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首页> 外文期刊>Developmental biology >Xebf3 is a regulator of neuronal differentiation during primaryneurogenesis in Xenopus
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Xebf3 is a regulator of neuronal differentiation during primaryneurogenesis in Xenopus

机译:Xebf3是非洲爪蟾原代神经发生过程中神经元分化的调节剂。

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During primary neurogenesis in Xenopus, a cascade of helix-loop-helix (HLH) transcription factors regulates neuronal determination and differentiation. While XNeuroD functions at a late step in this cascade to regulate neuronal differentiation, the factors that carry out terminal differentiation are still unknown. We have isolated a new Xenopus member of the Ebf/Olf-1 family of HLH transcription factors, Xebf3, and provide evidence that, during primary neurogenesis, it regulates neuronal differentiation downstream of XNeuroD. In developing Xenopus embryos, Xebf3 is turned on in the three stripes of primary neurons at stage 15.5, after XNeuroD. In vitro, XEBF3 binds the EBF/OLF-1 binding site and functions as a transcriptional activator. When overexpressed, Xebf3 is able to induce ectopic neurons at neural plate stages and directly convert ectodermal cells into neurons in animal cap explants. Expression of Xebf3 can be activated by XNeuroD both in whole embryos and in animal caps, indicating that this new HLH factor might be regulated by XNeuroD. Furthermore, in animal caps, XNeuroD can activate Xebf3 in the absence of protein synthesis, suggesting that, in vitro, this regulation is direct. Similar to XNeuroD, but unlike Xebf2/Xcoe2, Xebf3 expression and function are insensitive to Delta/Notch-mediated lateral inhibition. In summary, we conclude that Xebf3 functions downstream of XNeuroD and is a regulator of neuronal differentiation in Xenopus.
机译:在非洲爪蟾的原代神经发生过程中,一系列的螺旋-环-螺旋(HLH)转录因子调节神经元的确定和分化。虽然XNeuroD在此级联反应的后期起作用以调节神经元分化,但进行终末分化的因素仍然未知。我们已经分离出HLH转录因子Ebf / Olf-1家族的新非洲爪蟾成员Xebf3,并提供证据表明,在原代神经发生过程中,它调节了XNeuroD下游的神经元分化。在发育中的非洲爪蟾胚胎中,在XNeuroD之后的15.5阶段,Xebf3在原代神经元的三个条纹中打开。在体外,XEBF3结合EBF / OLF-1结合位点并起转录激活剂的作用。当过表达时,Xebf3能够在神经板阶段诱导异位神经元,并将外胚层细胞直接转化为动物帽外植体中的神经元。 Xebf3的表达可以通过XNeuroD在整个胚胎和动物帽中被激活,这表明这种新的HLH因子可能受到XNeuroD的调控。此外,在动物帽中,XNeuroD可以在没有蛋白质合成的情况下激活Xebf3,这表明在体外,这种调节是直接的。与XNeuroD相似,但与Xebf2 / Xcoe2不同,Xebf3的表达和功能对Delta / Notch介导的侧向抑制不敏感。总之,我们得出的结论是,Xebf3在XNeuroD的下游起作用,并且是非洲爪蟾中神经元分化的调节剂。

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