Highly Selective SERCA2a Activators: Preclinical Development of a Congeneric Group of First-in-Class Drug Leads against Heart Failure.
Andrea LuraghiMara FerrandiPaolo BarassiMartina AriciShih-Che HsuEleonora TorreCarlotta RonchiAlessio RomerioGwo-Jyh ChangPatrizia FerrariGiuseppe BianchiAntonio ZazaMarcella RocchettiFrancesco PeriPublished in: Journal of medicinal chemistry (2022)
The stimulation of sarcoplasmic reticulum calcium ATPase SERCA2a emerged as a novel therapeutic strategy to efficiently improve overall cardiac function in heart failure (HF) with reduced arrhythmogenic risk. Istaroxime is a clinical-phase IIb compound with a double mechanism of action, Na + /K + ATPase inhibition and SERCA2a stimulation. Starting from the observation that istaroxime metabolite PST3093 does not inhibit Na + /K + ATPase while stimulates SERCA2a, we synthesized a series of bioisosteric PST3093 analogues devoid of Na + /K + ATPase inhibitory activity. Most of them retained SERCA2a stimulatory action with nanomolar potency in cardiac preparations from healthy guinea pigs and streptozotocin (STZ)-treated rats. One compound was further characterized in isolated cardiomyocytes, confirming SERCA2a stimulation and in vivo showing a safety profile and improvement of cardiac performance following acute infusion in STZ rats. We identified a new class of selective SERCA2a activators as first-in-class drug candidates for HF treatment.
Keyphrases
- heart failure
- left ventricular
- acute heart failure
- endoplasmic reticulum
- low dose
- liver failure
- drug induced
- stem cells
- type diabetes
- mesenchymal stem cells
- intensive care unit
- oxidative stress
- cell therapy
- respiratory failure
- acute respiratory distress syndrome
- mechanical ventilation
- electronic health record
- aortic dissection
- diabetic nephropathy