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Cardiac Troponin Activator CK-963 Increases Cardiac Contractility in Rats

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posted on 2024-03-07, 15:40 authored by Scott E. Collibee, Antonio Romero, Alexander R. Muci, Darren T. Hwee, Chihyuan Chuang, James J. Hartman, Alykhan S. Motani, Luke Ashcraft, Andre DeRosier, Mark Grillo, Qing Lu, Fady I. Malik, Bradley P. Morgan
Novel cardiac troponin activators were identified using a high throughput cardiac myofibril ATPase assay and confirmed using a series of biochemical and biophysical assays. HTS hit 2 increased rat cardiomyocyte fractional shortening without increasing intracellular calcium concentrations, and the biological target of 1 and 2 was determined to be the cardiac thin filament. Subsequent optimization to increase solubility and remove PDE-3 inhibition led to the discovery of CK-963 and enabled pharmacological evaluation of cardiac troponin activation without the competing effects of PDE-3 inhibition. Rat echocardiography studies using CK-963 demonstrated concentration-dependent increases in cardiac fractional shortening up to 95%. Isothermal calorimetry studies confirmed a direct interaction between CK-963 and a cardiac troponin chimera with a dissociation constant of 11.5 ± 3.2 μM. These results provide evidence that direct activation of cardiac troponin without the confounding effects of PDE-3 inhibition may provide benefit for patients with cardiovascular conditions where contractility is reduced.

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    Journal of Medicinal Chemistry

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    results provide evidenceenabled pharmacological evaluationcardiac troponin withoutcardiac troponin chimeracardiac troponin activatorcardiac thin filamentcardiac fractional shortening5 ± 3963 1 3 inhibition led2 increases cardiac contractility3 inhibitiondependent increases2 μmsubsequent optimizationincrease solubilityidentified usinghts hitdissociation constantdirect interactiondirect activationdemonstrated concentrationconfounding effectsconfirmed usingcompeting effectscardiovascular conditionsbiophysical assaysbiological target95 %.

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