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Distinct Contributions of Conserved Modules to Runt Transcription Factor Activity

机译:保守模块对矮子转录因子活性的不同贡献

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Runx proteins play vital roles in regulating transcription in numerous developmental pathways throughout the animal kingdom. Two Runx protein hallmarks are the DNA-binding Runt domain and a C-terminal VWRPY motif that mediates interaction with TLE/Gro corepressor proteins. A phylogenetic analysis of Runt, the founding Runx family member, identifies four distinct regions C-terminal to the Runt domain that are conserved in Drosophila and other insects. We used a series of previously described ectopic expression assays to investigate the functions of these different conserved regions in regulating gene expression during embryogenesis and in controlling axonal projections in the developing eye. The results indicate each conserved region is required for a different subset of activities and identify distinct regions that participate in the transcriptional activation and repression of the segmentation gene sloppy-paired-1 ( slp1 ). Interestingly, the C-terminal VWRPY-containing region is not required for repression but instead plays a role in slp1 activation. Genetic experiments indicating that Groucho ( Gro ) does not participate in slp1 regulation further suggest that Runt's conserved C-terminus interacts with other factors to promote transcriptional activation. These results provide a foundation for further studies on the molecular interactions that contribute to the context-dependent properties of Runx proteins as developmental regulators.
机译:Runx蛋白在整个动物界的众多发育途径中调节转录起着至关重要的作用。两个Runx蛋白的标志是与DNA结合的Runt结构域和一个介导与TLE / Gro核心降压蛋白相互作用的C末端VWRPY基序。对Runt家族的创始成员Runt进行的系统发育分析确定了在Runt域C端的四个不同区域,这些区域在果蝇和其他昆虫中均保守。我们使用了一系列先前描述的异位表达测定法来研究这些不同的保守区在胚胎发生过程中调控基因表达和控制发育中的轴突投影中的功能。结果表明,每个保守区对于不同的活动子​​集都是必需的,并且识别参与分段基因sloppypaired-1(slp1)的转录激活和抑制的不同区域。有趣的是,压制不需要C端含VWRPY的区域,而是在slp1激活中起作用。遗传实验表明,Groucho(Gro)不参与slp1调控,这进一步表明Runt保守的C末端与其他因子相互作用以促进转录激活。这些结果为进一步研究分子相互作用提供了基础,这些分子相互作用有助于Runx蛋白作为发育调节因子的上下文相关特性。

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