Background: Disruption of Ca 2+ homeostasis is a key pathomechanism in heart failure. CaMKII-dependent hyperphosphorylation of ryanodine receptors in the sarcoplasmic reticulum (SR) increases the arrhythmogenic SR Ca 2+ leak and depletes SR Ca 2+ stores. The contribution of conversely acting serine/threonine phosphatases [protein phosphatase 1 (PP1) and 2A (PP2A)] is largely unknown. Methods and results: Human myocardium from three groups of patients was investigated: (i) healthy controls (non-failing, NF, n = 8), (ii) compensated hypertrophy (Hy, n = 16), and (iii) end-stage heart failure (HF, n = 52). Expression of PP1 was unchanged in Hy but greater in HF compared to NF while its endogenous inhibitor-1 (I-1) was markedly lower expressed in both compared to NF, suggesting increased total PP1 activity. In contrast, PP2A expression was lower in Hy and HF compared to NF. Ca 2+ homeostasis was severely disturbed in HF compared to Hy signified by a higher SR Ca 2+ leak, lower systolic Ca 2+ transients as well as a decreased SR Ca 2+ load. Inhibition of PP1/PP2A by okadaic acid increased SR Ca 2+ load and systolic Ca 2+ transients but severely aggravated diastolic SR Ca 2+ leak and cellular arrhythmias in Hy. Conversely, selective activation of PP1 by a PP1-disrupting peptide (PDP3) in HF potently reduced SR Ca 2+ leak as well as cellular arrhythmias and, importantly, did not compromise systolic Ca 2+ release and SR Ca 2+ load. Conclusion: This study is the first to functionally investigate the role of PP1/PP2A for Ca 2+ homeostasis in diseased human myocardium. Our data indicate that a modulation of phosphatase activity potently impacts Ca 2+ cycling properties. An activation of PP1 counteracts increased kinase activity in heart failure and successfully seals the arrhythmogenic SR Ca 2+ leak. It may thus represent a promising future antiarrhythmic therapeutic approach.
CITATION STYLE
Fischer, T. H., Eiringhaus, J., Dybkova, N., Saadatmand, A., Pabel, S., Weber, S., … Sossalla, S. (2018). Activation of protein phosphatase 1 by a selective phosphatase disrupting peptide reduces sarcoplasmic reticulum Ca 2+ leak in human heart failure. European Journal of Heart Failure, 20(12), 1673–1685. https://doi.org/10.1002/ejhf.1297
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