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Combinatorial binding predicts spatio-temporal cis-regulatory activity.组合结合预测时空顺式调控活性。
Nature. 2009 Nov 5;462(7269):65-70. doi: 10.1038/nature08531.
2
Hox specificity unique roles for cofactors and collaborators.同源框基因(Hox)特异性:辅助因子和协同因子的独特作用。
Curr Top Dev Biol. 2009;88:63-101. doi: 10.1016/S0070-2153(09)88003-4.
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Multifactorial regulation of a hox target gene.一个Hox靶基因的多因素调控
PLoS Genet. 2009 Mar;5(3):e1000412. doi: 10.1371/journal.pgen.1000412. Epub 2009 Mar 13.
4
A systematic analysis of Tinman function reveals Eya and JAK-STAT signaling as essential regulators of muscle development.对Tinman功能的系统分析表明,Eya和JAK-STAT信号传导是肌肉发育的重要调节因子。
Dev Cell. 2009 Feb;16(2):280-91. doi: 10.1016/j.devcel.2009.01.006.
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Integration of Insulin receptor/Foxo signaling and dMyc activity during muscle growth regulates body size in Drosophila.胰岛素受体/Foxo信号与dMyc活性在肌肉生长过程中的整合调控果蝇的体型。
Development. 2009 Mar;136(6):983-93. doi: 10.1242/dev.027466. Epub 2009 Feb 11.
6
Shaping segments: Hox gene function in the genomic age.塑造节段:基因组时代的Hox基因功能
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The PDZ protein Canoe regulates the asymmetric division of Drosophila neuroblasts and muscle progenitors.PDZ蛋白Canoe调控果蝇神经母细胞和肌肉祖细胞的不对称分裂。
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10
Control of multidendritic neuron differentiation in Drosophila: the role of Collier.果蝇中多树突神经元分化的调控:Collier的作用。
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果蝇胚胎中 Hox 蛋白对肌肉多样性的多步控制。

Multi-step control of muscle diversity by Hox proteins in the Drosophila embryo.

机构信息

Centre de Biologie du Développement, UMR 5547 CNRS/UPS, IFR 109 Institut d'Exploration Fonctionnelle des Génomes, 31062 Toulouse cedex 9, France.

出版信息

Development. 2010 Feb;137(3):457-66. doi: 10.1242/dev.045286. Epub 2010 Jan 7.

DOI:10.1242/dev.045286
PMID:20056681
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2858909/
Abstract

Hox transcription factors control many aspects of animal morphogenetic diversity. The segmental pattern of Drosophila larval muscles shows stereotyped variations along the anteroposterior body axis. Each muscle is seeded by a founder cell and the properties specific to each muscle reflect the expression by each founder cell of a specific combination of 'identity' transcription factors. Founder cells originate from asymmetric division of progenitor cells specified at fixed positions. Using the dorsal DA3 muscle lineage as a paradigm, we show here that Hox proteins play a decisive role in establishing the pattern of Drosophila muscles by controlling the expression of identity transcription factors, such as Nautilus and Collier (Col), at the progenitor stage. High-resolution analysis, using newly designed intron-containing reporter genes to detect primary transcripts, shows that the progenitor stage is the key step at which segment-specific information carried by Hox proteins is superimposed on intrasegmental positional information. Differential control of col transcription by the Antennapedia and Ultrabithorax/Abdominal-A paralogs is mediated by separate cis-regulatory modules (CRMs). Hox proteins also control the segment-specific number of myoblasts allocated to the DA3 muscle. We conclude that Hox proteins both regulate and contribute to the combinatorial code of transcription factors that specify muscle identity and act at several steps during the muscle-specification process to generate muscle diversity.

摘要

同源盒转录因子控制着动物形态发生多样性的许多方面。果蝇幼虫肌肉的节段模式沿体轴表现出刻板的变化。每块肌肉都是由一个创始细胞产生的,每个创始细胞表达特定的“身份”转录因子组合,决定了肌肉的特性。创始细胞起源于在固定位置指定的前体细胞的不对称分裂。我们使用背侧 DA3 肌肉谱系作为范例,表明 Hox 蛋白通过在祖细胞阶段控制身份转录因子(如 Nautilus 和 Collier,简称 Col)的表达,在建立果蝇肌肉模式方面发挥决定性作用。使用新设计的包含内含子的报告基因进行高分辨率分析,显示祖细胞阶段是 Hox 蛋白携带的节段特异性信息叠加在节内位置信息的关键步骤。触角足和超臀胸节/腹部 A 等位基因对 col 转录的差异控制是由独立的顺式调控模块(CRMs)介导的。Hox 蛋白还控制分配给 DA3 肌肉的肌母细胞的节段特异性数量。我们得出结论,Hox 蛋白既调节又有助于确定肌肉身份的转录因子的组合代码,并在肌肉特异性过程的几个步骤中发挥作用,以产生肌肉多样性。