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14-3-3σ蛋白-蛋白相互作用的协同稳定作用:共价蛋白修饰

Cooperative stabilisation of 14-3-3σ protein-protein interactions covalent protein modification.

作者信息

Falcicchio Marta, Ward Jake A, Chothia Sara Y, Basran Jaswir, Mohindra Alisha, Macip Salvador, Roversi Pietro, Doveston Richard G

机构信息

Leicester Institute for Structural and Chemical Biology, University of Leicester University Road Leicester LE1 7RH UK

School of Chemistry, University of Leicester University Road Leicester LE1 7RH UK.

出版信息

Chem Sci. 2021 Sep 6;12(39):12985-12992. doi: 10.1039/d1sc02120f. eCollection 2021 Oct 13.

DOI:10.1039/d1sc02120f
PMID:34745529
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8513901/
Abstract

14-3-3 proteins are an important family of hub proteins that play important roles in many cellular processes a large network of interactions with partner proteins. Many of these protein-protein interactions (PPI) are implicated in human diseases such as cancer and neurodegeneration. The stabilisation of selected 14-3-3 PPIs using drug-like 'molecular glues' is a novel therapeutic strategy with high potential. However, the examples reported to date have a number of drawbacks in terms of selectivity and potency. Here, we report that WR-1065, the active species of the approved drug amifostine, covalently modifies 14-3-3σ at an isoform-unique cysteine residue, Cys38. This modification leads to isoform-specific stabilisation of two 14-3-3σ PPIs in a manner that is cooperative with a well characterised molecular glue, fusicoccin A. Our findings reveal a novel stabilisation mechanism for 14-3-3σ, an isoform with particular involvement in cancer pathways. This mechanism can be exploited to harness the enhanced potency conveyed by covalent drug molecules and dual ligand cooperativity. This is demonstrated in two cancer cell lines whereby the cooperative behaviour of fusicoccin A and WR-1065 leads to enhanced efficacy for inducing cell death and attenuating cell growth.

摘要

14-3-3蛋白是一类重要的中心蛋白家族,在许多细胞过程中发挥重要作用,与伴侣蛋白形成庞大的相互作用网络。这些蛋白质-蛋白质相互作用(PPI)中的许多都与癌症和神经退行性疾病等人类疾病有关。使用类药物“分子胶”稳定选定的14-3-3 PPI是一种具有高潜力的新型治疗策略。然而,迄今为止报道的例子在选择性和效力方面存在一些缺点。在这里,我们报告已批准药物氨磷汀的活性成分WR-1065在一个亚型独特的半胱氨酸残基Cys38处共价修饰14-3-3σ。这种修饰以一种与特征明确的分子胶——藤镰刀壳梭链孢酸A协同的方式导致两个14-3-3σ PPI的亚型特异性稳定。我们的研究结果揭示了14-3-3σ的一种新型稳定机制,14-3-3σ是一种特别参与癌症通路的亚型。这种机制可被利用来利用共价药物分子和双配体协同作用所带来的增强效力。这在两种癌细胞系中得到了证明,其中梭链孢酸A和WR-1065的协同行为导致诱导细胞死亡和减弱细胞生长的功效增强。

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Regulation of p53 by the 14-3-3 protein interaction network: new opportunities for drug discovery in cancer.14-3-3蛋白相互作用网络对p53的调控:癌症药物研发的新机遇
Cell Death Discov. 2020 Nov 16;6(1):126. doi: 10.1038/s41420-020-00362-3.
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Fragment-Based Stabilizers of Protein-Protein Interactions through Imine-Based Tethering.
利用天然质谱追踪共价分子胶稳定化的机制。
Chem Sci. 2023 May 31;14(24):6756-6762. doi: 10.1039/d3sc01732j. eCollection 2023 Jun 21.
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Front Mol Biosci. 2022 Nov 8;9:1043673. doi: 10.3389/fmolb.2022.1043673. eCollection 2022.
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