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Stage-specific signaling through TGFβ family members and WNT regulates patterning and pancreatic specification of human pluripotent stem cells

机译:通过TGFβ家族成员和WNT进行的阶段特异性信号传导调节人多能干细胞的模式和胰腺功能

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摘要

The generation of insulin-producing β-cells from human pluripotent stem cells is dependent on efficient endoderm induction and appropriate patterning and specification of this germ layer to a pancreatic fate. In this study, we elucidated the temporal requirements for TGFβ family members and canonical WNT signaling at these developmental stages and show that the duration of nodal/activin A signaling plays a pivotal role in establishing an appropriate definitive endoderm population for specification to the pancreatic lineage. WNT signaling was found to induce a posterior endoderm fate and at optimal concentrations enhanced the development of pancreatic lineage cells. Inhibition of the BMP signaling pathway at specific stages was essential for the generation of insulin-expressing cells and the extent of BMP inhibition required varied widely among the cell lines tested. Optimal stage-specific manipulation of these pathways resulted in a striking 250-fold increase in the levels of insulin expression and yielded populations containing up to 25% C-peptide+ cells.
机译:由人多能干细胞产生胰岛素的β细胞的产生取决于有效的内胚层诱导以及该胚层对胰腺命运的适当模式和规格。在这项研究中,我们阐明了在这些发育阶段对TGFβ家族成员和经典WNT信号转导的时间要求,并表明节点/激活素A信号转导的持续时间在建立合适的定形内胚层群体以规范胰腺谱系中起着关键作用。发现WNT信号传导诱导后内胚层命运,并且在最佳浓度下增强了胰腺谱系细胞的发育。在特定阶段抑制BMP信号通路对于表达胰岛素的细胞至关重要,并且在所测试的细胞系之间,所需的BMP抑制程度差异很大。这些途径的最佳阶段特异性操作导致胰​​岛素表达水平显着提高250倍,并产生了包含高达25%C-肽+细胞的群体。

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