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EpCAM induction functionally links to the Wnt-enhanced cell proliferation in human keratinocytes

机译:EpCAM诱导功能上与人类角质形成细胞中Wnt增强的细胞增殖相关

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Accelerating proliferation of primary keratinocytes benefits skin autografts for severely burned patients. Wnt signal, a conserved pathway controlling cell cycle and morphogenesis in embryo, also involves in cell proliferation and tumorigenesis in adult tissues. Here the effects of Wnt signal on the growth of human interfollicular keratinocytes were investigated. We demonstrated that recombinant Wnt3a significantly promoted the growth of primary keratinocytes at a low cell density. A well-characterized GSK-3β inhibitor, BIO, activated the Wnt signals and also enhanced the colony formation of keratinocytes dose dependently. Gene expression profile of the BIO-treated keratinocytes revealed the linkage of BIO with cell mitosis and indicated that epithelial cell adhesion molecule (EpCAM), a Wnt target gene, was significantly upregulated. Compared to the sorted EpCAM-keratinocytes, the EpCAM+ cells showed a higher proliferation rate and efficacy of colony formation. Inhibiting the EpCAM expression by shRNA attenuated the proliferation effect of BIO and the growth advantage of the EpCAM+ keratinocytes. These evidences emphasize the positive roles of canonical Wnt and EpCAM on the regulation of cell growth and self-renewal of human keratinocytes.
机译:对于严重烧伤的患者,加速原代角质形成细胞的增殖有益于皮肤自体移植。 Wnt信号是控制胚胎中细胞周期和形态发生的保守途径,也参与成年组织的细胞增殖和肿瘤发生。在这里,研究了Wnt信号对人小泡间角质形成细胞生长的影响。我们证明了重组Wnt3a在低细胞密度下可显着促进原代角质形成细胞的生长。表征良好的GSK-3β抑制剂BIO激活Wnt信号,并剂量依赖性地增强了角质形成细胞的集落形成。经BIO处理的角质形成细胞的基因表达谱揭示了BIO与细胞有丝分裂的联系,并表明Wnt目标基因上皮细胞粘附分子(EpCAM)明显上调。与分选的EpCAM-角质形成细胞相比,EpCAM +细胞显示出更高的增殖速率和集落形成功效。 shRNA抑制EpCAM表达会减弱BIO的增殖作用以及EpCAM +角质形成细胞的生长优势。这些证据强调了经典的Wnt和EpCAM在调节人类角质形成细胞的细胞生长和自我更新中的积极作用。

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