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蛋白激酶C诱导ATP敏感性钾通道激活的分子基础。

Molecular basis of protein kinase C-induced activation of ATP-sensitive potassium channels.

作者信息

Light P E, Bladen C, Winkfein R J, Walsh M P, French R J

机构信息

Departments of Physiology and Biophysics, Pharmacology and Therapeutics, and Biochemistry and Molecular Biology, University of Calgary, Calgary, AB, Canada T2N 4N1.

出版信息

Proc Natl Acad Sci U S A. 2000 Aug 1;97(16):9058-63. doi: 10.1073/pnas.160068997.

Abstract

Potassium channels that are inhibited by internal ATP (K(ATP) channels) provide a critical link between metabolism and cellular excitability. Protein kinase C (PKC) acts on K(ATP) channels to regulate diverse cellular processes, including cardioprotection by ischemic preconditioning and pancreatic insulin secretion. PKC action decreases the Hill coefficient of ATP binding to cardiac K(ATP) channels, thereby increasing their open probability at physiological ATP concentrations. We show that PKC similarly regulates recombinant channels from both the pancreas and heart. Surprisingly, PKC acts via phosphorylation of a specific, conserved threonine residue (T180) in the pore-forming subunit (Kir6.2). Additional PKC consensus sites exist on both Kir and the larger sulfonylurea receptor (SUR) subunits. Nonetheless, T180 controls changes in open probability induced by direct PKC action either in the absence of, or in complex with, the accessory SUR1 (pancreatic) or SUR2A (cardiac) subunits. The high degree of conservation of this site among different K(ATP) channel isoforms suggests that this pathway may have wide significance for the physiological regulation of K(ATP) channels in various tissues and organelles.

摘要

受细胞内ATP抑制的钾通道(K(ATP)通道)在新陈代谢与细胞兴奋性之间提供了关键联系。蛋白激酶C(PKC)作用于K(ATP)通道以调节多种细胞过程,包括缺血预处理的心脏保护作用和胰腺胰岛素分泌。PKC的作用降低了ATP与心脏K(ATP)通道结合的希尔系数,从而在生理ATP浓度下增加其开放概率。我们发现PKC同样调节来自胰腺和心脏的重组通道。令人惊讶的是,PKC通过孔形成亚基(Kir6.2)中一个特定的、保守的苏氨酸残基(T180)的磷酸化起作用。在Kir和较大的磺脲类受体(SUR)亚基上都存在其他PKC共有位点。尽管如此,T180在不存在辅助SUR1(胰腺)或SUR2A(心脏)亚基或与它们结合的情况下,控制由直接PKC作用诱导的开放概率变化。该位点在不同K(ATP)通道亚型中的高度保守表明,这条途径可能对各种组织和细胞器中K(ATP)通道的生理调节具有广泛意义。

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