首页> 外文期刊>The Journal of biological chemistry >Direct Transactivator-Transcription Factor IID (TFIID) Contacts Drive Yeast Ribosomal Protein Gene Transcription
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Direct Transactivator-Transcription Factor IID (TFIID) Contacts Drive Yeast Ribosomal Protein Gene Transcription

机译:直接异椎动因子转录因子IID(TFIID)接触驱动酵母核糖体蛋白基因转录

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Transcription factor IID (TFIID) plays a key role in regulating eukaryotic gene expression by directly binding promoters and enhancer-bound transactivator proteins. However, the precise mechanisms and outcomes of transactivator-TFIID interaction remain unclear. Transcription of yeast ribosomal protein genes requires TFIID and the DNA-binding transactivator Rap1. We have previously shown that Rap1 directly binds to the TFIID complex through interaction with its TATA-binding protein-associated factor (Taf) subunits Taf4, -5, and -12. Here, we identify and characterize the Rap1 binding domains (RBDs) of Taf4 and Taf5. These RBDs are essential for viability but dispensable for Taf-Taf interactions and TFIID stability. Cells expressing altered Rap1 binding domains exhibit conditional growth, synthetic phenotypes when expressed in combination or with altered Rap1, and are selectively defective in ribosomal protein gene transcription. Taf4 and Taf5 proteins with altered RBDs bind Rap1 with reduced affinity. We propose that collectively the Taf4, Taf5, and Taf12 subunits of TFIID represent the physical and functional targets for Rap1 interaction and, furthermore, that these interactions drive ribosomal protein gene transcription.
机译:转录因子IID(TFIID)在通过直接结合启动子和增强剂结合的反辐期剂蛋白来调节真核基因表达的关键作用。然而,逆变剂-TFIID相互作用的精确机制和结果仍不清楚。酵母核糖体蛋白基因的转录需要TFIID和DNA结合的转移剂RAP1。我们之前已经表明,RAP1通过与其TATA结合蛋白相关因子(TAF)亚基TAF4,-5和-12的相互作用直接与TFIID复合物结合。在这里,我们识别并表征TAF4和TAF5的RAP1结合结构域(RBD)。这些RBD对于可行性,对于TAF-TAF相互作用和TFIID稳定性至关重要。表达改变的RAP1结合结构域的细胞表现出条件生长,合成表型在组合或改变的RAP1中表达时,并在核糖体蛋白基因转录中选择性地缺陷。 TAF4和TAF5蛋白质改变RBD染色RAP1,亲和力降低。我们提出了TFIID的TFIID的TAF4,TAF5和TAF12亚基,代表了RAP1相互作用的物理和功能靶标,并且此外,这些相互作用驱动核糖体蛋白基因转录。

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