SR9009 administered for one day after myocardial ischemia-reperfusion prevents heart failure in mice by targeting the cardiac inflammasome.
Cristine J ReitzFaisal J AlibhaiTarak N KhatuaMina RasouliByram W BridleThomas P BurrisTami A MartinoPublished in: Communications biology (2019)
Reperfusion of patients after myocardial infarction (heart attack) triggers cardiac inflammation that leads to infarct expansion and heart failure (HF). We previously showed that the circadian mechanism is a critical regulator of reperfusion injury. However, whether pharmacological targeting using circadian medicine limits reperfusion injury and protects against HF is unknown. Here, we show that short-term targeting of the circadian driver REV-ERB with SR9009 benefits long-term cardiac repair post-myocardial ischemia reperfusion in mice. Gain and loss of function studies demonstrate specificity of targeting REV-ERB in mice. Treatment for just one day abates the cardiac NLRP3 inflammasome, decreasing immunocyte recruitment, and thereby allowing the vulnerable infarct to heal. Therapy is given in vivo, after reperfusion, and promotes efficient repair. This study presents downregulation of the cardiac inflammasome in fibroblasts as a cellular target of SR9009, inviting more targeted therapeutic investigations in the future.
Keyphrases
- left ventricular
- acute myocardial infarction
- heart failure
- cerebral ischemia
- nlrp inflammasome
- cancer therapy
- high fat diet induced
- cardiac resynchronization therapy
- acute ischemic stroke
- end stage renal disease
- newly diagnosed
- atrial fibrillation
- ejection fraction
- oxidative stress
- acute heart failure
- peritoneal dialysis
- type diabetes
- acute coronary syndrome
- percutaneous coronary intervention
- transcription factor
- mouse model
- current status
- structural basis
- replacement therapy