Orthophosphate increases the efficiency of slow muscle-myosin isoform in the presence of omecamtiv mecarbil.
Serena GovernaliMarco CaremaniCristina GallartIrene PerticiGer StienenGabriella PiazzesiCoen OttenheijmVincenzo LombardiMarco LinariPublished in: Nature communications (2020)
Omecamtiv mecarbil (OM) is a putative positive inotropic tool for treatment of systolic heart dysfunction, based on the finding that in vivo it increases the ejection fraction and in vitro it prolongs the actin-bond life time of the cardiac and slow-skeletal muscle isoforms of myosin. OM action in situ, however, is still poorly understood as the enhanced Ca2+-sensitivity of the myofilaments is at odds with the reduction of force and rate of force development observed at saturating Ca2+. Here we show, by combining fast sarcomere-level mechanics and ATPase measurements in single slow demembranated fibres from rabbit soleus, that the depressant effect of OM on the force per attached motor is reversed, without effect on the ATPase rate, by physiological concentrations of inorganic phosphate (Pi) (1-10 mM). This mechanism could underpin an energetically efficient reduction of systolic tension cost in OM-treated patients, whenever [Pi] increases with heart-beat frequency.
Keyphrases
- ejection fraction
- skeletal muscle
- heart failure
- aortic stenosis
- left ventricular
- single molecule
- blood pressure
- newly diagnosed
- end stage renal disease
- binding protein
- atrial fibrillation
- insulin resistance
- oxidative stress
- chronic kidney disease
- heart rate
- type diabetes
- prognostic factors
- protein kinase
- coronary artery disease
- aortic valve
- replacement therapy
- smoking cessation