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Notch signaling controls multiple steps of pancreatic differentiation

机译:Notch信号控制胰腺分化的多个步骤

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Multiple cell types of the pancreas appear asynchronously during embryogenesis, which requires that pancreatic progenitor cell potential changes over time. Loss-of-function studies have shown that Notch signaling modulates the differentiation of these progenitors, but it remains unclear how and when the Notch pathway acts. We established a modular transgenic system to heritably activate mouse Notch1 in multiple types of progenitors and differentiated cells. We find that misexpression of activated Notch in Pdx1-expressing progenitor cells prevents differentiation of both exocrine and endocrine lineages. Progenitors remain trapped in an undifferentiated state even if Notch activation occurs long after the pancreas has been specified. Furthermore, endocrine differentiation is associated with escape from this activity, because Ngn3-expressing endocrine precursors are susceptible to Notch inhibition, whereas fully differentiated endocrine cells are resistant.
机译:胰腺的多种细胞类型在胚胎发生过程中异步出现,这要求胰腺祖细胞电位随时间变化。功能丧失的研究表明,Notch信号传导可调节这些祖细胞的分化,但尚不清楚Notch途径的作用方式和作用时间。我们建立了一个模块化的转基因系统,以遗传激活多种类型的祖细胞和分化细胞中的小鼠Notch1。我们发现,在表达Pdx1的祖细胞中激活的Notch的错误表达阻止了外分泌和内分泌谱系的分化。即使在指定了胰腺后很长时间才发生Notch激活,祖细胞仍处于未分化状态。此外,内分泌分化与逃避该活性有关,因为表达Ngn3的内分泌前体易受Notch抑制,而完全分化的内分泌细胞则具有抗性。

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