Cardiac resynchronization therapy restored maximal calcium-activated force and calcium sensitivity in failing dyssynchronous canine hearts through GSK-3β reactivation.
Does cardiac resynchronization therapy improve myofilament calcium responsiveness in a canine model of dyssynchronous heart failure?
CRT improves systolic function in dyssynchronous heart failure not just through macroscopic resynchronization, but by reactivating GSK-3β to restore myofilament calcium sensitivity.
Absolute Event Rate: 40.3% vs 21.5%
p-value: p=<0.001
Cardiac resynchronization therapy (CRT), the application of biventricular stimulation to correct discoordinate contraction, is the only heart failure treatment that enhances acute and chronic systolic function, increases cardiac work, and reduces mortality. Resting myocyte function also increases after CRT despite only modest improvement in calcium transients, suggesting that CRT may enhance myofilament calcium responsiveness. To test this hypothesis, we examined adult dogs subjected to tachypacing-induced heart failure for 6 weeks, concurrent with ventricular dyssynchrony (HF(dys)) or CRT. Myofilament force-calcium relationships were measured in skinned trabeculae and/or myocytes. Compared with control, maximal calcium-activated force and calcium sensitivity declined globally in HF(dys); however, CRT restored both. Phosphatase PP1 induced calcium desensitization in control and CRT-treated cells, while HF(dys) cells were unaffected, implying that CRT enhances myofilament phosphorylation. Proteomics revealed phosphorylation sites on Z-disk and M-band proteins, which were predicted to be targets of glycogen synthase kinase-3β (GSK-3β). We found that GSK-3β was deactivated in HF(dys) and reactivated by CRT. Mass spectrometry of myofilament proteins from HF(dys) animals incubated with GSK-3β confirmed GSK-3β–dependent phosphorylation at many of the same sites observed with CRT. GSK-3β restored calcium sensitivity in HF(dys), but did not affect control or CRT cells. These data indicate that CRT improves calcium responsiveness of myofilaments following HF(dys) through GSK-3β reactivation, identifying a therapeutic approach to enhancing contractile function
Kirk et al. (Sun,) conducted a other in Heart failure with dyssynchrony (canine model). Cardiac resynchronization therapy (CRT) vs. Dyssynchronous heart failure (HFdys) was evaluated on Maximal calcium-activated force (Fmax) in skinned myocytes (mN/mm2) (p=<0.001). Cardiac resynchronization therapy restored maximal calcium-activated force and calcium sensitivity in failing dyssynchronous canine hearts through GSK-3β reactivation.
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