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p120-catenin-dependent junctional recruitment of Shroom3 is required for apical constriction during lens pit morphogenesis

机译:Shroom3的p120-catenin依赖性连接募集是晶状体窝形态形成过程中根尖收缩所需的

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摘要

Apical constriction (AC) is a widely utilized mechanism of cell shape change whereby epithelial cells transform from a cylindrical to conical shape, which can facilitate morphogenetic movements during embryonic development. Invertebrate epithelial cells undergoing AC depend on the contraction of apical cortex-spanning actomyosin filaments that generate force on the apical junctions and pull them toward the middle of the cell, effectively reducing the apical circumference. A current challenge is to determine whether these mechanisms are conserved in vertebrates and to identify the molecules responsible for linking apical junctions with the AC machinery. Utilizing the developing mouse eye as a model, we have uncovered evidence that lens placode AC may be partially dependent on apically positioned myosin-containing filaments associated with the zonula adherens. In addition we found that, among several junctional components, p120-catenin genetically interacts with Shroom3, a protein required for AC during embryonic morphogenesis. Further analysis revealed that, similar to Shroom3, p120-catenin is required for AC of lens cells. Finally, we determined that p120-catenin functions by recruiting Shroom3 to adherens junctions. Together, these data identify a novel role for p120-catenin during AC and further define the mechanisms required for vertebrate AC.
机译:根尖收缩(AC)是细胞形状变化的一种广泛使用的机制,通过这种机制上皮细胞可以从圆柱状转变为圆锥形,从而可以促进胚胎发育过程中的形态发生运动。经受AC的无脊椎动物上皮细胞取决于跨过根尖的皮层肌动蛋白丝的收缩,这些细丝在根尖连接处产生力并将其拉向细胞中间,从而有效地减小了根尖周长。当前的挑战是确定这些机制在脊椎动物中是否保守,并确定负责将顶点连接与AC机械连接的分子。利用发育中的小鼠眼作为模型,我们发现证据表明晶状体斑AC可能部分取决于与小带粘连相关的顶端定位的含肌球蛋白的细丝。此外,我们发现,在几个连接元件中,p120-catenin与Shroom3遗传相互作用,Shroom3是胚胎形态发生过程中AC所需的蛋白质。进一步的分析表明,与Shroom3相似,晶状体细胞AC需要p120-catenin。最后,我们通过募集Shroom3到粘附连接来确定p120-catenin的功能。这些数据共同确定了AC中p120-catenin的新作用,并进一步定义了脊椎动物AC所需的机制。

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