• Circ Cardiovasc Genet · Jun 2014

    Induction of microRNA-21 with exogenous hydrogen sulfide attenuates myocardial ischemic and inflammatory injury in mice.

    • Stefano Toldo, Anindita Das, Eleonora Mezzaroma, Vinh Q Chau, Carlo Marchetti, David Durrant, Arun Samidurai, Benjamin W Van Tassell, Chang Yin, Ramzi A Ockaili, Navin Vigneshwar, Nitai D Mukhopadhyay, Rakesh C Kukreja, Antonio Abbate, and Fadi N Salloum.
    • From the Pauley Heart Center, Division of Cardiology, Department of Internal Medicine (S.T., A.D., E.M., V.Q.C., C.M., D.D., A.S., B.W.V.T., C.Y., R.A.O., N.V., R.C.K., A.A., F.N.S.) and Department of Biostatistics (N.D.M.), Virginia Commonwealth University, Richmond.
    • Circ Cardiovasc Genet. 2014 Jun 1;7(3):311-20.

    BackgroundMaintaining physiological levels of hydrogen sulfide during ischemia is necessary to limit injury to the heart. Because of the anti-inflammatory effects of hydrogen sulfide, we proposed that the hydrogen sulfide donor, sodium sulfide (Na2S), would attenuate myocardial injury through upregulation of protective microRNA-21 (miR-21) and suppression of the inflammasome, a macromolecular structure that amplifies inflammation and mediates further injury.Methods And ResultsNa2S-induced miR-21 expression was measured by quantitative polymerase chain reaction in adult primary rat cardiomyocytes and in the mouse heart. We measured inflammasome formation and activity in cardiomyocytes challenged with lipopolysaccharide and ATP or simulated ischemia/reoxygenation and in the heart after regional myocardial ischemia/reperfusion, in the presence or absence of Na2S. To assess the direct anti-inflammatory effects of hydrogen sulfide in vivo, we used a peritonitis model by way of intraperitoneal injection of zymosan A. Na2S attenuated inflammasome formation and activity, measured by counting cytoplasmic aggregates of the scaffold protein apoptosis speck-like protein containing a caspase-recruitment domain (-57%) and caspase-1 activity (-50%) in isolated cardiomyocytes and in the mouse heart (all P<0.05). Na2S also inhibited apoptosis (-38%) and necrosis (-43%) in cardiomyocytes in vitro and reduced myocardial infarct size (-63%) after ischemia/reperfusion injury in vivo (all P<0.05). These protective effects were absent in cells treated with the miR-21 eraser, antagomiR-21, and in miR-21 knockout mice. Na2S also limited the severity of inflammasome-dependent inflammation in the model of peritonitis (P<0.05) in wild-type but not in miR-21 knockout mice.ConclusionsNa2S induces cardioprotective effects through miR-21-dependent attenuation of ischemic and inflammatory injury in cardiomyocytes.© 2014 American Heart Association, Inc.

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