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首页> 外文期刊>Biochemical and Biophysical Research Communications >In vitro reprogramming of rat bone marrow-derived mesenchymal stem cells into insulin-producing cells by genetically manipulating negative and positive regulators
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In vitro reprogramming of rat bone marrow-derived mesenchymal stem cells into insulin-producing cells by genetically manipulating negative and positive regulators

机译:通过遗传调控负调控因子和正调控因子,将大鼠骨髓间充质干细胞体外重编程为胰岛素产生细胞

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摘要

Islet cell replacement therapy represents the most promising approach for the cure of type 1 diabetes if autoimmunity to β cells is under control. However, this potential is limited by a shortage of pancreas donors. To address the donor shortage problem, we determined whether bone marrow-derived mesenchymal stem cells (bmMSCs) can be directly reprogrammed to islet lineages by simultaneously forced suppression and over-expression of key regulator genes that play critical roles during pancreas development. Here, we report that rat bmMSCs were converted . in vitro into insulin-producing cells by suppressing two-repressor genes repressor element-1 silencing transcription factoreuronal restrictive silencing factor (Rest/Nrsf) and sonic hedgehog (Shh) and by over-expressing pancreas and duodenal transcription factor 1 (Pdx1). The reprogrammed bmMSCs expressed both genes and proteins specific for islet cells. These converted cells were capable of releasing insulin in a glucose-responsive manner. Our study suggests that bmMSCs may ultimately be reprogrammed to functional insulin-secreting cells.
机译:如果对β细胞的自身免疫得到控制,则胰岛细胞替代疗法是治愈1型糖尿病的最有前途的方法。但是,由于胰腺供体的缺乏,这种潜力受到了限制。为了解决供体短缺的问题,我们确定了是否可以通过同时强制抑制和过度表达在胰腺发育过程中起关键作用的关键调节基因来直接将骨髓来源的间充质干细胞(bmMSC)重新编程为胰岛谱系。在这里,我们报道了大鼠bmMSC已被转化。通过抑制两个阻遏物基因阻遏物1沉默转录因子/神经元限制性沉默因子(Rest / Nrsf)和声波刺猬(Shh)以及过量表达胰腺和十二指肠转录因子1(Pdx1)体外进入产生胰岛素的细胞。重新编程的bmMSC表达了胰岛细胞特异的基因和蛋白质。这些转化的细胞能够以葡萄糖应答方式释放胰岛素。我们的研究表明,bmMSCs最终可能会被重新编程为功能性胰岛素分泌细胞。

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