Thick filament protein network, functions, and disease association

L Wang, J Geist, A Grogan, LYR Hu… - Comprehensive …, 2018 - pmc.ncbi.nlm.nih.gov
L Wang, J Geist, A Grogan, LYR Hu, A Kontrogianni-Konstantopoulos
Comprehensive Physiology, 2018pmc.ncbi.nlm.nih.gov
Sarcomeres consist of highly ordered arrays of thick myosin and thin actin filaments along
with accessory proteins. Thick filaments occupy the center of sarcomeres where they
partially overlap with thin filaments. The sliding of thick filaments past thin filaments is a
highly regulated process that occurs in an ATP-dependent manner driving muscle
contraction. In addition to myosin that makes up the backbone of the thick filament, four other
proteins which are intimately bound to the thick filament, myosin binding protein-C, titin …
Sarcomeres consist of highly ordered arrays of thick myosin and thin actin filaments along with accessory proteins. Thick filaments occupy the center of sarcomeres where they partially overlap with thin filaments. The sliding of thick filaments past thin filaments is a highly regulated process that occurs in an ATP-dependent manner driving muscle contraction. In addition to myosin that makes up the backbone of the thick filament, four other proteins which are intimately bound to the thick filament, myosin binding protein-C, titin, myomesin, and obscurin play important structural and regulatory roles. Consistent with this, mutations in the respective genes have been associated with idiopathic and congenital forms of skeletal and cardiac myopathies. In this review, we aim to summarize our current knowledge on the molecular structure, subcellular localization, interacting partners, function, modulation via posttranslational modifications, and disease involvement of these five major proteins that comprise the thick filament of striated muscle cells.
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