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真菌介体尾部亚基包含经典转录激活结构域。

Fungal mediator tail subunits contain classical transcriptional activation domains.

作者信息

Liu Zhongle, Myers Lawrence C

机构信息

Department of Biochemistry, Geisel School of Medicine at Dartmouth, Hanover, New Hampshire, USA.

Department of Biochemistry, Geisel School of Medicine at Dartmouth, Hanover, New Hampshire, USA

出版信息

Mol Cell Biol. 2015 Apr;35(8):1363-75. doi: 10.1128/MCB.01508-14. Epub 2015 Feb 2.

Abstract

Classical activation domains within DNA-bound eukaryotic transcription factors make weak interactions with coactivator complexes, such as Mediator, to stimulate transcription. How these interactions stimulate transcription, however, is unknown. The activation of reporter genes by artificial fusion of Mediator subunits to DNA binding domains that bind to their promoters has been cited as evidence that the primary role of activators is simply to recruit Mediator. We have identified potent classical transcriptional activation domains in the C termini of several tail module subunits of Saccharomyces cerevisiae, Candida albicans, and Candida dubliniensis Mediator, while their N-terminal domains are necessary and sufficient for their incorporation into Mediator but do not possess the ability to activate transcription when fused to a DNA binding domain. This suggests that Mediator fusion proteins actually are functioning in a manner similar to that of a classical DNA-bound activator rather than just recruiting Mediator. Our finding that deletion of the activation domains of S. cerevisiae Med2 and Med3, as well as C. dubliniensis Tlo1 (a Med2 ortholog), impairs the induction of certain genes shows these domains function at native promoters. Activation domains within coactivators are likely an important feature of these complexes and one that may have been uniquely leveraged by a common fungal pathogen.

摘要

与DNA结合的真核转录因子中的经典激活结构域与共激活因子复合物(如中介体)进行弱相互作用,以刺激转录。然而,这些相互作用如何刺激转录尚不清楚。通过将中介体亚基人工融合到与其启动子结合的DNA结合结构域来激活报告基因,这被引为证据,证明激活因子的主要作用仅仅是招募中介体。我们在酿酒酵母、白色念珠菌和都柏林念珠菌中介体的几个尾部模块亚基的C末端鉴定出了强效的经典转录激活结构域,而它们的N末端结构域对于它们整合到中介体中是必要且充分的,但当与DNA结合结构域融合时不具备激活转录的能力。这表明中介体融合蛋白实际上是以类似于经典的与DNA结合的激活因子的方式发挥作用,而不仅仅是招募中介体。我们发现,删除酿酒酵母Med2和Med3以及都柏林念珠菌Tlo1(Med2的直系同源物)的激活结构域会损害某些基因的诱导,这表明这些结构域在天然启动子处发挥作用。共激活因子中的激活结构域可能是这些复合物的一个重要特征,并且可能是一种常见真菌病原体独特利用的特征。

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