JAK activity regulates mesoderm cell fate by controlling MESP1 expression

IF 4.5 3区 生物学 Q2 CELL BIOLOGY
Su Yao , Yalin Zhu , Fenglian He , Min Yuan , Rui Jiang , Hongjie Zhang , Yanbin Fu , Ke Wei
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引用次数: 0

Abstract

Cardiac development requires precise gene expression programs at each developmental stage guided by multiple signaling pathways and transcription factors (TFs). MESP1 is transiently expressed in mesoderm, and is essential for subsequent cardiac development, while the precise mechanism regulating its own transcription and mesoderm cell fate is not fully understood. Therefore, we developed a high content screen assay to identify regulators of MESP1 expression in mesodermal cells differentiated from human pluripotent stem cells (hPSCs). The screen identified CYT387, a JAK1/JAK2 kinase inhibitor, as a potent activator of MESP1 expression, which was also found to promote cardiomyocyte differentiation in vitro. Mechanistic studies found that JAK inhibition promotes MESP1 expression by reducing cytoplasmic calcium concentration and subsequently activating canonical WNT signaling. Our study identified a role of JAK signaling in early mesodermal cells, and sheds light on the connection between the JAK-STAT pathway and transcriptional regulation of MESP1, which expands our understanding of mesoderm and cardiac development.

JAK 活性通过控制 MESP1 的表达调节中胚层细胞的命运
心脏的发育需要在每个发育阶段由多种信号通路和转录因子(TFs)引导的精确基因表达程序。MESP1 在中胚层瞬时表达,对随后的心脏发育至关重要,但其自身转录和中胚层细胞命运的精确调控机制尚不完全清楚。因此,我们开发了一种高含量筛选检测方法,以确定人多能干细胞(hPSCs)分化出的中胚层细胞中 MESP1 表达的调节因子。筛选结果表明,JAK1/JAK2 激酶抑制剂 CYT387 是 MESP1 表达的强效激活剂,它还能促进体外心肌细胞分化。机理研究发现,JAK抑制通过降低细胞质钙离子浓度并随后激活典型WNT信号来促进MESP1的表达。我们的研究发现了 JAK 信号在早期中胚层细胞中的作用,并揭示了 JAK-STAT 通路与 MESP1 转录调控之间的联系,从而拓展了我们对中胚层和心脏发育的认识。
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来源期刊
European journal of cell biology
European journal of cell biology 生物-细胞生物学
CiteScore
7.30
自引率
1.50%
发文量
80
审稿时长
38 days
期刊介绍: The European Journal of Cell Biology, a journal of experimental cell investigation, publishes reviews, original articles and short communications on the structure, function and macromolecular organization of cells and cell components. Contributions focusing on cellular dynamics, motility and differentiation, particularly if related to cellular biochemistry, molecular biology, immunology, neurobiology, and developmental biology are encouraged. Manuscripts describing significant technical advances are also welcome. In addition, papers dealing with biomedical issues of general interest to cell biologists will be published. Contributions addressing cell biological problems in prokaryotes and plants are also welcome.
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