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多功能 SAGA 复合物的结构和结合 TBP 的分子机制。

Architecture of the multi-functional SAGA complex and the molecular mechanism of holding TBP.

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, Illkirch, France.

Centre National de la Recherche Scientifique, UMR7104, Institut National de la Santé et de la Recherche Médicale, U1258, Université de Strasbourg, France.

出版信息

FEBS J. 2021 May;288(10):3135-3147. doi: 10.1111/febs.15563. Epub 2020 Sep 29.

DOI:10.1111/febs.15563
PMID:32946670
Abstract

In eukaryotes, transcription of protein encoding genes is initiated by the controlled deposition of the TATA-box binding protein TBP onto gene promoters, followed by the ordered assembly of a pre-initiation complex. The SAGA co-activator is a 19-subunit complex that stimulates transcription by the action of two chromatin-modifying enzymatic modules, a transcription activator binding module, and by delivering TBP. Recent cryo electron microscopy structures of yeast SAGA with bound nucleosome or TBP reveal the architecture of the different functional domains of the co-activator. An octamer of histone fold domains is found at the core of SAGA. This octamer, which deviates considerably from the symmetrical analogue forming the nucleosome, establishes a peripheral site for TBP binding where steric hindrance represses interaction with spurious DNA. The structures point to a mechanism for TBP delivery and release from SAGA that requires TFIIA and whose efficiency correlates with the affinity of DNA to TBP. These results provide a structural basis for understanding specific TBP delivery onto gene promoters and the role played by SAGA in regulating gene expression. The properties of the TBP delivery machine harboured by SAGA are compared with the TBP loading device present in the TFIID complex and show multiple similitudes.

摘要

在真核生物中,蛋白编码基因的转录是通过 TATA 框结合蛋白 TBP 受控地沉积到基因启动子上开始的,随后是起始前复合物的有序组装。SAGA 共激活因子是一个由 19 个亚基组成的复合物,通过两种染色质修饰酶模块、一个转录激活剂结合模块和传递 TBP 的作用来刺激转录。最近的酵母 SAGA 与结合核小体或 TBP 的冷冻电子显微镜结构揭示了共激活因子不同功能域的结构。在 SAGA 的核心发现了一个组蛋白折叠结构域的八聚体。这个八聚体与形成核小体的对称类似物有很大的不同,它为 TBP 结合建立了一个外围位点,空间位阻抑制了与虚假 DNA 的相互作用。这些结构为 TBP 从 SAGA 上的递呈和释放机制提供了结构基础,该机制需要 TFIIA,其效率与 DNA 与 TBP 的亲和力相关。这些结果为理解特定的 TBP 递呈到基因启动子以及 SAGA 在调节基因表达中所起的作用提供了结构基础。SAGA 所具有的 TBP 递呈机器的特性与 TFIID 复合物中存在的 TBP 加载装置进行了比较,显示出多种相似之处。

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