首页> 外文期刊>The Review of Diabetic Studies : RDS >Human Placenta-Derived Mesenchymal Stem Cells and Islet-Like Cell Clusters Generated From These Cells as a Novel Source for Stem Cell Therapy in Diabetes
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Human Placenta-Derived Mesenchymal Stem Cells and Islet-Like Cell Clusters Generated From These Cells as a Novel Source for Stem Cell Therapy in Diabetes

机译:人胎盘来源的间充质干细胞和从这些细胞产生的胰岛样细胞簇,作为糖尿病干细胞治疗的新来源

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Placental tissue holds great promise as a source of cells for regenerative medicine due to its plasticity, and easy availability. Human placenta-derived mesenchymal stem cells (hPDMSCs) have the potential to differentiate into insulin-producing cells. Upon transplantation, they can reverse experimental diabetes in mice. However, it is not known whether culture-expanded undifferentiated hPDMSCs are capable of restoring normoglycemia upon transplantation in streptozotocin (STZ)-induced diabetic mice. Hence we prepared long-term cultures of hPDMSCs from the chorionic villi of full-term human placenta. Flow cytometry analyses and immunocytochemistry study revealed bonafide mesenchymal nature of the isolated hPDMSCs. These cultures could differentiate into adipogenic, oesteogenic, chondrogenic, and neuronal lineages on exposure to lineage-specific cocktails. Furthermore, we showed that hPDMSCs can form islet-like cell clusters (ILCs) on stepwise exposure to serum-free defined media containing specific growth factors and differentiating agents. qRT-PCR showed the expression of insulin, glucagon, and somatostatin in undifferentiated hPDMSCs and in ILCs. Differentiated ILCs were found to express human insulin, glucagon, and somatostatin by immunocytochemistry. Additionally, ILCs also showed abundance of pancreatic transcription factors ngn3 and isl1. Both undifferentiated hPDMSCs and ILCs exihibited insulin secretion in response to glucose. Transplantation of hPDMSCs or ILCs derived from hPDMSCs in STZ-induced diabetic mice led to restoration of normoglycemia. Our results demonstrate, for the first time, reversal of hyperglycemia by undifferentiated hPDMSCs and ILCs derived from hPDMSCs. These results suggest human placenta-derived MSCs as an alternative source for cell replacement therapy in diabetes.
机译:胎盘组织由于其可塑性和易获得性而有望作为再生医学的细胞来源。人胎盘来源的间充质干细胞(hPDMSC)具有分化为胰岛素产生细胞的潜力。移植后,它们可以逆转小鼠的实验性糖尿病。但是,尚不知道在链脲佐菌素(STZ)诱导的糖尿病小鼠中移植后,培养物扩增的未分化hPDMSC是否能够恢复正常血糖。因此,我们从足月人胎盘的绒毛中制备了hPDMSC的长期培养物。流式细胞仪分析和免疫细胞化学研究揭示了分离的hPDMSC的间质性质。暴露于特定谱系的鸡尾酒后,这些培养物可分为成脂,成骨,成软骨和神经元​​谱系。此外,我们表明,hPDMSCs逐步暴露于含有特定生长因子和分化剂的无血清定义培养基后,可形成胰岛样细胞簇(ILC)。 qRT-PCR显示未分化的hPDMSC和ILC中胰岛素,胰高血糖素和生长抑素的表达。通过免疫细胞化学发现分化的ILC表达人胰岛素,胰高血糖素和生长抑素。此外,ILC还显示出大量的胰腺转录因子ngn3和isl1。未分化的hPDMSC和ILC都响应葡萄糖而分泌胰岛素。在STZ诱导的糖尿病小鼠中移植hPDMSC或源自hPDMSC的ILC可以恢复正常血糖。我们的结果首次证明了未分化的hPDMSC和源自hPDMSC的ILC逆转了高血糖。这些结果表明人胎盘来源的MSCs作为糖尿病细胞替代治疗的替代来源。

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