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首页> 外文期刊>Development >Barhl2 maintains T cell factors as repressors and thereby switches off the Wnt/beta-Catenin response driving Spemann organizer formation
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Barhl2 maintains T cell factors as repressors and thereby switches off the Wnt/beta-Catenin response driving Spemann organizer formation

机译:Barhl2将T细胞因子维持作为阻遏物,从而切断Wnt /β-catenin响应驾驶Spemann组织者的形成

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摘要

A hallmark of Wnt/beta-Catenin signaling is the extreme diversity of its transcriptional response, which varies depending on the cell and developmental context. What controls this diversity is poorly understood. In all cases, the switch from transcriptional repression to activation depends on a nuclear increase in beta-Catenin, which detaches the transcription factor T cell factor 7 like 1 (Tcf711) bound to Groucho (Gro) transcriptional co-repressors from its DNA-binding sites and transiently converts Tcf7/Lymphoid enhancer binding factor 1 (Lef1) into a transcriptional activator. One of the earliest and evolutionarily conserved functions of Wnt/beta-Catenin signaling is the induction of the blastopore lip organizer. Here, we demonstrate that the evolutionarily conserved BarH-like homeobox-2 (Barhl2) protein stabilizes the Tcf7l1-Gro complex and maintains the repressed expression of Tcf target genes by a mechanism that depends on histone deacetylase 1 (Hdac-1) activity. In this way, Barhl2 switches off the Wnt/beta-Catenin-dependent early transcriptional response, thereby limiting the formation of the organizer in time and/or space. This study reveals a novel nuclear inhibitory mechanism of Wnt/Tcf signaling that switches off organizer fate determination.
机译:Wnt / Beta-catenin信号传导的标志是其转录响应的极端多样性,这取决于细胞和发育背景。这种多样性的控制是什么难以理解的。在所有情况下,从转录镇压到激活的切换取决于β-连环蛋白的核增加,它从其DNA结合中脱离Groucho(TCF711)的转录因子T细胞因子7如1(TCF711)网站和瞬时将TCF7 /淋巴增强子结合因子1(LEF1)转化为转录活化剂。 WNT / Beta-catenin信号传导的最早和进化的保守功能之一是囊泡唇部组织器的诱导。这里,我们证明了进化保守的Barh样Homeobox-2(BarHH12)蛋白稳定了TCF7L1-GRO络合物,并通过取决于组蛋白脱乙酰酶1(HDAC-1)活性的机制来保持TCF靶基因的抑制表达。以这种方式,BarHl2关闭WNT /β-连环蛋白依赖性早期转录响应,从而限制了组织者的时间和/或空间。本研究显示了WNT / TCF信号传导的新型核抑制机制,关闭组织者命运测定。

著录项

  • 来源
    《Development》 |2019年第10期|共16页
  • 作者单位

    Univ Paris Sud PSL Res Univ Ctr Univ Inst Curie Res Div CNRS UMR 3347 INSERM U102 Batiment 110;

    Univ Paris Sud PSL Res Univ Ctr Univ Inst Curie Res Div CNRS UMR 3347 INSERM U102 Batiment 110;

    Univ Paris Sud PSL Res Univ Ctr Univ Inst Curie Res Div CNRS UMR 3347 INSERM U102 Batiment 110;

    Ecole Normale Super Inst Biol ENS IBENS S1 7 CNRS 8197 INSERM U1024 46 Rue Ulm F-75005 Paris;

    Univ Paris Saclay Univ Paris Sud CNRS Paris Saclay Inst Neurosci F-91405 Orsay France;

    PSL Res Univ CNRS UMR3664 Inst Curie Equipe Labellisee Ligue Canc F-75005 Paris France;

    Univ Paris Saclay Univ Paris Sud CNRS Paris Saclay Inst Neurosci F-91405 Orsay France;

    Univ Paris Sud PSL Res Univ Ctr Univ Inst Curie Res Div CNRS UMR 3347 INSERM U102 Batiment 110;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 人体形态学;
  • 关键词

    Organizer; Groucho/Tle; Tcf/Lef; Barhl2; Hdac; Stem cells; Wnt; Pluripotency; Transcription;

    机译:组织者;Groucho / tle;TCF / LEF;BARHL2;HDAC;干细胞;WNT;多能性;转录;

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