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环磷腺苷效应元件结合蛋白(Epac)与环磷酸腺苷依赖性蛋白激酶(PKA)协同作用,是环磷酸腺苷介导的有丝分裂所必需的。

Epac, in synergy with cAMP-dependent protein kinase (PKA), is required for cAMP-mediated mitogenesis.

作者信息

Hochbaum Daniel, Hong Kyoungja, Barila Guillermo, Ribeiro-Neto Fernando, Altschuler Daniel L

机构信息

Department of Pharmacology, School of Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania 15261, USA.

出版信息

J Biol Chem. 2008 Feb 22;283(8):4464-8. doi: 10.1074/jbc.C700171200. Epub 2007 Dec 6.

Abstract

cAMP stimulates proliferation in many cell types. For many years, cAMP-dependent protein kinase (PKA) represented the only known cAMP effector. PKA, however, does not fully mimic the action of cAMP, indicating the existence of a PKA-independent component. Since cAMP-mediated activation of the G-protein Rap1 and its phosphorylation by PKA are strictly required for the effects of cAMP on mitogenesis, we hypothesized that the Rap1 activator Epac might represent the PKA-independent factor. Here we report that Epac acts synergistically with PKA in cAMP-mediated mitogenesis. We have generated a new dominant negative Epac mutant that revealed that activation of Epac is required for thyroid-stimulating hormone or cAMP stimulation of DNA synthesis. We demonstrate that Epac's action on cAMP-mediated activation of Rap1 and cAMP-mediated mitogenesis depends on the subcellular localization of Epac via its DEP domain. Disruption of the DEP-dependent subcellular targeting of Epac abolished cAMP-Epac-mediated Rap1 activation and thyroid-stimulating hormone-mediated cell proliferation, indicating that an Epac-Rap-PKA signaling unit is critical for the mitogenic action of cAMP.

摘要

环磷酸腺苷(cAMP)可刺激多种细胞类型的增殖。多年来,依赖cAMP的蛋白激酶(PKA)一直是唯一已知的cAMP效应器。然而,PKA并不能完全模拟cAMP的作用,这表明存在一个不依赖PKA的成分。由于cAMP对有丝分裂的影响严格需要cAMP介导的G蛋白Rap1激活及其被PKA磷酸化,我们推测Rap1激活剂Epac可能代表不依赖PKA的因子。在此我们报告,Epac在cAMP介导的有丝分裂中与PKA协同作用。我们构建了一种新的显性负性Epac突变体,该突变体表明Epac的激活是促甲状腺激素或cAMP刺激DNA合成所必需的。我们证明,Epac对cAMP介导的Rap1激活和cAMP介导的有丝分裂的作用取决于Epac通过其DEP结构域的亚细胞定位。破坏Epac依赖DEP的亚细胞靶向作用可消除cAMP-Epac介导的Rap1激活和促甲状腺激素介导的细胞增殖,这表明Epac-Rap-PKA信号单元对cAMP的促有丝分裂作用至关重要。

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