首页> 外文期刊>Differentiation: The Journal of the International Society of Differentiation >Human bone marrow mesenchymal stem cells differentiate into insulin-producing cells upon microenvironmental manipulation in vitro.
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Human bone marrow mesenchymal stem cells differentiate into insulin-producing cells upon microenvironmental manipulation in vitro.

机译:在体外微环境操作下,人骨髓间充质干细胞分化为产生胰岛素的细胞。

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It was recently reported that pluripotent mesenchymal stem cells (MSCs) in rodent bone marrow (BM) have the capacity to generate insulin-producing cells (IPCs) in vitro. However, little is known about this capacity in human BM-MSCs. We developed a nongenetic method to induce human BM-MSCs to transdifferentiate into IPCs both phenotypically and functionally. BM-MSCs from 12 human donors were sequentially cultured in specially defined conditions. Their differentiation extent toward beta-cell phenotype was evaluated systemically. Specifically, after induction human BM-MSCs formed spheroid islet-like clusters containing IPCs, which was further confirmed by dithizone (DTZ) staining and electron microscopy. These IPCs expressed multiple genes related to the development or function of pancreatic beta cells (including NKX6.1, ISL-1, Beta2/Neurod, Glut2, Pax6, nestin, PDX-1, ngn3, insulin and glucagon). The coexpression of insulin and c-peptide was observed in IPCs by immunofluorescence. Moreover, they were able to release insulin in a glucose-dependent manner and ameliorate the diabetic conditions of streptozotocin (STZ)-treated nude mice. These results indicate that human BM-MSCs might be an available candidate to overcome limitations of islet transplantation.
机译:最近有报道说,啮齿动物骨髓(BM)中的多能间充质干细胞(MSC)具有在体外产生胰岛素产生细胞(IPC)的能力。但是,关于人BM-MSC的这种能力知之甚少。我们开发了一种非遗传方法来诱导人类BM-MSC在表型和功能上转分化为IPC。在特殊定义的条件下顺序培养来自12个人类供体的BM-MSC。系统评价了它们向β细胞表型的分化程度。具体而言,诱导后,人BM-MSC形成了包含IPC的类胰岛样簇,这通过双硫zone(DTZ)染色和电子显微镜进一步证实。这些IPC表达了与胰腺β细胞的发育或功能相关的多个基因(包括NKX6.1,ISL-1,Beta2 / Neurod,Glut2,Pax6,巢蛋白,PDX-1,ngn3,胰岛素和胰高血糖素)。通过免疫荧光在IPC中观察到胰岛素和c肽的共表达。此外,它们能够以葡萄糖依赖性方式释放胰岛素,并改善经链脲佐菌素(STZ)治疗的裸鼠的糖尿病状况。这些结果表明,人类BM-MSCs可能是克服胰岛移植局限性的有效候选者。

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