Small Heat-Shock Protein Hsp20 Attenuates {beta}-Agonist-Mediated Cardiac Remodeling Through Apoptosis Signal-Regulating Kinase 1

doi:10.1161/01.RES.0000251074.19348.af

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Circulation Research. 2006;99:1233-1242
Published online before print October 26, 2006, doi: 10.1161/01.RES.0000251074.19348.af

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Small Heat-Shock Protein Hsp20 Attenuates ß-Agonist–Mediated Cardiac Remodeling Through Apoptosis Signal–Regulating Kinase 1

Guo-Chang Fan, Qunying Yuan, Guojie Song, Yigang Wang, Guoli Chen, Jiang Qian, Xiaoyang Zhou, Yong J. Lee, Muhammad Ashraf, Evangelia G. Kranias

From the Departments of Pharmacology and Cell Biophysics (G.-C.F., Q.Y., G.C., J.Q., X.Z., E.G.K.) and Pathology and Laboratory Medicine (Y.W., MA.), University of Cincinnati College of Medicine, Ohio; Department of Cardiology (G.S.), 2nd Clinical School of Yangzhou University Medical College, China; Department of Surgery and Pharmacology (Y.J.L.), University of Pittsburgh, Pa; and Molecular Biology Division (E.G.K.), Center for Basic Research, Foundation for Biomedical Research of the Academy of Athens, Greece.

Correspondence to Evangelia G. Kranias, PhD, Department of Pharmacology and Cell Biophysics, University of Cincinnati, 231 Albert Sabin Way, Cincinnati, OH 45267-0575. E-mail Litsa.Kranias{at}uc.edu

Chronic stimulation of the ß-adrenergic neurohormonalaxis contributes to the progression of heart failure and mortalityin animal models and human patients. In cardiomyocytes, activationof the ß-adrenergic pathway has been shown to resultin transiently increased expression of a cardiac small heat-shockprotein Hsp20. The present study shows that cardiac overexpression(10-fold) of Hsp20 may protect the heart against ß-agonist–inducedcardiac remodeling, associated with isoproterenol (50 µg/gper day) infusion for 14 days. Hsp20 attenuated the cardiachypertrophic response, markedly reduced interstitial fibrosis,and decreased apoptosis. Contractility was also preserved inhearts with increased Hsp20 levels. These beneficial effectswere associated with attenuation of the ASK1-JNK/p38 (apoptosissignal–regulating kinase 1/c-Jun NH₂-terminal kinase/p38)signaling cascade triggered by isoproterenol, whereas therewas no difference in either extracellular signal-related kinase1/2 or Akt activation. Parallel in vitro experiments supportedthe inhibitory role of Hsp20 on enforced ASK1-JNK/p38 activationin both H9c2 cells and adult rat cardiomyocytes. Immunostainingstudies also demonstrated that Hsp20 colocalizes with ASK1 incardiomyocytes. Taken together, our findings indicate that (1)ß-agonist–induced cardiac injury is associatedwith activation of the ASK1-JNK/p38 cascade; (2) increased expressionof Hsp20 attenuates the induction of remodeling, dysfunction,and apoptosis in response to sustained ß-adrenergicstimulation; and (3) the beneficial effects of Hsp20 are atleast partially attributable to inhibition of the ASK1-signalingcascade.

Key Words: small heat-shock protein Hsp20 • apoptosis • ß-adrenergic receptor • apoptosis signal–regulating kinase 1 (ASK1)

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