Point mutations in the tri-helix bundle of the M-domain of cardiac myosin binding protein-C influence systolic duration and delay cardiac relaxation

Sabine J. van Dijk(University of Arizona), Samantha P. Harris(University of Arizona), Nathaniel C. Napierski(University of Arizona), Kristina B. Kooiker(University of Washington), Stacy Mazzalupo(University of Arizona), Katia Touma(University of Arizona)
Journal of Molecular and Cellular Cardiology
May 3, 2018
10.1016/j.yjmcc.2018.05.001
Cited by 23

Related Papers

Ablation of cardiac myosin binding protein-C disrupts the super-relaxed state of myosin in murine cardiomyocytes
|Journal of Molecular and Cellular Cardiology|2016|152
Physiological Mitochondrial Fragmentation Is a Normal Cardiac Adaptation to Increased Energy Demand
|Circulation Research|2017|143
Rapamycin persistently improves cardiac function in aged, male and female mice, even following cessation of treatment
|Aging Cell|2019|102
Early-Onset Hypertrophic Cardiomyopathy Mutations Significantly Increase the Velocity, Force, and Actin-Activated ATPase Activity of Human β-Cardiac Myosin
|Cell Reports|2016|94
β-Cardiac myosin hypertrophic cardiomyopathy mutations release sequestered heads and increase enzymatic activity
|Nature Communications|2019|90