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Spatiotemporal Dynamics of β-Adrenergic cAMP Signals and L-Type Ca2+ Channel Regulation in Adult Rat Ventricular Myocytes

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dc.contributor.author Leroy, Jerome
dc.contributor.author Abi-Gerges, Aniella
dc.contributor.author Nikolaev, Viacheslav O.
dc.contributor.author Richter, Wito
dc.contributor.author Lecheme, Patrick
dc.contributor.author Mazet, Jean-Luc
dc.contributor.author Conti, Marco
dc.contributor.author Fischmeister, Rodolphe
dc.contributor.author Vandecasteele, Gregoire
dc.date.accessioned 2017-10-19T10:15:53Z
dc.date.available 2017-10-19T10:15:53Z
dc.date.copyright 2008 en_US
dc.date.issued 2017-10-19
dc.identifier.issn 1524-4571 en_US
dc.identifier.uri http://hdl.handle.net/10725/6356
dc.description.abstract Steady-state activation of cardiac β-adrenergic receptors leads to an intracellular compartmentation of cAMP resulting from localized cyclic nucleotide phosphodiesterase (PDE) activity. To evaluate the time course of the cAMP changes in the different compartments, brief (15 seconds) pulses of isoprenaline (100 nmol/L) were applied to adult rat ventricular myocytes (ARVMs) while monitoring cAMP changes beneath the membrane using engineered cyclic nucleotide-gated channels and within the cytosol with the fluorescence resonance energy transfer–based sensor, Epac2-camps. cAMP kinetics in the two compartments were compared to the time course of the L-type Ca2+ channel current (ICa,L) amplitude. The onset and recovery of cAMP transients were, respectively, 30% and 50% faster at the plasma membrane than in the cytosol, in agreement with a rapid production and degradation of the second messenger at the plasma membrane and a restricted diffusion of cAMP to the cytosol. ICa,L amplitude increased twice slower than cAMP at the membrane, and the current remained elevated for ≈5 minutes after cAMP had already returned to basal level, indicating that cAMP changes are not rate-limiting in channel phosphorylation/dephosphorylation. Inhibition of PDE4 (with 10 μmol/L Ro 20-1724) increased the amplitude and dramatically slowed down the onset and recovery of cAMP signals, whereas PDE3 blockade (with 1 μmol/L cilostamide) had a minor effect only on subsarcolemmal cAMP. However, when both PDE3 and PDE4 were inhibited, or when all PDEs were blocked using 3-isobutyl-l-methylxanthine (300 μmol/L), cAMP signals and ICa,L declined with a time constant >10 minutes. cAMP-dependent protein kinase inhibition with protein kinase inhibitor produced a similar effect as a partial inhibition of PDE4 on the cytosolic cAMP transient. Consistently, cAMP-PDE assay on ARVMs briefly (15 seconds) exposed to isoprenaline showed a pronounced (up to ≈50%) dose-dependent increase in total PDE activity, which was mainly attributable to activation of PDE4. These results reveal temporally distinct β-adrenergic receptor cAMP compartments in ARVMs and shed new light on the intricate roles of PDE3 and PDE4. en_US
dc.language.iso en en_US
dc.title Spatiotemporal Dynamics of β-Adrenergic cAMP Signals and L-Type Ca2+ Channel Regulation in Adult Rat Ventricular Myocytes en_US
dc.type Article en_US
dc.description.version Published en_US
dc.author.school SOM en_US
dc.author.idnumber 201402416 en_US
dc.author.department N/A en_US
dc.description.embargo N/A en_US
dc.relation.journal Circulation Research en_US
dc.journal.volume 102 en_US
dc.journal.issue 9 en_US
dc.article.pages 1091-1100 en_US
dc.keywords cAMP en_US
dc.keywords L-type calcium current en_US
dc.keywords 5′-3′ cyclic nucleotide phosphodiesterases en_US
dc.keywords β-adrenergic receptors en_US
dc.keywords Compartmentation en_US
dc.identifier.doi https://doi.org/10.1161/CIRCRESAHA.107.167817 en_US
dc.identifier.ctation Leroy, J., Abi-Gerges, A., Nikolaev, V. O., Richter, W., Lechêne, P., Mazet, J. L., ... & Vandecasteele, G. (2008). Spatiotemporal Dynamics of β-Adrenergic cAMP Signals and L-Type Ca2+ Channel Regulation in Adult Rat Ventricular Myocytes. Circulation research, 102(9), 1091-1100. en_US
dc.author.email aniella.abigerges@lau.edu.lb en_US
dc.identifier.tou http://libraries.lau.edu.lb/research/laur/terms-of-use/articles.php en_US
dc.identifier.url https://www.ahajournals.org/doi/full/10.1161/CIRCRESAHA.107.167817 en_US
dc.orcid.id https://orcid.org/0000-0001-9974-4023 en_US
dc.author.affiliation Lebanese American University en_US


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