Phosphatidylinositol 3-Kinase Offsets cAMP-Mediated Positive Inotropic Effect via Inhibiting Ca2+ Influx in Cardiomyocytes

doi:10.1161/01.RES.0000150049.74539.8a

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Circulation Research. 2004;95:1183-1190
Published online before print November 11, 2004, doi: 10.1161/01.RES.0000150049.74539.8a

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(Circulation Research. 2004;95:1183.)
© 2004 American Heart Association, Inc.

Cellular Biology

Phosphatidylinositol 3-Kinase Offsets cAMP-Mediated Positive Inotropic Effect via Inhibiting Ca²⁺ Influx in Cardiomyocytes

Veronique Leblais^*, Su-Hyun Jo^*, Khalid Chakir^*, Victor Maltsev, Ming Zheng, Michael T. Crow, Wang Wang, Edward G. Lakatta, Rui-Ping Xiao

From the Laboratory of Cardiovascular Science (V.L., S.-H.J., K.C., V.M., M.Z., M.T.C., W.W., E.G.L., R.-P.X.), Gerontology Research Center, National Institute on Aging, NIH, Baltimore, Md; The Institute of Molecular Medicine and The Institute of Cardiovascular Sciences (M.Z., R.-P.X.), Peking University, Beijing, China. Present address for V.L. is Laboratoire de Pharmacologie de l’UFR de Pharmacie & INSERM EMI0356, Université Victor Segalen Bordeaux 2, Bordeaux, France; and for S.-H.J., Department of Physiology, Cheju National University College of Medicine, Ara 1-Dong, Jeju, Korea.

Correspondence to Rui-Ping Xiao, MD, PhD, Laboratory of Cardiovascular Science, Gerontology Research Center, National Institute on Aging, 5600 Nathan Shock Dr, Baltimore, MD 21224. E-mail XiaoR{at}grc.nia.nih.gov

Phosphoinositide 3-kinase (PI3K) has been implicated in ß₂-adrenergicreceptor (ß₂-AR)/G_i-mediated compartmentation of theconcurrent G_s-cAMP signaling, negating ß₂-AR–inducedphospholamban phosphorylation and the positive inotropic andlusitropic responses in cardiomyocytes. However, it is unclearwhether PI3K crosstalks with the ß₁-AR signal transduction,and even more generally, with the cAMP/PKA pathway. In thisstudy, we show that selective ß₁-AR stimulation markedlyincreases PI3K activity in adult rat cardiomyocytes. Inhibitionof PI3K by LY294002 significantly enhances ß₁-AR–inducedincreases in L-type Ca²⁺ currents, intracellular Ca²⁺ transients,and myocyte contractility, without altering the receptor-mediatedphosphorylation of phospholamban. The LY294002 potentiatingeffects are completely prevented by ßARK-ct, a peptideinhibitor of ß-adrenergic receptor kinase-1 (ßARK1)as well as G_ß signaling, but not by disrupting G_ifunction with pertussis toxin. Moreover, forskolin, an adenylylcyclase activator, also elevates PI3K activity and inhibitionof PI3K enhances forskolin-induced contractile response in aßARK-ct sensitive manner. In contrast, PI3K inhibitionaffects neither the basal contractility nor high extracellularCa²⁺-induced increase in myocyte contraction. These resultssuggest that ß₁-AR stimulation activates PI3K viaa PKA-dependent mechanism, and that G_ß and the subsequentactivation of ßARK1 are critically involved in thePKA-induced PI3K signaling which, in turn, negates cAMP-inducedpositive inotropic effect via inhibiting sarcolemmal Ca²⁺ influxand the subsequent increase in intracellular Ca²⁺ transients,without altering the receptor-mediated phospholamban phosphorylation,in intact cardiomyocytes.

Key Words: PI3K • PKA • cardiac contractility • L-type calcium current • ß₁-adrenergic receptor

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