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首页> 外文期刊>Development >Notch pathway activation can replace the requirement for Wnt4 and Wnt9b in mesenchymal-to-epithelial transition of nephron stem cells.
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Notch pathway activation can replace the requirement for Wnt4 and Wnt9b in mesenchymal-to-epithelial transition of nephron stem cells.

机译:Notch通路的激活可以替代肾干细胞间质向上皮转化过程中对Wnt4和Wnt9b的需求。

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The primary excretory organ in vertebrates is the kidney, which is responsible for blood filtration, solute homeostasis and pH balance. These functions are carried out by specialized epithelial cells organized into tubules called nephrons. Each of these cell types arise during embryonic development from a mesenchymal stem cell pool through a process of mesenchymal-to-epithelial transition (MET) that requires sequential action of specific Wnt signals. Induction by Wnt9b directs cells to exit the stem cell niche and express Wnt4, which is both necessary and sufficient for the formation of epithelia. Without either factor, MET fails, nephrons do not form and newborn mice die owing to kidney failure. Ectopic Notch activation in stem cells induces mass differentiation and exhaustion of the stem cell pool. To investigate whether this reflected an interaction between Notch and Wnt, we employed a novel gene manipulation strategy in cultured embryonic kidneys. We show that Notch activation is capable of inducing MET in the absence of both Wnt4 and Wnt9b. Following MET, the presence of Notch directs cells primarily to the proximal tubule fate. Only nephron stem cells have the ability to undergo MET in response to Wnt or Notch, as activation in the closely related stromal mesenchyme has no inductive effect. These data demonstrate that stem cells for renal epithelia are uniquely poised to undergo MET, and that Notch activation can replace key inductive Wnt signals in this process. After MET, Notch provides an instructive signal directing cells towards the proximal tubule lineage at the expense of other renal epithelial fates.
机译:脊椎动物的主要排泄器官是肾脏,肾脏负责血液过滤,溶质稳态和pH平衡。这些功能是通过组织成肾小管的特殊上皮细胞来实现的。这些细胞类型中的每一种都在胚胎发育过程中从间充质干细胞库通过间充质到上皮的转变(MET)过程产生,该过程需要特定Wnt信号的顺序作用。 Wnt9b的诱导可引导细胞离开干细胞生态位并表达Wnt4,这对于上皮细胞的形成既必要又充分。没有任何一个因素,MET就会失效,肾单位不会形成,新生小鼠会因肾衰竭而死亡。干细胞中的异位Notch激活诱导干细胞池的质量分化和衰竭。为了调查这是否反映了Notch和Wnt之间的相互作用,我们在培养的胚胎肾脏中采用了一种新颖的基因操纵策略。我们表明Notch激活能够在没有Wnt4和Wnt9b的情况下诱导MET。 MET后,Notch的存在主要将细胞引导至近端小管命运。只有肾单位干细胞才具有响应Wnt或Notch的能力,因为在紧密相关的基质间质中的激活没有诱导作用。这些数据表明,肾上皮的干细胞具有独特的平衡能力,可以进行MET,并且Notch激活可以取代这一过程中的关键诱导性Wnt信号。 MET后,Notch提供指导性信号,将细胞引向近端小管细胞系,但以其他肾上皮的命运为代价。

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