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The TAF10-containing TFIID and SAGA transcriptional complexes are dispensable for early somitogenesis in the mouse embryo

机译:包含TAF10的TFIID和SAGA转录复合物对于小鼠胚胎早期的体发生是必不可少的

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摘要

During development, tightly regulated gene expression programs control cell fate and patterning. A key regulatory step in eukaryotic transcription is the assembly of the pre-initiation complex (PIC) at promoters. The PIC assembly has mainly been studied in vitro, and little is known about its composition during development. In vitro data suggests that TFIID is the general transcription factor that nucleates PIC formation at promoters. Here we show that TAF10, a subunit of TFIID and of the transcriptional co-activator SAGA, is required for the assembly of these complexes in the mouse embryo. We performed Taf10 conditional deletions during mesoderm development and show that Taf10 loss in the presomitic mesoderm (PSM) does not prevent cyclic gene transcription or PSM segmental patterning, while lateral plate differentiation is profoundly altered. During this period, global mRNA levels are unchanged in the PSM, with only a minor subset of genes dysregulated. Together, our data strongly suggest that the TAF10-containing canonical TFIID and SAGA complexes, are dispensable for early paraxial mesoderm development, arguing against the generic role in transcription proposed for these fully assembled holo complexes.
机译:在发育过程中,严格调控的基因表达程序可控制细胞命运和模式。真核转录中的关键调控步骤是启动子上启动前复合物(PIC)的组装。 PIC组件主要是在体外研究的,在开发过程中对其组成了解甚少。体外数据表明,TFIID是使启动子上PIC形成成核的通用转录因子。在这里我们显示,TAF10是TFIID的一个亚基,也是转录共激活因子SAGA的亚基,在小鼠胚胎中组装这些复合物是必需的。我们在中胚层发育过程中进行了Taf10条件删除,并显示了在早熟中胚层(PSM)中Taf10的丢失并不能阻止环状基因转录或PSM节段模式,而侧板的分化则发生了深远的变化。在此期间,PSM中的整体mRNA水平没有变化,只有一小部分基因失调。总之,我们的数据强烈表明,含有TAF10的规范性TFIID和SAGA复合物对于早期近轴中胚层的发育是必不可少的,这与这些完全组装的全息复合物在转录中的一般作用形成了争论。

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