首页> 外文期刊>In Vitro Cellular and Developmental Biology. Animal: Journal of the Tissues Culture Association >Differentiation of human skin-derived precursor cells into functional islet-like insulin-producing cell clusters
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Differentiation of human skin-derived precursor cells into functional islet-like insulin-producing cell clusters

机译:人皮肤来源的前体细胞分化为功能性胰岛样胰岛素产生细胞簇

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Advances in cell-replacement strategies for diabetes have focused on renewable sources of glucose-responsive, insulin-producing cells (IPCs). One of the most proper alternatives is multipotent skin-derived precursors cells (SKPs), which can be differentiated into IPCs. In this study, we reported the isolation and expansion of human skin-derived precursors (hSKPs) followed by their differentiation into IPCs in vitro, through exposure to suitable differentiation factors. The gene expression of endocrine beta cell markers was analyzed by reverse transcriptase-polymerase chain reaction. In addition, insulin production was examined immunocytochemically, and insulin and C-peptide secretion were examined using enzyme-linked immunosorbent assay. Dithizone-stained cellular clusters were observed after approximately 20 d. The clusters were found to be immunoreactive to insulin and expressed multiple genes related to pancreatic beta cell development and function: insulin, Pdx-1, Islet-1, NeuroD, Glut-2, Pax-4, Ngn-3, and Nkx2.2, but not to other pancreas-specific hormones such as glucagon and somatostatin. Cellular clusters were also able to secrete detectable amounts of insulin and C-peptide in a glucose dose-dependent manner. These findings suggest that human SKPs can differentiate into functional IPCs. This may offer a safer cell source for future stem cell-based therapies.
机译:糖尿病细胞替代策略的进展集中在葡萄糖反应性,胰岛素产生细胞(IPC)的可再生来源上。最合适的替代方法之一是多能皮肤来源的前体细胞(SKP),可以将其分化为IPC。在这项研究中,我们报道了人类皮肤来源的前体(hSKPs)的分离和扩增,随后通过暴露于合适的分化因子而在体外分化为IPC。内分泌β细胞标记的基因表达通过逆转录聚合酶链反应进行了分析。另外,通过免疫细胞化学检查胰岛素的产生,并使用酶联免疫吸附测定法检查胰岛素和C-肽的分泌。大约20天后观察到双硫zone染色的细胞簇。发现这些簇对胰岛素具有免疫反应性,并表达了与胰腺β细胞发育和功能相关的多个基因:胰岛素,Pdx-1,Islet-1,NeuroD,Glut-2,Pax-4,Ngn-3和Nkx2.2。 ,但其他胰脏特异性激素(例如胰高血糖素和生长抑素)则不适用。细胞簇还能够以葡萄糖剂量依赖性方式分泌可检测量的胰岛素和C肽。这些发现表明人类SKP可以分化为功能性IPC。这可能为将来基于干细胞的疗法提供更安全的细胞来源。

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