| Literature DB >> 26792326 |
James A Spudich1, Tural Aksel2, Sadie R Bartholomew2, Suman Nag2, Masataka Kawana2, Elizabeth Choe Yu2, Saswata S Sarkar2, Jongmin Sung2, Ruth F Sommese2, Shirley Sutton2, Carol Cho2, Arjun S Adhikari2, Rebecca Taylor2, Chao Liu2, Darshan Trivedi2, Kathleen M Ruppel3.
Abstract
Hypertrophic cardiomyopathy is the most frequently occurring inherited cardiovascular disease, with a prevalence of more than one in 500 individuals worldwide. Genetically acquired dilated cardiomyopathy is a related disease that is less prevalent. Both are caused by mutations in the genes encoding the fundamental force-generating protein machinery of the cardiac muscle sarcomere, including human β-cardiac myosin, the motor protein that powers ventricular contraction. Despite numerous studies, most performed with non-human or non-cardiac myosin, there is no clear consensus about the mechanism of action of these mutations on the function of human β-cardiac myosin. We are using a recombinantly expressed human β-cardiac myosin motor domain along with conventional and new methodologies to characterize the forces and velocities of the mutant myosins compared with wild type. Our studies are extending beyond myosin interactions with pure actin filaments to include the interaction of myosin with regulated actin filaments containing tropomyosin and troponin, the roles of regulatory light chain phosphorylation on the functions of the system, and the possible roles of myosin binding protein-C and titin, important regulatory components of both cardiac and skeletal muscles.Entities:
Keywords: Cardiac myosin; Cardiomyopathy mutations; Force–velocity curves
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Year: 2016 PMID: 26792326 PMCID: PMC6514469 DOI: 10.1242/jeb.125930
Source DB: PubMed Journal: J Exp Biol ISSN: 0022-0949 Impact factor: 3.312