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NOTCH signaling specifies arterial-type definitive hemogenic endothelium from human pluripotent stem cells

机译:NOTCH信号传导可指定人类多能干细胞的动脉型定型造血内皮

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摘要

NOTCH signaling is required for the arterial specification and formation of hematopoietic stem cells (HSCs) and lympho-myeloid progenitors in the embryonic aorta-gonad-mesonephros region and extraembryonic vasculature from a distinct lineage of vascular endothelial cells with hemogenic potential. However, the role of NOTCH signaling in hemogenic endothelium (HE) specification from human pluripotent stem cell (hPSC) has not been studied. Here, using a chemically defined hPSC differentiation system combined with the use of DLL1-Fc and DAPT to manipulate NOTCH, we discover that NOTCH activation in hPSC-derived immature HE progenitors leads to formation of CD144+CD43CD73DLL4+Runx1 + 23-GFP+ arterial-type HE, which requires NOTCH signaling to undergo endothelial-to-hematopoietic transition and produce definitive lympho-myeloid and erythroid cells. These findings demonstrate that NOTCH-mediated arterialization of HE is an essential prerequisite for establishing definitive lympho-myeloid program and suggest that exploring molecular pathways that lead to arterial specification may aid in vitro approaches to enhance definitive hematopoiesis from hPSCs.
机译:NOTCH信号是动脉规格和在胚胎主动脉-性腺-中肾区域和胚胎外脉管系统中形成的造血干细胞(HSC)和淋巴-髓系祖细胞以及具有血管生成潜能的独特血管系所必需的。但是,尚未研究NOTCH信号在人多能干细胞(hPSC)的造血内皮(HE)规范中的作用。在这里,使用化学定义的hPSC分化系统,结合使用DLL1-Fc和DAPT来操纵NOTCH,我们发现,hPSC衍生的未成熟HE祖细胞中的NOTCH激活导致CD144 + CD43 < sup>- CD73 - DLL4 + Runx1 + 23-GFP + 动脉型HE,需要进行NOTCH信号转入内皮到造血细胞的过渡并产生确定的淋巴髓样和红系细胞。这些发现表明,NOTCH介导的HE的动脉化是建立确定的淋巴-髓样程序的必要先决条件,并表明探索导致动脉特异性的分子途径可能有助于增强hPSCs的确定性造血作用的体外方法。

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