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Transient cytokine treatment induces acinar cell reprogramming and regenerates functional beta cell mass in diabetic mice

机译:瞬时细胞因子治疗诱导糖尿病小鼠的腺泡细胞重编程并再生功能性β细胞

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摘要

Reprogramming of pancreatic exocrine cells into cells resembling beta cells may provide a strategy for treating diabetes. Here we show that transient administration of epidermal growth factor and ciliary neurotrophic factor to adult mice with chronic hyperglycemia efficiently stimulates the conversion of terminally differentiated acinar cells to beta-like cells. Newly generated beta-like cells are epigenetically reprogrammed, functional and glucose responsive, and they reinstate normal glycemic control for up to 248 d. The regenerative process depends on Stat3 signaling and requires a threshold number of Neurogenin 3 (Ngn3)-expressing acinar cells. In contrast to previous work demonstrating in vivo conversion of acinar cells to beta-like cells by viral delivery of exogenous transcription factors, our approach achieves acinar-to-beta-cell reprogramming through transient cytokine exposure rather than genetic modification.
机译:胰腺外分泌细胞重编程为类似于β细胞的细胞可能提供治疗糖尿病的策略。在这里,我们显示向患有慢性高血糖症的成年小鼠短暂施用表皮生长因子和睫状神经营养因子有效刺激了终末分化的腺泡细胞向β样细胞的转化。新产生的β样细胞经过表观遗传重编程,功能性和葡萄糖反应性,可恢复正常血糖控制长达248 d。再生过程取决于Stat3信号传导,并需要一定数量的表达Neurogenin 3(Ngn3)的腺泡细胞。与以前的研究表明通过病毒传递外源转录因子在体内将腺泡细胞转化为β样细胞的工作相反,我们的方法是通过短暂的细胞因子暴露而不是基因修饰实现了腺泡到β细胞的重编程。

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