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Update of extracellular matrix, its receptors, and cell adhesion molecules in mammalian nephrogenesis.

机译:哺乳动物肾发生中细胞外基质,其受体和细胞粘附分子的更新。

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摘要

One of the hallmarks of mammalian nephrogenesis includes a mesenchymal-epithelial transition that is accomplished by intercalation of the ureteric bud, an epithelium-lined tubelike structure, into an undifferentiated mesenchyme, and the latter then undergoes an inductive transformation and differentiates into an epithelial phenotype. At the same time, the differentiating mesenchyme reciprocates by inducing branching morphogenesis of the ureteric bud, which forms a treelike structure with dichotomous iterations. These reciprocal inductive interactions lead to the development of a functioning nephron unit made up of a glomerulus and proximal and distal tubules. The inductive interactions and differentiation events are modulated by a number of transcription factors, protooncogenes, and growth factors and their receptors, which regulate the expression of target morphogenetic modulators including the ECM, integrin receptors, and cell adhesion molecules. These target macromolecules exhibit spatiotemporal andstage-specific developmental regulation in the metanephros. The ECM molecules expressed at the epithelial-mesenchymal interface are perhaps the most relevant and conducive to the paracrine-juxtacrine interactions in a scenario where the ligand is expressed in the mesenchyme while the receptor is located in the ureteric bud epithelium or vice versa. In addition, expression of the target ECM macromolecules is regulated by matrix metalloproteinases and their inhibitors to generate a concentration gradient at the interface to further propel epithelial-mesenchymal interactions so that nephrogenesis can proceed seamlessly. In this review, we discuss and update our current understanding of the role of the ECM and related macromolecules with respect to metanephric development.
机译:哺乳动物肾发生的标志之一包括间充质-上皮转变,该过程通过将输尿管芽,上皮衬里的管状结构插入未分化的间充质而实现,然后后者进行诱导转化并分化为上皮表型。同时,分化的间充质通过诱导输尿管芽的分支形态发生往复运动,形成带有二分迭代的树状结构。这些相互的感应相互作用导致功能性肾单位的发展,该单位由肾小球以及近端和远端小管组成。诱导相互作用和分化事件受到许多转录因子,原癌基因,生长因子及其受体的调节,这些转录因子调节包括ECM,整联蛋白受体和细胞粘附分子在内的目标形态发生调节剂的表达。这些目标大分子在后肾中表现出时空和阶段特定的发育调节。在配体在间充质中表达而受体位于输尿管芽上皮的情况下,在上皮-间质界面表达的ECM分子可能与旁分泌-邻分泌相互作用最相关,也最有利。另外,靶ECM大分子的表达受到基质金属蛋白酶及其抑制剂的调节,以在界面处产生浓度梯度,以进一步推进上皮-间质相互作用,从而肾发生可以无缝地进行。在这篇综述中,我们讨论并更新了我们目前对ECM和相关大分子在后肾发展方面的作用的理解。

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