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Zebrafish Noxa promotes mitosis in early embryonic development and regulates apoptosis in subsequent embryogenesis

机译:斑马鱼Noxa促进早期胚胎发育中的有丝分裂并在随后的胚胎发生中调节细胞凋亡

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摘要

Noxa functions in apoptosis and immune system of vertebrates, but its activities in embryo development remain unclear. In this study, we have studied the role of zebrafish Noxa (zNoxa) by using zNoxa-specifc morpholino knockdown and overexpression approaches in developing zebrafish embryos. Expression pattern analysis indicates that zNoxa transcript is of maternal origin, which displays a uniform distribution in early embryonic development until shield stage, and the zygote zNoxa transcription is initiated from this stage and mainly localized in YSL of the embryos. The zNoxa expression alterations result in strong embryonic development defects, demonstrating that zNoxa regulates apoptosis from 75% epiboly stage of development onward, in which zNoxa firstly induces the expression of zBik, and then cooperates with zBik to regulate apoptosis. Moreover, zNoxa knockdown also causes a reduction in number of mitotic cells before 8 h.p.f., suggesting that zNoxa also promotes mitosis before 75% epiboly stage. The effect of zNoxa on mitosis is mediated by zWnt4b in early embryos, whereas zMcl1a and zMcl1b suppress the ability of zNoxa to regulate mitosis and apoptosis at different developmental stages. In addition, mammalian mouse Noxa (mNoxa) mRNA was demonstrated to rescue the arrest of mitosis when zNoxa was knocked down, suggesting that mouse and zebrafish Noxa might have similar dual functions. Therefore, the current findings indicate that Noxa is a novel regulator of early mitosis before 75% epiboly stage when it translates into a key mediator of apoptosis in subsequent embryogenesis.
机译:Noxa在脊椎动物的细胞凋亡和免疫系统中起作用,但其在胚胎发育中的活性仍不清楚。在这项研究中,我们已经研究了斑马鱼Noxa(zNoxa)的作用,方法是使用zNoxa特异的吗啉代敲除和过度表达方法开发斑马鱼胚胎。表达模式分析表明zNoxa转录本是母本来源,在早期胚胎发育直至屏蔽阶段均显示均匀分布,合子zNoxa转录从该阶段开始,主要位于胚胎的YSL中。 zNoxa表达改变导致强烈的胚胎发育缺陷,表明zNoxa从75%的表皮发育阶段开始调节细胞凋亡,其中zNoxa首先诱导zBik表达,然后与zBik协同调节细胞凋亡。此外,zNoxa的敲除还导致8 h.p.f.之前有丝分裂细胞的数量减少,这表明zNoxa在表皮外生期达到75%之前也促进有丝分裂。 zNoxa对有丝分裂的影响由zWnt4b在早期胚胎中介导,而zMcl1a和zMcl1b抑制zNoxa在不同发育阶段调节有丝分裂和凋亡的能力。此外,哺乳动物小鼠Noxa(mNoxa)mRNA被证实可在击倒zNoxa时挽救有丝分裂的停止,这表明小鼠和斑马鱼Noxa可能具有相似的双重功能。因此,目前的研究结果表明,Noxa是一种新的早期有丝分裂调节剂,在表皮期达到75%之前可转化为后续胚胎发生过程中凋亡的关键介体。

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