Post‐translational modifications of vertebrate striated muscle myosin heavy chains

Author:

Morales Paula Nieto1,Coons Arianna N.2ORCID,Koopman Amelia J.2ORCID,Patel Sonu3,Chase P. Bryant2ORCID,Parvatiyar Michelle S.3,Pinto Jose R.1

Affiliation:

1. Department of Biomedical Sciences Florida State University College of Medicine Tallahassee Florida USA

2. Department of Biological Science Florida State University Tallahassee Florida USA

3. Department of Health, Nutrition and Food Sciences Florida State University Tallahassee Florida USA

Abstract

AbstractPost‐translational modifications (PTMs) play a crucial role in regulating the function of many sarcomeric proteins, including myosin. Myosins comprise a family of motor proteins that play fundamental roles in cell motility in general and muscle contraction in particular. A myosin molecule consists of two myosin heavy chains (MyHCs) and two pairs of myosin light chains (MLCs); two MLCs are associated with the neck region of each MyHC's N‐terminal head domain, while the two MyHC C‐terminal tails form a coiled‐coil that polymerizes with other MyHCs to form the thick filament backbone. Myosin undergoes extensive PTMs, and dysregulation of these PTMs may lead to abnormal muscle function and contribute to the development of myopathies and cardiovascular disorders. Recent studies have uncovered the significance of PTMs in regulating MyHC function and showed how these PTMs may provide additional modulation of contractile processes. Here, we discuss MyHC PTMs that have been biochemically and/or functionally studied in mammals' and rodents' striated muscle. We have identified hotspots or specific regions in three isoforms of myosin (MYH2, MYH6, and MYH7) where the prevalence of PTMs is more frequent and could potentially play a significant role in fine‐tuning the activity of these proteins.

Funder

National Heart, Lung, and Blood Institute

Publisher

Wiley

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