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首页> 外文期刊>Cell cycle >Nitric oxide coordinates cell proliferation and cell movements during early development of Xenopus.
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Nitric oxide coordinates cell proliferation and cell movements during early development of Xenopus.

机译:在Xenopus早期发育期间,一氧化氮坐标细胞增殖和细胞运动。

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摘要

The establishment of a vertebrate body plan during embryogenesis is achieved through precise coordination of cell proliferation and morphogenetic cell movements. Here we show that nitric oxide (NO) suppresses cell division and facilitates cell movements during early development of Xenopus, such that inhibition of NO synthase (NOS) increases proliferation in the neuroectoderm and suppresses convergent extension in the axial mesoderm and neuroectoderm. NO controls cell division and cell movement through two separate signaling pathways. Both rely on RhoA-ROCK signaling but can be distinguished by the involvement of either guanylate cyclase or the planar cell polarity regulator Dishevelled. Through the cGMP-dependent pathway, NO suppresses cell division by negatively regulating RhoA and controlling the nuclear distribution of ROCK and p21WAF1. Through the cGMP-independent pathway, NO facilitates cell movement by regulating the intracellular distribution and level of Dishevelled and the activity of RhoA, thereby controlling the activity of ROCK and regulating actin cytoskeleton remodeling and cell polarization. Concurrent control by NO helps ensure that the crucial processes of cell proliferation and morphogenetic movements are coordinated during early development.
机译:通过精确配位细胞增殖和形态发生细胞运动来实现胚胎发生期间的脊椎动物体规划。在这里,我们表明一氧化氮(NO)抑制细胞分裂并促进在XENOPUS的早期发育期间的细胞运动,使得NO合酶(NOS)的抑制增加了神经分区中的增殖,并抑制了轴向中胚层和神经外胚层中的会聚延伸。无控制细胞分裂和细胞运动通过两个单独的信号通路。依靠RhoA岩石信号传导,但可以通过致醋酸环酸盐环化酶或平面细胞极性调节器的涉及来区分。通过CGMP依赖性途径,通过对ROOA产生负面调节并控制岩石和P21WAF1的核分布,不抑制细胞分裂。通过CGMP无关的途径,通过调节细胞内分布和乳清露活性的细胞内分布和水平,无促进细胞运动,从而控制岩石的活性和调节肌动蛋白细胞骨架改造和细胞偏振的活性。并发控制不会有助于确保在早期发育期间协调细胞增殖和形态发生运动的关键过程。

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