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首页> 外文期刊>International journal of oncology >Alterations in a defined extracellular region of the RON receptor tyrosine kinase promote RON-mediated motile and invasive phenotypes in epithelial cells
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Alterations in a defined extracellular region of the RON receptor tyrosine kinase promote RON-mediated motile and invasive phenotypes in epithelial cells

机译:RON受体酪氨酸激酶的特定细胞外区域的变化促进上皮细胞中RON介导的运动和侵袭性表型

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摘要

Cell migration followed by matrix invasion is a critical step required for epithelial cell differentiation, growth and survival. This study determined the RON receptor in regulation of motile-invasive phenotypes of epithelial cells. Two RON variants, RON165.e11p and RON165, with alterations in a defined extracellular domain were used as the model. RON165 is a splicing variant generated by an mRNA transcript with an in-frame deletion of 49 amino acids encoded by exon 11. In contrast, RON165.e11p was produced by a partial deletion of exon 11 with the elimination of the first 40 amino acids. Thus, RON165.e11p differs from RON165 with nine amino acids retained in the fourth immunoglobulin-plexin-transcription (IPT) domain. Biochemically, both RON165 and RON165.e11p exist as a single-chain protein, residing in the cytoplasm, and failed to mature into the two-chain receptor. Both RON165 and RON165.e11p spontaneously formed oligomers in vivo leading to constitutive phosphorylation and the activation of downstream signaling proteins. Although lacking cell-transforming activities, RON165 and RON165.e11p mediated the epithelial to mesenchymal transition with spindle-like cell morphologies, diminished E-cadherin expression, and increased N-cadherin and vimentin expression. These changes facilitated epithelial cell migration and invasion as modeled in Martin-Darby canine kidney (MDCK) cells. Moreover, expression of RON165 or RON165.e11p in breast epithelial MCF-7 cells diminished epithelial cell phenotypes and increased motile and invasive activities. Thus, alterations in the defined extracellular region result in two unique RON variants with similar biological properties. The ability of RON165 or RON165.e11p to promote motile-invasive phenotypes may represent a mechanism by which RON regulates epithelial cell phenotypes and biological activities.
机译:细胞迁移然后基质侵袭是上皮细胞分化,生长和存活所必需的关键步骤。这项研究确定了RON受体在上皮细胞运动侵袭性表型的调节。模型中使用了两个RON变体RON165.e11p和RON165,它们在定义的细胞外结构域中发生了改变。 RON165是由mRNA转录物产生的剪接变体,其中有外显子11编码的49个氨基酸的读框内缺失。相反,RON165.e11p是通过外显子11的部分缺失并消除了前40个氨基酸而产生的。因此,RON165.e11p与RON165不同,在第四个免疫球蛋白-plexin转录(IPT)域中保留了9个氨基酸。从生化角度看,RON165和RON165.e11p均以单链蛋白形式存在,存在于细胞质中,但未能成熟为双链受体。 RON165和RON165.e11p在体内自发形成寡聚物,导致组成型磷酸化和下游信号蛋白的激活。尽管缺乏细胞转化活性,RON165和RON165.e11p以纺锤状细胞形态介导上皮到间质的转变,减少了E-钙粘蛋白的表达,并增加了N-钙粘蛋白和波形蛋白的表达。如Martin-Darby犬肾(MDCK)细胞中所模拟的,这些变化促进了上皮细胞的迁移和侵袭。此外,RON165或RON165.e11p在乳腺癌上皮MCF-7细胞中的表达减少了上皮细胞的表型,并增加了活动和侵袭活动。因此,限定的细胞外区域的改变导致具有相似生物学特性的两个独特的RON变体。 RON165或RON165.e11p促进运动侵袭性表型的能力可能代表RON调节上皮细胞表型和生物学活性的机制。

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