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中介亚基 Med15 决定了酵母转录激活因子 Gal4 和 Gcn4 的保守“模糊”结合机制。

Mediator subunit Med15 dictates the conserved "fuzzy" binding mechanism of yeast transcription activators Gal4 and Gcn4.

机构信息

Division of Basic Sciences, Fred Hutchinson Cancer Research Center, Seattle, WA, USA.

Department of Biochemistry, University of Washington, Seattle, WA, USA.

出版信息

Nat Commun. 2021 Apr 13;12(1):2220. doi: 10.1038/s41467-021-22441-4.

Abstract

The acidic activation domain (AD) of yeast transcription factor Gal4 plays a dual role in transcription repression and activation through binding to Gal80 repressor and Mediator subunit Med15. The activation function of Gal4 arises from two hydrophobic regions within the 40-residue AD. We show by NMR that each AD region binds the Mediator subunit Med15 using a "fuzzy" protein interface. Remarkably, comparison of chemical shift perturbations shows that Gal4 and Gcn4, two intrinsically disordered ADs of different sequence, interact nearly identically with Med15. The finding that two ADs of different sequence use an identical fuzzy binding mechanism shows a common sequence-independent mechanism for AD-Mediator binding, similar to interactions within a hydrophobic cloud. In contrast, the same region of Gal4 AD interacts strongly with Gal80 via a distinct structured complex, implying that the structured binding partner of an intrinsically disordered protein dictates the type of protein-protein interaction.

摘要

酵母转录因子 Gal4 的酸性激活结构域 (AD) 通过与 Gal80 抑制子和 Mediator 亚基 Med15 结合,在转录抑制和激活中发挥双重作用。Gal4 的激活功能源于 AD 中 40 个残基内的两个疏水区。我们通过 NMR 表明,每个 AD 区域都使用“模糊”的蛋白质界面与 Mediator 亚基 Med15 结合。值得注意的是,化学位移扰动的比较表明,Gal4 和 Gcn4,两个不同序列的固有无序 AD,与 Med15 几乎相同地相互作用。这一发现表明,两个不同序列的 AD 采用相同的模糊结合机制,表明 AD-Mediator 结合存在一种常见的序列非依赖性机制,类似于疏水区内的相互作用。相比之下,Gal4 AD 的相同区域通过独特的结构复合物与 Gal80 强烈相互作用,这意味着无序蛋白质的结构结合伴侣决定了蛋白质-蛋白质相互作用的类型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/53e3/8044209/5f0de983ec3d/41467_2021_22441_Fig1_HTML.jpg

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