatic cancer. These functions of Sox9 are discussed in this article, with special emphasis on the knowledge gained from various loss-of-function and lineage tracing mouse models. Also, current controversies regarding Sox9 function in healthy and injured adult pancreas and unanswered questions and avenues of future study are discussed.
机译:在过去的十年中,已经发现转录因子Sox9在控制胚胎胰腺的发育和成熟器官的体内平衡方面起着关键作用。虽然最初受Sox9单倍剂量不足综合症候群影响的患者的胰脏分析表明,Sop9在胰腺形态发生中起功能性作用,但转基因小鼠模型在机械解剖此类作用中发挥了作用。尽管最初将Sox9定义为胰腺祖细胞的标志物和维持因子,但现在认为Sox9通过与其他转录因子和信号传导途径(例如Fgf和Notch)的相互作用,在胰腺生成过程中和产后器官中履行额外的必不可少的功能。除了维持多能胰腺和双能胰腺祖细胞外,Sox9还需要用于启动内分泌分化和维持胰腺导管特性,并且最近被公认为是引发胰腺癌的关键因素。本文讨论了Sox9的这些功能,特别着重于从各种功能丧失和沿袭追踪鼠标模型获得的知识。此外,还讨论了有关健康和受伤成人胰腺中Sox9功能的当前争议,以及未解决的问题和未来研究的途径。

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