Effects of Pathogenic Proline Mutations on Myosin Assembly

Overview

Journal J Mol Biol

Publisher Elsevier

Specialties Microbiology
Molecular Biology

Date 2011 Dec 14

PMID 22155079

Citations 13

Authors

Massimo Buvoli

Ada Buvoli

Leslie A Leinwand

Affiliations

Soon will be listed here.

Abstract

Laing distal myopathy (MPD1) is a genetically dominant myopathy characterized by early and selective weakness of the distal muscles. Mutations in the MYH7 gene encoding for the β-myosin heavy chain are the underlying genetic cause of MPD1. However, their pathogenic mechanisms are currently unknown. Here, we measure the biological effects of the R1500P and L1706P MPD1 mutations in different cellular systems. We show that, while the two mutations inhibit myosin self-assembly in non-muscle cells, they do not prevent incorporation of the mutant myosin into sarcomeres. Nevertheless, we find that the L1706P mutation affects proper antiparallel myosin association by accumulating in the bare zone of the sarcomere. Furthermore, bimolecular fluorescence complementation assay shows that the α-helix containing the R1500P mutation folds into homodimeric (mutant/mutant) and heterodimeric [mutant/wild type (WT)] myosin molecules that are competent for sarcomere incorporation. Both mutations also form aggregates consisting of cytoplasmic vacuoles surrounding paracrystalline arrays and amorphous rod-like inclusions that sequester WT myosin. Myosin aggregates were also detected in transgenic nematodes expressing the R1500P mutation. By showing that the two MPD1 mutations can have dominant effects on distinct components of the contractile apparatus, our data provide the first insights into the pathogenesis of the disease.

Citing Articles

A Laing distal myopathy-associated proline substitution in the β-myosin rod perturbs myosin cross-bridging activity.

Buvoli M, Wilson G, Buvoli A, Gugel J, Hau A, Bonnemann C J Clin Invest. 2024; 134(9).

PMID: 38690726 PMC: 11060730. DOI: 10.1172/JCI172599.

A novel MYH7 mutation resulting in Laing distal myopathy in a Chinese family.

Liu X, Zhang Y, Sun A, Zhong Y, Zheng D, Fan D Chin Med J (Engl). 2019; 132(7):856-859.

PMID: 30897599 PMC: 6595854. DOI: 10.1097/CM9.0000000000000148.

model of myosin myopathy rescued by overexpression of a TRIM-protein family member.

Dahl-Halvarsson M, Olive M, Pokrzywa M, Ejeskar K, Palmer R, Uv A Proc Natl Acad Sci U S A. 2018; 115(28):E6566-E6575.

PMID: 29946036 PMC: 6048496. DOI: 10.1073/pnas.1800727115.

A1603P and K1617del, Mutations in β-Cardiac Myosin Heavy Chain that Cause Laing Early-Onset Distal Myopathy, Affect Secondary Structure and Filament Formation In Vitro and In Vivo.

Parker F, Batchelor M, Wolny M, Hughes R, Knight P, Peckham M J Mol Biol. 2018; 430(10):1459-1478.

PMID: 29660325 PMC: 5958240. DOI: 10.1016/j.jmb.2018.04.006.

Design considerations in coiled-coil fusion constructs for the structural determination of a problematic region of the human cardiac myosin rod.

Andreas M, Ajay G, Gellings J, Rayment I J Struct Biol. 2017; 200(3):219-228.

PMID: 28743637 PMC: 9115891. DOI: 10.1016/j.jsb.2017.07.006.

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