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MiR218 Modulates Wnt Signaling in Mouse Cardiac Stem Cells by Promoting Proliferation and Inhibiting Differentiation through a Positive Feedback Loop

机译:MiR218通过促进增殖和通过正反馈环抑制分化来调节小鼠心脏干细胞中的Wnt信号传导

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摘要

MiRNA expression was determined in both proliferating and differentiated cardiac stem cells (CSCs) through a comprehensive miRNA microarray analysis. We selected miR218 for functional follow-up studies to examine its significance in CSCs. First, we observed that the expression of miR218 was altered in CSCs during differentiation into cardiomyocytes, and transfection of an miR218 mimic or miR218 inhibitor affected the myocardial differentiation of CSCs. Furthermore, we observed that a negative regulator of Wnt signaling, sFRP2, was a direct target of miR218, and the protein levels of sFRP2 were increased in cells transfected with the synthetic miR218 inhibitor. In contrast, transfection with the miR218 mimic decreased the expression of sFRP2 and potentiated Wnt signaling. The subsequent down-regulation of sFRP2 by shRNA potentiated Wnt signaling, contributing to a gene expression program that is important for CSC proliferation and cardiac differentiation. Specifically, canonical Wnt signaling induced miR218 transcription. Thus, miR218 and Wnt signaling were coupled through a feed-forward positive feedback loop, forming a biological regulatory circuit. Together, these results provide the first evidence that miR218 plays an important role in CSC proliferation and differentiation through the canonical Wnt signaling pathway.
机译:通过全面的miRNA微阵列分析,可以确定增殖和分化的心脏干细胞(CSC)中的miRNA表达。我们选择miR218进行功能随访研究,以检查其在CSC中的重要性。首先,我们观察到在分化为心肌细胞的过程中,miR218的表达在CSC中发生了变化,miR218模拟物或miR218抑制剂的转染影响了CSC的心肌分化。此外,我们观察到Wnt信号的负调控因子sFRP2是miR218的直接靶标,并且在用合成miR218抑制剂转染的细胞中sFRP2的蛋白水平升高。相反,用miR218模拟物转染会降低sFRP2的表达并增强Wnt信号传导。后来,shRNA增强了Wnt信号传导,从而下调了sFRP2,从而促进了对CSC增殖和心脏分化至关重要的基因表达程序。具体而言,规范的Wnt信号传导诱导miR218转录。因此,miR218和Wnt信号通过前馈正反馈回路耦合,形成生物调节电路。在一起,这些结果提供了第一个证据,证明miR218通过经典Wnt信号通路在CSC增殖和分化中起重要作用。

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