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感光磷酸二酯酶PDE6的GAF结构域与催化结构域之间的直接变构调节。

Direct allosteric regulation between the GAF domain and catalytic domain of photoreceptor phosphodiesterase PDE6.

作者信息

Zhang Xiu-Jun, Cahill Karyn B, Elfenbein Arye, Arshavsky Vadim Y, Cote Rick H

机构信息

Department of Biochemistry and Molecular Biology, University of New Hampshire, Durham, New Hampshire 03824, USA.

出版信息

J Biol Chem. 2008 Oct 31;283(44):29699-705. doi: 10.1074/jbc.M803948200. Epub 2008 Sep 8.

Abstract

Photoreceptor cGMP phosphodiesterase (PDE6) is the central enzyme in the visual transduction cascade. The PDE6 catalytic subunit contains a catalytic domain and regulatory GAF domains. Unlike most GAF domain-containing cyclic nucleotide phosphodiesterases, little is known about direct allosteric communication of PDE6. In this study, we demonstrate for the first time direct, inter-domain allosteric communication between the GAF and catalytic domains in PDE6. The binding affinity of PDE6 for pharmacological inhibitors or for the C-terminal region of the inhibitory gamma subunit (Pgamma), known to directly inhibit PDE6 catalysis, was increased approximately 2-fold by ligands binding to the GAF domain. Binding of the N-terminal half of Pgamma to the GAF domains suffices to induce this allosteric effect. Allosteric communication between GAF and catalytic domains is reciprocal, in that drug binding to the catalytic domain slowed cGMP dissociation from the GAF domain. Although cGMP hydrolysis was not affected by binding of Pgamma1-60, Pgamma lacking its last seven amino acids decreased the Michaelis constant of PDE6 by 2.5-fold. Pgamma1-60 binding to the GAF domain increased vardenafil but not cGMP affinity, indicating that substrate- and inhibitor-binding sites do not totally overlap. In addition, prolonged incubation of PDE6 with vardenafil or sildenafil (but not 3-isobutyl-1-methylxanthine and zaprinast) induced a distinct conformational change in the catalytic domain without affecting the binding properties of the GAF domains. We conclude that although Pgamma-mediated regulation plays the dominant role in visual excitation, the direct, inter-domain allosteric regulation described in this study may play a feedback role in light adaptational processes during phototransduction.

摘要

光感受器环鸟苷酸磷酸二酯酶(PDE6)是视觉转导级联反应中的核心酶。PDE6催化亚基包含一个催化结构域和调节性GAF结构域。与大多数含GAF结构域的环核苷酸磷酸二酯酶不同,关于PDE6的直接变构通讯知之甚少。在本研究中,我们首次证明了PDE6中GAF结构域和催化结构域之间存在直接的结构域间变构通讯。通过与GAF结构域结合的配体,PDE6对药理抑制剂或已知可直接抑制PDE6催化作用的抑制性γ亚基(Pγ)C末端区域的结合亲和力增加了约2倍。Pγ的N末端一半与GAF结构域的结合足以诱导这种变构效应。GAF结构域和催化结构域之间的变构通讯是相互的,因为药物与催化结构域的结合减缓了环鸟苷酸从GAF结构域的解离。尽管环鸟苷酸水解不受Pγ1 - 60结合的影响,但缺少最后七个氨基酸的Pγ使PDE6的米氏常数降低了2.5倍。Pγ1 - 60与GAF结构域的结合增加了伐地那非的亲和力,但未增加环鸟苷酸的亲和力,表明底物和抑制剂结合位点并不完全重叠。此外,PDE6与伐地那非或西地那非(但不是3 - 异丁基 - 1 - 甲基黄嘌呤和扎普司特)长时间孵育会在催化结构域中诱导明显的构象变化,而不影响GAF结构域的结合特性。我们得出结论,尽管Pγ介导的调节在视觉兴奋中起主导作用,但本研究中描述的直接的结构域间变构调节可能在光转导过程中的光适应过程中起反馈作用。

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