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首页> 外文期刊>Small GTPases >MicroRNAs as key regulators of GTPase-mediated apical actin reorganization in multiciliated epithelia
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MicroRNAs as key regulators of GTPase-mediated apical actin reorganization in multiciliated epithelia

机译:MicroRNA作为多纤毛上皮细胞中GTPase介导的根尖肌动蛋白重组的关键调控因子

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摘要

Multiciliated cells (MCCs), which are present in specialized vertebrate tissues such as mucociliary epithelia, project hundreds of motile cilia from their apical membrane. Coordinated ciliary beating in MCCs contributes to fluid propulsion in several biological processes. In a previous work, we demonstrated that microRNAs of the miR-34/449 family act as new conserved regulators of MCC differentiation by specifically repressing cell cycle genes and the Notch pathway. Recently, we have shown that miR-34/449 also modulate small GTPase pathways to promote, in a later stage of differentiation, the assembly of the apical actin network, a prerequisite for proper anchoring of centrioles-derived neo-synthesized basal bodies. We characterized several miR-34/449targets related to small GTPase pathways including R-Ras, which represents a key and conserved regulator during MCC differentiation. Direct RRAS repression by miR-34/449 is necessary for apical actin meshwork assembly, notably by allowing the apical relocalization of the actin binding protein Fflamln-A near basal bodies. Our studies establish miR-34/449 as central players that orchestrate several steps of MCC differentiation program by regulating distinct signaling pathways.
机译:存在于特殊脊椎动物组织(如粘膜纤毛上皮)中的多纤毛细胞(MCC)从其顶膜投射出数百个活动纤毛。 MCC中的纤毛协调性跳动在几种生物学过程中有助于液体的推进。在先前的工作中,我们证明了miR-34 / 449家族的microRNA通过特异性抑制细胞周期基因和Notch途径,作为MCC分化的新保守调节子。最近,我们已经表明,miR-34 / 449还可以调节小GTPase途径,以在分化的后期促进根尖肌动蛋白网络的组装,这是正确锚定来自中心粒的新合成基体的前提。我们表征了几个与小GTPase途径相关的miR-34 / 449靶标,包括R-Ras,它代表了MCC分化过程中的关键且保守的调节子。对于顶端肌动蛋白网状装配,必须通过miR-34 / 449直接抑制RRAS,特别是通过使肌动蛋白结合蛋白Fflamln-A在基体附近进行顶端重新定位。我们的研究将miR-34 / 449定位为通过调节独特的信号通路来协调MCC分化程序的几个步骤的中心参与者。

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