首页> 美国卫生研究院文献>PLoS Clinical Trials >DMH1, a Novel BMP Small Molecule Inhibitor, Increases Cardiomyocyte Progenitors and Promotes Cardiac Differentiation in Mouse Embryonic Stem Cells
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DMH1, a Novel BMP Small Molecule Inhibitor, Increases Cardiomyocyte Progenitors and Promotes Cardiac Differentiation in Mouse Embryonic Stem Cells

机译:DMH1,一种新型的BMP小分子抑制剂,可增加心肌祖细胞并促进小鼠胚胎干细胞的心脏分化。

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摘要

The possibility of using cell-based therapeutics to treat cardiac failure has generated significant interest since the initial introduction of stem cell-based technologies. However, the methods to quickly and robustly direct stem cell differentiation towards cardiac cell types have been limited by a reliance on recombinant growth factors to provide necessary biological cues. We report here the use of dorsomorphin homologue 1 (DMH1), a second-generation small molecule BMP inhibitor based on dorsomorphin, to efficiently induce beating cardiomyocyte formation in mouse embryonic stem cells (ESCs) and to specifically upregulate canonical transcriptional markers associated with cardiac development. DMH1 differs significantly from its predecessor by its ability to enrich for pro-cardiac progenitor cells that respond to late-stage Wnt inhibition using XAV939 and produce secondary beating cardiomyocytes. Our study demonstrates the utility of small molecules to complement existing in vitro cardiac differentiation protocols and highlights the role of transient BMP inhibition in cardiomyogenesis.
机译:自从最初引入基于干细胞的技术以来,使用基于细胞的疗法来治疗心力衰竭的可能性引起了人们的极大兴趣。但是,通过依赖重组生长因子来提供必要的生物学线索,将干细胞分化快速而有力地引导至心脏细胞类型的方法受到了限制。我们在这里报告使用dorsomorphin同源物1(DMH1),基于dorsomorphin的第二代小分子BMP抑制剂,以有效诱导小鼠胚胎干细胞(ESC)中跳动的心肌细胞形成,并特异性上调与心脏发育相关的规范转录标记。 DMH1与它的前代产品的显着不同之处在于,它能够富集使用XAV939对后期Wnt抑制产生响应的前心脏祖细胞并产生继发性跳动的心肌细胞。我们的研究表明小分子补充现有体外心脏分化方案的效用,并强调了短暂BMP抑制作用在心肌发生中的作用。

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