The Muscle Thin Filament As a Classical Cooperative/allosteric Regulatory System

Overview

Journal J Mol Biol

Publisher Elsevier

Specialties Microbiology
Molecular Biology

Date 1998 May 22

PMID 9571024

Citations 82

Authors

S S Lehrer

M A Geeves

Affiliations

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Abstract

It is generally accepted that the regulation of muscle contraction involves cooperative and allosteric interactions among the protein components, actin, myosin, tropomyosin and troponin. But, as yet, the individual role of each component has not been clearly identified. Here we compare the properties of the components of the muscle regulatory system with the corresponding components of two systems, hemoglobin and aspartate transcarbamylase, that are well described by the classical Monod, Wyman and Changeux (MWC) model. The analogy indicates that actin is the catalytic subunit, tropomyosin is the regulatory subunit and troponin in the absence and presence of Ca2+ is the allosteric inhibitor and activator, respectively. The analogy additionally indicates that the substrate is myosin-ATP (or myosin-ADP-Pi) rather than ATP. Also, in contrast to other MWC systems, the activating ligand for actin-tropomyosin is a myosin-nucleotide intermediate or product that binds tightly to actin, rather than the substrate which binds weakly. This tightly bound intermediate switches the system from the off-state to the on-state (T to R-state in MWC nomenclature) in a concerted transition, affecting n actin subunits, allowing force to be developed.

Citing Articles

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High-resolution cryo-EM structure of the junction region of the native cardiac thin filament in relaxed state.

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Single-molecule imaging reveals the concerted release of myosin from regulated thin filaments.

Smith Q, Inchingolo A, Mihailescu M, Dai H, Kad N Elife. 2021; 10.

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