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磷酸二酯酶诱导的环磷酸腺苷(cAMP)从蛋白激酶A解离的动力学:通过氢氘交换质谱法捕获瞬时三元复合物

Dynamics of phosphodiesterase-induced cAMP dissociation from protein kinase A: capturing transient ternary complexes by HDXMS.

作者信息

Krishnamurthy Srinath, Moorthy Balakrishnan Shenbaga, Liqin Lin, Anand Ganesh S

机构信息

Department of Biological Sciences, National University of Singapore, Singapore.

出版信息

Biochim Biophys Acta. 2013 Jun;1834(6):1215-21. doi: 10.1016/j.bbapap.2013.02.028. Epub 2013 Mar 15.

DOI:10.1016/j.bbapap.2013.02.028
PMID:23501673
Abstract

cAMP signaling is a fundamental cellular process necessary for mediating responses to hormonal stimuli. In contrast to cAMP-dependent activation of protein kinase A (PKA), an important cellular target, far less is known on termination in cAMP signaling, specifically how phosphodiesterases (PDEs) facilitate dissociation and hydrolysis of bound cAMP. In this study, we have probed the dynamics of a ternary complex of PKA and a PDE-RegA with an excess of a PDE-nonhydrolyzable cAMP analog, Sp-cAMPS by amide hydrogen/deuterium exchange mass spectrometry (HDXMS). Our results highlight how HDXMS can be used to monitor reactions together with mapping conformational dynamics of transient signaling complexes. Our results confirm a two-state model for active RegA-mediated dissociation of bound cAMP. Further, our results reveal that Sp-cAMPS and RegA mediate mutually exclusive interactions with the same region of PKA and at specific concentrations of Sp-cAMPS, RegA is capable of blocking Sp-cAMPS reassociation to PKA. This provides a molecular basis for how PDEs modulate levels of intracellular cAMP so that PKA is better suited to responding to fluxes rather than constant levels of cAMP. This study underscores how HDXMS can be a powerful tool for monitoring reactions together with mapping conformational dynamics in signaling proteins. This article is part of a Special Issue entitled: Mass spectrometry in structural biology.

摘要

环磷酸腺苷(cAMP)信号传导是介导对激素刺激反应所必需的基本细胞过程。与作为重要细胞靶点的蛋白激酶A(PKA)的cAMP依赖性激活相反,人们对cAMP信号传导的终止了解甚少,特别是磷酸二酯酶(PDEs)如何促进结合的cAMP的解离和水解。在本研究中,我们通过酰胺氢/氘交换质谱(HDXMS),用过量的PDE不可水解的cAMP类似物Sp-cAMPS探测了PKA和PDE-RegA三元复合物的动力学。我们的结果突出了HDXMS如何能够用于监测反应以及绘制瞬时信号复合物的构象动力学图谱。我们的结果证实了活性RegA介导的结合cAMP解离的双态模型。此外,我们的结果表明,Sp-cAMPS和RegA与PKA的同一区域介导相互排斥的相互作用,并且在特定浓度的Sp-cAMPS下,RegA能够阻止Sp-cAMPS重新结合到PKA。这为PDEs如何调节细胞内cAMP水平提供了分子基础,从而使PKA更适合于对cAMP的通量而非恒定水平做出反应。这项研究强调了HDXMS如何能够成为监测反应以及绘制信号蛋白构象动力学图谱的强大工具。本文是名为:结构生物学中的质谱分析的特刊的一部分。

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