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Signals From the Embryonic Mouse Pancreas Induce Differentiation of Human Embryonic Stem Cells Into Insulin-Producing {beta}-Cell-Like Cells.

机译:来自胚胎小鼠胰腺的信号诱导人胚胎干细胞分化成胰岛素产生的{β}细胞样细胞。

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摘要

The recent success in restoring normoglycemia in type 1 diabetes by islet cell transplantation indicates that cell replacement therapy of this severe disease is achievable. However, the severe lack of donor islets has increased the demand for alternative sources of beta-cells, such as adult and embryonic stem cells. Here, we investigate the potential of human embryonic stem cells (hESCs) to differentiate into beta-cells. Spontaneous differentiation of hESCs under two-dimensional growth conditions resulted in differentiation of Pdx1(+)/Foxa2(+) pancreatic progenitors and Pdx1(+)/Isl1(+) endocrine progenitors but no insulin-producing cells. However, cotransplantation of differentiated hESCs with the dorsal pancreas, but not with the liver or telencephalon, from mouse embryos resulted in differentiation of beta-cell-like cell clusters. Comparative analysis of the basic characteristics of hESC-derived insulin(+) cell clusters with human adult islets demonstrated that the insulin(+) cells share important features with normal beta-cells, such as synthesis (proinsulin) and processing (C-peptide) of insulin and nuclear localization of key beta-cell transcription factors, including Foxa2, Pdx1, and Isl1.
机译:通过胰岛细胞移植在恢复1型糖尿病的正常血糖方面的最新成功表明,可以对这种严重疾病进行细胞替代治疗。然而,供体胰岛的严重缺乏增加了对β细胞替代来源的需求,例如成人和胚胎干细胞。在这里,我们研究了人类胚胎干细胞(hESCs)分化为β细胞的潜力。 hESCs在二维生长条件下的自发分化导致分化的Pdx1(+)/ Foxa2(+)胰腺祖细胞和Pdx1(+)/ Isl1(+)内分泌祖细胞,但没有产生胰岛素的细胞。然而,从小鼠胚胎中分化出的hESCs与背胰的共移植,而不是肝脏或端脑的共同移植,导致了β细胞样细胞簇的分化。与人类成年胰岛的hESC衍生的胰岛素(+)细胞簇的基本特征的比较分析表明,胰岛素(+)细胞与正常的β细胞具有重要的功能,例如合成(胰岛素原)和加工(C肽)胰岛素和关键β细胞转录因子(包括Foxa2,Pdx1和Isl1)的核定位。

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