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Probing the 14-3-3 Isoform-Specificity Profile of Protein–Protein Interactions Stabilized by Fusicoccin A

机译:探讨Fusicccin A稳定的蛋白质 - 蛋白质相互作用的14-3-3种异构特异性分布

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摘要

Fusicoccin A (FC) is a fungal phytotoxin that stabilizes protein–protein interactions (PPIs) between 14-3-3 adapter proteins and their phosphoprotein interaction partners. Recently, FC has emerged as an important chemical probe of human 14-3-3 PPIs involved in cancer and neurobiology. These previous studies have established the structural requirements for FC-induced stabilization of 14-3-3·client phosphoprotein complexes; however, the effect of 14-3-3 isoforms on FC activity remains underexplored. This is a relevant question for the continued development of FC variants because there are seven isoforms of 14-3-3 in humans. Despite their sequence and structural similarities, a growing body of experimental evidence supports both tissue-specific expression of 14-3-3 isoforms and isoform-specific functions in vivo . Herein, we interrogate the isoform-specificity profile of FC in vitro using recombinant 14-3-3 isoforms and a library of fluorescein-labeled hexaphosphopeptides mimicking the C-terminal recognition domains of client proteins that are characterized targets of FC in vivo . Our results reveal modest isoform preferences for individual client phospholigands and demonstrate that FC differentially stabilizes PPIs involving 14-3-3σ. Together, these data support the feasibility of developing FC variants with enhanced isoform selectivity.
机译:FusiCoccin A(Fc)是一种真菌植物毒素,其稳定14-3-3〜3〜3-3次蛋白质和磷蛋白相互作用伴侣之间的蛋白质 - 蛋白质相互作用(PPI)。最近,FC已成为涉及癌症和神经生物学的人为14-3-3 PPI的重要化学探针。以前的研究已经建立了FC诱导的14-3-3·客户磷蛋白复合物的结构要求;然而,14-3-3同种型对Fc活性的影响仍然是缺乏缺陷的。这是对FC变体继续发展的有关问题,因为人类有七个同种型14-3-3。尽管它们的序列和结构性相似,但实验证据的生长体均支持组织特异性表达14-3-3同种型和同种型特异性函数在体内。在此,我们使用重组14-3-3种同种型询问Fc IM的异常特异性分布,并使用荧光素标记的六磷酸盐库,其模仿诸如Fc 体内。我们的结果揭示了适用于个体客户磷酸胆碱的适度同种型偏好,并证明FC差异稳定PPI涉及14-3-3σ。这些数据在一起,支持开发FC变体的可行性,具有增强的同种型选择性。

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