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Id genes are essential for early heart formation

机译:ID基因对于早期心脏形成至关重要

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摘要

Deciphering the fundamental mechanisms controlling cardiac specification is critical for our understanding of how heart formation is initiated during embryonic development and for applying stem cell biology to regenerative medicine and disease modeling. Using systematic and unbiased functional screening approaches, we discovered that the Id family of helix-loop-helix proteins is both necessary and sufficient to direct cardiac mesoderm formation in frog embryos and human embryonic stem cells. Mechanistically, Id proteins specify cardiac cell fate by repressing two inhibitors of cardiogenic mesoderm formation-Tcf3 and Foxa2-and activating inducers Evx1, Grrp1, and Mesp1. Most importantly, CRISPR/Cas9-mediated ablation of the entire Id (Id1-4) family in mouse embryos leads to failure of anterior cardiac progenitor specification and the development of heartless embryos. Thus, Id proteins play a central and evolutionarily conserved role during heart formation and provide a novel means to efficiently produce cardiovascular progenitors for regenerative medicine and drug discovery applications.
机译:解读控制心脏规范的基本机制对于我们了解在胚胎发育期间如何启动心脏形成以及将干细胞生物学应用于再生医学和疾病建模。使用系统和无偏函数的功能筛选方法,我们发现螺旋环螺旋蛋白的ID系列是必要的,并且足以引导青蛙胚胎和人胚胎干细胞中的心脏切片形成。机械地,ID蛋白通过抑制胸膜内胚层形成-TCF3和FOXA2-和活化诱导剂EVX1,GRRP1和MES1的两种抑制剂来指定心脏细胞命运。最重要的是,CRISPR / CAS9介导的小鼠胚胎中的整个ID(ID1-4)家族的消融导致前心祖细胞规格的失效和无心胚胎的发育。因此,ID蛋白在心脏形成期间发挥着中心和进化的保守作用,并提供一种新颖的手段,以有效地生产用于再生药和药物发现应用的心血管祖细胞。

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