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Inversin Forms a Complex with Catenins and N-Cadherin in Polarized Epithelial Cells

机译:转化蛋白在极化的上皮细胞中与连环蛋白和N-钙黏着蛋白形成复合物

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摘要

Nephrogenesis starts with the reciprocal induction of two embryonically distinct analages, metanephric mesenchyme and ureteric bud. This complex process requires the refined and coordinated expression of numerous developmental genes, such as inv. Mice that are homozygous for a mutation in the inv gene (inv/inv) develop renal cysts resembling autosomal-recessive polycystic kidney disease. The gene locus containing inv has been proposed to serve as a common modifier for some human and rodent polycystic kidney disease phenotypes. We generated polyclonal antibodies to inversin to study its subcellular distribution, potential binding partners, and functional aspects in cultured murine proximal tubule cells. A 125-kDa inversin protein isoform was found at cell-cell junctions. Two inversin isoforms, 140- and 90-kDa, were identified in the nuclear and perinuclear compartments. Plasma membrane allocation of inversin is dependent upon cell-cell contacts and was redistributed when cell adhesion was disrupted after incubation of the cell monolayer with low-calcium/EGTA medium. We further show that the membrane-associated 125-kDa inversin forms a complex with N-cadherin and the catenins. The 90-kDa nuclear inversin complexes with β-catenin. These findings indicate that the inv gene product functions in several cellular compartments, including the nucleus and cell-cell adhesion sites.
机译:肾发生始于两种胚胎上不同的肛门,即后肾间充质和输尿管芽的相互诱导。这个复杂的过程需要许多发育基因(例如inv。)的精确协调表达。对inv基因(inv / inv)突变纯合的小鼠会形成类似于常染色体隐性多囊肾疾病的肾囊肿。有人提出含有inv的基因座可作为某些人类和啮齿动物多囊肾疾病表型的通用修饰子。我们生成了针对肌动蛋白的多克隆抗体,以研究其亚细胞分布,潜在的结合伴侣以及培养的鼠近端小管细胞的功能方面。在细胞与细胞的连接处发现了一个125 kDa的转化蛋白同工型。在核室和核周室中鉴定出两种逆转异构体,分别为140-kDa和90-kDa。肌钙蛋白的质膜分配取决于细胞与细胞之间的接触,当细胞单层与低钙/ EGTA培养基孵育后,细胞粘附受到破坏时,肌钙蛋白会重新分布。我们进一步表明,与膜相关的125 kDa转化酶与N-钙粘蛋白和连环蛋白形成复合物。 90 kDa核转化酶与β-连环蛋白复合。这些发现表明inv基因产物在几个细胞区室中起作用,包括细胞核和细胞-细胞粘附位点。

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