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En2、Pax2/5 和 Tcf-4 转录因子在调控非洲爪蟾脑的模式形成中合作。

En2, Pax2/5 and Tcf-4 transcription factors cooperate in patterning the Xenopus brain.

机构信息

Zoological Institute, Cell and Developmental Biology, Karlsruhe Institute of Technology, Kaiserstrasse 12, 76131 Karlsruhe, Germany.

出版信息

Dev Biol. 2010 Apr 15;340(2):318-28. doi: 10.1016/j.ydbio.2010.02.011. Epub 2010 Feb 18.

Abstract

Among Xenopus Lef/Tcfs, XTcf-4 has an outstanding role. In early development it is located exclusively in the midbrain where it is essential for midbrain and isthmus development. In order to identify transcription factors responsible for the restriction of XTcf-4 expression we isolated a 3.8kb fragment of the XTcf-4 promoter. We found that this promoter fragment is sufficient to mimic endogenous XTcf-4 expression in the midbrain. Characterization of putative binding sites for en2 and pax2/5 revealed that en2, but not pax2/5 directly represses XTcf-4 promoter activity. Gain-of-function experiments in Xenopus embryos confirmed this en2-mediated repression. Loss-of-function experiments demonstrate that both en2 and pax2/5 are essential for endogenous XTcf-4 expression. The primary effect of pax2/5 depletion thereby appears to be a reduced en2 expression at neurula stages. Because en2 can compensate for the depletion of pax2/5, we assume a hierarchical regulation of gene expression in the midbrain/isthmus region with pax2/5 acting upstream of en2. Furthermore, since the XTcf-4 expression domain does not overlap with the expression domains of the isthmus marker genes en2 and pax2/5, we conclude that the knock-down of en2 and pax2/5 results in a downregulation of a paracrine growth factor regulating XTcf-4 expression. We found that the growth factor for this non-cell-autonomous effect of en2 and pax2/5 is wnt-1 acting on the -1437 Lef/Tcf binding site on the XTcf-4 promoter. We provide evidence that the main nuclear wnt transducer for the autoregulation of XTcf-4 is XTcf-1.

摘要

在非洲爪蟾 Lef/Tcf 中,XTcf-4 具有突出的作用。在早期发育过程中,它仅位于中脑中,对于中脑和脑桥的发育是必不可少的。为了鉴定负责限制 XTcf-4 表达的转录因子,我们分离了 XTcf-4 启动子的 3.8kb 片段。我们发现,这个启动子片段足以模拟中脑中内源性 XTcf-4 的表达。对 en2 和 pax2/5 的潜在结合位点的特征分析表明,en2 而非 pax2/5 直接抑制 XTcf-4 启动子活性。在非洲爪蟾胚胎中的功能获得实验证实了这种 en2 介导的抑制作用。功能丧失实验表明,en2 和 pax2/5 对于内源性 XTcf-4 的表达都是必不可少的。因此,pax2/5 耗竭的主要影响似乎是在神经胚阶段降低 en2 的表达。由于 en2 可以补偿 pax2/5 的耗竭,我们假设中脑/脑桥区域的基因表达受到分级调控,pax2/5 在上游作用于 en2。此外,由于 XTcf-4 表达域与脑桥标记基因 en2 和 pax2/5 的表达域不重叠,我们得出结论,en2 和 pax2/5 的敲低导致调节 XTcf-4 表达的旁分泌生长因子的下调。我们发现,en2 和 pax2/5 的这种非细胞自主作用的生长因子是 wnt-1,它作用于 XTcf-4 启动子上的-1437 Lef/Tcf 结合位点。我们提供的证据表明,XTcf-4 自身调控的主要核 wnt 转导物是 XTcf-1。

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