Cardiomyopathic mutations in essential light chain reveal mechanisms regulating the super relaxed state of myosin

Yoel H Sitbon; Francisca Diaz; Katarzyna Kazmierczak; Jingsheng Liang; Medhi Wangpaichitr; Danuta Szczesna-Cordary

doi:10.1085/jgp.202012801

Cardiomyopathic mutations in essential light chain reveal mechanisms regulating the super relaxed state of myosin

J Gen Physiol. 2021 Jul 5;153(7):e202012801. doi: 10.1085/jgp.202012801. Epub 2021 May 20.

Authors

Yoel H Sitbon¹, Francisca Diaz², Katarzyna Kazmierczak¹, Jingsheng Liang¹, Medhi Wangpaichitr³, Danuta Szczesna-Cordary¹

Affiliations

¹ Department of Molecular and Cellular Pharmacology, University of Miami Miller School of Medicine, Miami, FL.
² Department of Neurology, University of Miami Miller School of Medicine, Miami, FL.
³ VA Health Care System, Research Service, Miami, FL.

Abstract

In this study, we assessed the super relaxed (SRX) state of myosin and sarcomeric protein phosphorylation in two pathological models of cardiomyopathy and in a near-physiological model of cardiac hypertrophy. The cardiomyopathy models differ in disease progression and severity and express the hypertrophic (HCM-A57G) or restrictive (RCM-E143K) mutations in the human ventricular myosin essential light chain (ELC), which is encoded by the MYL3 gene. Their effects were compared with near-physiological heart remodeling, represented by the N-terminally truncated ELC (Δ43 ELC mice), and with nonmutated human ventricular WT-ELC mice. The HCM-A57G and RCM-E143K mutations had antagonistic effects on the ATP-dependent myosin energetic states, with HCM-A57G cross-bridges fostering the disordered relaxed (DRX) state and the RCM-E143K model favoring the energy-conserving SRX state. The HCM-A57G model promoted the switch from the SRX to DRX state and showed an ∼40% increase in myosin regulatory light chain (RLC) phosphorylation compared with the RLC of normal WT-ELC myocardium. On the contrary, the RCM-E143K-associated stabilization of the SRX state was accompanied by an approximately twofold lower level of myosin RLC phosphorylation compared with the RLC of WT-ELC. Upregulation of RLC phosphorylation was also observed in Δ43 versus WT-ELC hearts, and the Δ43 myosin favored the energy-saving SRX conformation. The two disease variants also differently affected the duration of force transients, with shorter (HCM-A57G) or longer (RCM-E143K) transients measured in electrically stimulated papillary muscles from these pathological models, while no changes were displayed by Δ43 fibers. We propose that the N terminus of ELC (N-ELC), which is missing in the hearts of Δ43 mice, works as an energetic switch promoting the SRX-to-DRX transition and contributing to the regulation of myosin RLC phosphorylation in full-length ELC mice by facilitating or sterically blocking RLC phosphorylation in HCM-A57G and RCM-E143K hearts, respectively.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Cardiomyopathies* / genetics
Cardiomyopathies* / metabolism
Cardiomyopathy, Hypertrophic* / genetics
Cardiomyopathy, Hypertrophic* / metabolism
Mice
Mutation
Myosin Light Chains / genetics
Myosin Light Chains / metabolism
Phosphorylation
Sarcomeres / metabolism

Substances

Myosin Light Chains

Abstract

Publication types

MeSH terms

Substances

Grants and funding