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Dual transcriptional activator and repressor roles of TBX20 regulate adult cardiac structure and function

机译:TBX20的双重转录激活因子和阻遏因子调节成人心脏的结构和功能

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摘要

The ongoing requirement in adult heart for transcription factors with key roles in cardiac development is not well understood. We recently demonstrated that TBX20, a transcriptional regulator required for cardiac development, has key roles in the maintenance of functional and structural phenotypes in adult mouse heart. Conditional ablation of Tbx20 in adult cardiomyocytes leads to a rapid onset and progression of heart failure, with prominent conduction and contractility phenotypes that lead to death. Here we describe a more comprehensive molecular characterization of the functions of TBX20 in adult mouse heart. Coupling genome-wide chromatin immunoprecipitation and transcriptome analyses (RNA-Seq), we identified a subset of genes that change expression in Tbx20 adult cardiomyocyte-specific knockout hearts which are direct downstream targets of TBX20. This analysis revealed a dual role for TBX20 as both a transcriptional activator and a repressor, and that each of these functions regulates genes with very specialized and distinct molecular roles. We also show how TBX20 binds to its targets genome-wide in a context-dependent manner, using various cohorts of co-factors to either promote or repress distinct genetic programs within adult heart. Our integrative approach has uncovered several novel aspects of TBX20 and T-box protein function within adult heart.
机译:在成年心脏中对在心脏发育中起关键作用的转录因子的持续需求尚不十分清楚。我们最近证明,TBX20是心脏发育所需的转录调节因子,在成年小鼠心脏的功能和结构表型的维持中具有关键作用。成年心肌细胞中Tbx20的条件性消融导致心力衰竭的快速发作和进展,并伴有明显的传导和收缩表型,导致死亡。在这里,我们描述了成年小鼠心脏中TBX20功能的更全面的分子表征。耦合全基因组染色质免疫沉淀和转录组分析(RNA-Seq),我们确定了基因的一个子集,这些基因改变了Tbx20成人心肌特异性敲除心脏中的表达,这些心脏是TBX20的直接下游靶标。这项分析揭示了TBX20作为转录激活因子和阻遏物的双重作用,并且这些功能中的每一个都调节具有非常专门化和独特的分子作用的基因。我们还展示了TBX20如何以上下文依赖的方式结合全基因组靶标,使用各种辅助因子来促进或抑制成年心脏内不同的遗传程序。我们的综合方法发现了成年心脏中TBX20和T-box蛋白功能的几个新方面。

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