NIMA-related kinase 9 regulates the phosphorylation of the essential myosin light chain in the heart

Abstract

To adapt to changing hemodynamic demands, regulatory mechanisms mod ulate actin-myosin-kinetics by calcium-dependent and-independent mechanisms. We investigate the posttranslational modification of human essential myosinlightchain(ELC)andidentifyNIMA-relatedkinase9(NEK9)to interact with ELC. NEK9 is highly expressed in the heart and the interaction with ELC is calcium-dependent. Silencing of NEK9 results in blunting of calcium-dependent ELC-phosphorylation. CRISPR/Cas9-mediated disruption of NEK9 leads to cardiomyopathy in zebrafish. Binding to ELC is mediated via the protein kinase domain of NEK9. A causal relationship between NEK9 activity and ELC-phosphorylation is demonstrated by genetic sensitizing in vivo. Finally, we observe significantly upregulated ELC-phosphorylation in dilated cardiomyopathy patients and provide a unique map of human ELC phosphorylation-sites. In summary, NEK9-mediated ELC-phosphorylation is a calcium-dependent regulatory system mediating cardiac contraction and inotropy.