Elongation of the developing spinal cord is driven by Oct4-type transcription factor-mediated regulation of retinoic acid signaling in zebrafish embryos

IF 2 3区 生物学 Q2 ANATOMY & MORPHOLOGY
Tatsuya Yuikawa, Takehisa Sato, Masaaki Ikeda, Momo Tsuruoka, Kaede Yasuda, Yuto Sato, Kouhei Nasu, Kyo Yamasu
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引用次数: 0

Abstract

Background

Elongation of the spinal cord is dependent on neural development from neuromesodermal progenitors in the tail bud. We previously showed the involvement of the Oct4-type gene, pou5f3, in this process in zebrafish mainly by dominant-interference gene induction, but, to compensate for the limitation of this transgene approach, mutant analysis was indispensable. pou5f3 involvement in the signaling pathways was another unsolved question.

Results

We examined the phenotypes of pou5f3 mutants and the effects of Pou5f3 activation by the tamoxifen-ERT2 system in the posterior neural tube, together confirming the involvement of pou5f3. The reporter assays using P19 cells implicated tail bud-related transcription factors in pou5f3 expression. Regulation of tail bud development by retinoic acid (RA) signaling was confirmed by treatment of embryos with RA and the synthesis inhibitor, and in vitro reporter assays further showed that RA signaling regulated pou5f3 expression. Importantly, the expression of the RA degradation enzyme gene, cyp26a1, was down-regulated in embryos with disrupted pou5f3 activity.

Conclusions

The involvement of pou5f3 in spinal cord extension was supported by using mutants and the gain-of-function approach. Our findings further suggest that pou5f3 regulates the RA level, contributing to neurogenesis in the posterior neural tube.

Abstract Image

发育中脊髓的延伸是由Oct4型转录因子介导的斑马鱼胚胎中维甲酸信号传导的调节驱动的。
背景:脊髓的延伸取决于神经中胚层祖细胞在尾芽中的神经发育。我们之前表明,Oct4型基因pou5f3主要通过显性干扰基因诱导参与斑马鱼的这一过程,但为了弥补这种转基因方法的局限性,突变分析是必不可少的。pou5f3参与信号通路是另一个尚未解决的问题。结果:我们检测了pou5f3突变体的表型以及他莫昔芬-ET2系统在后神经管中激活pou5f3的影响,共同证实了pou5 f3的参与。使用P19细胞的报告基因分析表明,pou5f3表达中存在与尾芽相关的转录因子。通过用RA和合成抑制剂处理胚胎证实了维甲酸(RA)信号对尾芽发育的调节,体外报告基因分析进一步表明RA信号调节pou5f3的表达。重要的是,在pou5f3活性受损的胚胎中,RA降解酶基因cyp26a1的表达下调。结论:pou5f3参与脊髓延伸是通过使用突变体和功能获得方法来支持的。我们的研究结果进一步表明,pou5f3调节RA水平,有助于后神经管的神经发生。
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来源期刊
Developmental Dynamics
Developmental Dynamics 生物-发育生物学
CiteScore
5.10
自引率
8.00%
发文量
116
审稿时长
3-8 weeks
期刊介绍: Developmental Dynamics, is an official publication of the American Association for Anatomy. This peer reviewed journal provides an international forum for publishing novel discoveries, using any model system, that advances our understanding of development, morphology, form and function, evolution, disease, stem cells, repair and regeneration.
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