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首页> 外文期刊>Yonsei Medical Journal >Transdifferentiation of Cultured Bovine Lens Epithelial Cells into Myofibroblast-like Cells by Serum Modulation
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Transdifferentiation of Cultured Bovine Lens Epithelial Cells into Myofibroblast-like Cells by Serum Modulation

机译:血清调制将培养的牛晶状体上皮细胞转分化为成肌纤维细胞样细胞

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摘要

An after-cataract is caused by the proliferation of residual cells over the equator of the lens. These cells subsequently migrate to the posterior lens capsule, where they undergo aberrant differentiation into fiber-like cells or transdifferentiation into fibroblast-like cells. To study the precise molecular mechanisms of transdifferentiation, an attempt was made to establish an in vitro system, in which the lens epithelial cells (LECs) of the pre-equatorial zone could be transdifferentiated into fibroblast-like cells. The required conditions for culturing the LECs were identified as consisting of four phases; intact bovine explants, explant-cultured, serum-modulated and additionally modulated LECs. The LECs of each phase were compared by examining changes in the expression of the epithelial-mesenchymal transition (EMT)-related genes and changes in cellular morphology and adhesion. The explants that were cultured in a medium containing 10% fetal bovine serum (FBS) for 2 weeks, showed changes in the expression of the EMT-related genes, although the other explant-cultured cells maintained an epithelial morphology. To introduce a transition into mesenchymal cells, the explant cultures were subcultured in a medium containing 20% FBS for six passages. These cells displayed an elongated morphology and were able to grow and migrate in a similar way to fibroblast cells. The expression of the EMT-related genes, such as, extracellular matrix proteins and integrins, was altered. This was similar to the alteration of the 3-dimensional collagen gels model previously reported. During a further process of EMT by additional serum modulation, the inhibitory effect of disintegrin on cell adhesion was gradually decreased, integrin expression was differentially regulated and α-smooth muscle actin was post-translationally modified from the point of passage number six. Overall, it can be concluded that terminal transdifferentiation accompanies changes in the cytoskeletal proteins and cell surface molecules. These are modulated in systematic patterns of post-transcriptional and post-translational regulation and patterns of gene regulation, by the synergic effects of several transforming factors contained in serum. Therefore, posterior capsular opacification may also be accompanied by this molecular mechanism.
机译:白内障的后遗症是由晶状体的赤道上方的残留细胞的增殖引起的。这些细胞随后迁移到晶状体后囊,在那里它们经历异常分化为纤维状细胞或转分化为成纤维细胞状细胞。为了研究转分化的精确分子机制,尝试建立一种体外系统,在该系统中,赤道前区的晶状体上皮细胞(LEC)可以转分化为成纤维细胞样细胞。培养LEC的必要条件被确定为包括四个阶段。完整的牛外植体,外植培养,血清调节和额外调节的LEC。通过检查上皮-间质转化(EMT)相关基因的表达变化以及细胞形态和粘附的变化,比较了每个阶段的LEC。在含有10%胎牛血清(FBS)的培养基中培养了2周的外植体,显示了EMT相关基因表达的变化,尽管其他外植体培养的细胞保持了上皮形态。为了向间充质细胞中引入过渡,将外植体培养物在含有20%FBS的培养基中传代培养6代。这些细胞表现出细长的形态,并能够以与成纤维细胞相似的方式生长和迁移。 EMT相关基因,如细胞外基质蛋白和整合素的表达被改变。这类似于先前报道的3维胶原蛋白凝胶模型的改变。在通过额外的血清调节进一步进行EMT的过程中,从第6代的角度出发,Disintegrin对细胞黏附的抑制作用逐渐降低,Integrin表达受到差异调节,α-平滑肌肌动蛋白被翻译后修饰。总的来说,可以得出结论,终末转分化伴随着细胞骨架蛋白和细胞表面分子的变化。通过血清中包含的几种转化因子的协同作用,以转录后和翻译后调控的系统模式以及基因调控的模式来调节这些基因。因此,后囊混浊也可能伴随着这种分子机制。

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