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首页> 外文期刊>PLoS One >Genome-Wide Analysis of the Binding of the Hox Protein Ultrabithorax and the Hox Cofactor Homothorax in Drosophila
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Genome-Wide Analysis of the Binding of the Hox Protein Ultrabithorax and the Hox Cofactor Homothorax in Drosophila

机译:全基因组分析果蝇中的Hox蛋白Ultrabithorax和Hox辅因子Homothorax的结合

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Hox genes encode a family of transcription factors that are key developmental regulators with a highly conserved role in specifying segmental diversity along the metazoan body axis. Although they have been shown to regulate a wide variety of downstream processes, direct transcriptional targets have been difficult to identify and this has been a major obstacle to our understanding of Hox gene function. We report the identification of genome-wide binding sites for the Hox protein Ultrabithorax (Ubx) using a YFP-tagged Drosophila protein-trap line together with chromatin immunoprecipitation and microarray analysis. We identify 1,147 genes bound by Ubx at high confidence in chromatin from the haltere imaginal disc, a prominent site of Ubx function where it specifies haltere versus wing development. The functional relevance of these genes is supported by their overlap with genes differentially expressed between wing and haltere imaginal discs. The Ubx-bound gene set is highly enriched in genes involved in developmental processes and contains both high-level regulators as well as genes involved in more basic cellular functions. Several signalling pathways are highly enriched in the Ubx target gene set and our analysis supports the view that Hox genes regulate many levels of developmental pathways and have targets distributed throughout the gene network. We also performed genome-wide analysis of the binding sites for the Hox cofactor Homothorax (Hth), revealing a striking similarity with the Ubx binding profile. We suggest that these binding profiles may be strongly influenced by chromatin accessibility and provide evidence of a link between Ubx/Hth binding and chromatin state at genes regulated by Polycomb silencing. Overall, we define a set of direct Ubx targets in the haltere imaginal disc and suggest that chromatin accessibility has important implications for Hox target selection and for transcription factor binding in general.
机译:Hox基因编码的转录因子家族是关键的发育调节因子,在指定后生动物体轴的节段多样性方面具有高度保守的作用。尽管已显示它们可调节多种下游过程,但直接转录靶标很难鉴定,这已成为我们对Hox基因功能了解的主要障碍。我们报告使用YFP标记的果蝇蛋白质陷阱线与染色质免疫沉淀和微阵列分析一起鉴定Hox蛋白超bithorax(Ubx)的全基因组结合位点。我们从笼头假想盘中确定了染色质的高置信度,从而确定了受Ubx约束的1147个基因,Ubx功能的一个显着部位是Ubx功能,它指定了笼头与机翼的发育。这些基因与机翼和三角翼假想盘之间差异表达的基因重叠,从而支持了这些基因的功能相关性。与Ubx结合的基因集高度富集涉及发育过程的基因,既包含高级调节剂,又包含涉及更基本细胞功能的基因。 Ubx目标基因集中高度丰富了一些信号传导途径,我们的分析支持以下观点:Hox基因调节许多水平的发育途径,并且目标分布在整个基因网络中。我们还对Hox辅因子Homothorax(Hth)的结合位点进行了全基因组分析,揭示了与Ubx结合谱的惊人相似之处。我们建议这些绑定配置文件可能会受到染色质可及性的强烈影响,并提供证据表明Ubx / Hth结合与由Polycomb沉默调控的基因的染色质状态之间存在联系。总的来说,我们在the形影像盘中定义了一组直接的Ubx靶标,并提出染色质可及性对于Hox靶标选择和一般而言与转录因子结合具有重要意义。

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