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在非洲爪蟾胚胎中,XSmad2直接激活激活素诱导的背侧中胚层基因XFKH1。

XSmad2 directly activates the activin-inducible, dorsal mesoderm gene XFKH1 in Xenopus embryos.

作者信息

Howell M, Hill C S

机构信息

Ludwig Institute for Cancer Research, 91 Riding House Street, London W1P 8BT, UK.

出版信息

EMBO J. 1997 Dec 15;16(24):7411-21. doi: 10.1093/emboj/16.24.7411.

Abstract

Transforming growth factor (TGF)-beta family members play a central role in mesoderm induction during early embryogenesis in Xenopus. Although a number of target genes induced as an immediate-early response to activin-like members of the family have been described, little is known about the molecular mechanisms involved. Our systematic analysis of the activin induction of the target gene XFKH1 reveals two regions that mediate activin-responsive transcription: one, in the first intron, is targeted directly by the activin-signalling pathway; the other, in the 5' flanking sequences, responds to activin indirectly, possibly being required for maintenance of gene expression. We demonstrate that a 107 bp region of the XFKH1 first intron acts as an enhancer and confers activin inducibility onto a minimal uninducible promoter in the absence of new protein synthesis. It bears little sequence similarity to other activin responsive sequences. We further demonstrate that overexpression of a constitutively active derivative of Xenopus Smad2 (XSmad2), which has been implicated as a component of the activin signalling pathway, is sufficient for direct activation of transcription via this enhancer. Moreover, we show that XSmad2 acts indirectly on the proximal promoter element induced by activin via an indirect mechanism. These results establish the XFKH1 intron enhancer as a direct nuclear target of the activin signalling pathway in Xenopus embryos, and provide strong new evidence that XSmad2 is a transducer of activin signals.

摘要

转化生长因子(TGF)-β家族成员在非洲爪蟾早期胚胎发育过程中的中胚层诱导中起核心作用。尽管已经描述了许多作为对该家族激活素样成员的即时早期反应而诱导的靶基因,但对于其中涉及的分子机制知之甚少。我们对靶基因XFKH1的激活素诱导进行的系统分析揭示了两个介导激活素反应性转录的区域:一个在第一个内含子中,直接被激活素信号通路靶向;另一个在5'侧翼序列中,间接响应激活素,可能是维持基因表达所必需的。我们证明,XFKH1第一个内含子的一个107 bp区域作为增强子,在没有新蛋白质合成的情况下赋予最小的非诱导性启动子激活素诱导性。它与其他激活素反应序列几乎没有序列相似性。我们进一步证明,非洲爪蟾Smad2(XSmad2)的组成型活性衍生物的过表达足以通过该增强子直接激活转录,XSmad2已被认为是激活素信号通路的一个组成部分。此外,我们表明XSmad2通过间接机制间接作用于激活素诱导的近端启动子元件。这些结果确立了XFKH1内含子增强子作为非洲爪蟾胚胎中激活素信号通路的直接核靶点,并提供了强有力的新证据表明XSmad2是激活素信号的转导者。

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