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p53 转录激活结构域与中介体亚基 MED25 相互作用的结构基础。

Structural Basis for the Interaction between p53 Transactivation Domain and the Mediator Subunit MED25.

机构信息

Disease Target Structure Research Center, KRIBB, Daejeon 34141, Korea.

Department of Proteome Structural Biology, KRIBB School of Bioscience, Korea University of Science and Technology, Daejeon 34113, Korea.

出版信息

Molecules. 2018 Oct 22;23(10):2726. doi: 10.3390/molecules23102726.

Abstract

Eukaryotic transcription initiation is mediated by interactions between transcriptional activators and the mediator coactivator complex. Molecular interaction of p53 transcription factor with mediator complex subunit 25 (MED25) is essential for its target gene transcription. In this study, we characterized the molecular interaction between p53 transactivation domain (p53TAD) and activator interaction domain (ACID) of MED25 using nuclear magnetic resonance (NMR) spectroscopy. The NMR chemical shift perturbation and isothermal titration calorimetry (ITC) data showed that p53TAD interacted with MED25 ACID mainly through the p53TAD2 sequence motif. Taken together with the mutagenesis data, the refined structural model of MED25 ACID/p53TAD2 peptide complex showed that an amphipathic α-helix of p53TAD2 peptide bound an elongated hydrophobic groove of MED25 ACID. Furthermore, our results revealed the highly conserved mechanism of MED25 interaction with intrinsically unfolded acidic TADs from the transcriptional activators p53, ERM (Ets-related molecule), and herpes simplex virus protein 16 (VP16).

摘要

真核生物转录起始是由转录激活因子与中介共激活因子复合物之间的相互作用介导的。p53 转录因子与中介复合物亚基 25(MED25)的分子相互作用对于其靶基因转录是必不可少的。在这项研究中,我们使用核磁共振(NMR)光谱法表征了 p53 转录激活结构域(p53TAD)与 MED25 的激活剂相互作用结构域(ACID)之间的分子相互作用。NMR 化学位移扰动和等温热滴定(ITC)数据表明,p53TAD 主要通过 p53TAD2 序列基序与 MED25 ACID 相互作用。与突变数据相结合,MED25 ACID/p53TAD2 肽复合物的精细化结构模型表明,p53TAD2 肽的一个两亲性α-螺旋结合了 MED25 ACID 的一个拉长的疏水性凹槽。此外,我们的结果揭示了 MED25 与转录激活因子 p53、ERM(Ets 相关分子)和单纯疱疹病毒蛋白 16(VP16)中的固有无规则酸性 TAD 相互作用的高度保守机制。

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