Structural basis for myopathic defects engendered by alterations in the myosin rod

Anthony Cammarato; Xiaochuan Li; Mary C. Reedy; Chi F. Lee; William Lehman; Sanford I. Bernstein

doi:10.1016/j.jmb.2011.10.019

Structural basis for myopathic defects engendered by alterations in the myosin rod

Anthony Cammarato, Xiaochuan Li, Mary C. Reedy, Chi F. Lee, William Lehman, Sanford I. Bernstein

School of Medicine

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

While mutations in the myosin subfragment 1 motor domain can directly disrupt the generation and transmission of force along myofibrils and lead to myopathy, the mechanism whereby mutations in the myosin rod influences mechanical function is less clear. Here, we used a combination of various imaging techniques and molecular dynamics simulations to test the hypothesis that perturbations in the myosin rod can disturb normal sarcomeric uniformity and, like motor domain lesions, would influence force production and propagation. We show that disrupting the rod can alter its nanomechanical properties and, in vivo, can drive asymmetric myofilament and sarcomere formation. Our imaging results indicate that myosin rod mutations likely disturb production and/or propagation of contractile force. This provides a unifying theory where common pathological cascades accompany both myosin motor and specific rod domain mutations. Finally, we suggest that sarcomeric inhomogeneity, caused by asymmetric thick filaments, could be a useful index of myopathic dysfunction.

Original language	English (US)
Pages (from-to)	477-484
Number of pages	8
Journal	Journal of molecular biology
Volume	414
Issue number	4
DOIs	https://doi.org/10.1016/j.jmb.2011.10.019
State	Published - Dec 9 2011

Keywords

electron microscopy
molecular dynamics
myopathy
myosin

ASJC Scopus subject areas

Molecular Biology
Biophysics
Structural Biology

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10.1016/j.jmb.2011.10.019

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title = "Structural basis for myopathic defects engendered by alterations in the myosin rod",

abstract = "While mutations in the myosin subfragment 1 motor domain can directly disrupt the generation and transmission of force along myofibrils and lead to myopathy, the mechanism whereby mutations in the myosin rod influences mechanical function is less clear. Here, we used a combination of various imaging techniques and molecular dynamics simulations to test the hypothesis that perturbations in the myosin rod can disturb normal sarcomeric uniformity and, like motor domain lesions, would influence force production and propagation. We show that disrupting the rod can alter its nanomechanical properties and, in vivo, can drive asymmetric myofilament and sarcomere formation. Our imaging results indicate that myosin rod mutations likely disturb production and/or propagation of contractile force. This provides a unifying theory where common pathological cascades accompany both myosin motor and specific rod domain mutations. Finally, we suggest that sarcomeric inhomogeneity, caused by asymmetric thick filaments, could be a useful index of myopathic dysfunction.",

keywords = "electron microscopy, molecular dynamics, myopathy, myosin",

author = "Anthony Cammarato and Xiaochuan Li and Reedy, {Mary C.} and Lee, {Chi F.} and William Lehman and Bernstein, {Sanford I.}",

note = "Funding Information: A.C. was funded by an American Heart Association Western States Affiliate Postdoctoral Fellowship and by the American Heart Association grant 10SDG4180089 ; W.L., by the National Institutes of Health grant HL36153 ; and S.I.B., by the National Institutes of Health grants AR43396 and GM32443 .",

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AU - Lee, Chi F.

AU - Lehman, William

AU - Bernstein, Sanford I.

N1 - Funding Information: A.C. was funded by an American Heart Association Western States Affiliate Postdoctoral Fellowship and by the American Heart Association grant 10SDG4180089 ; W.L., by the National Institutes of Health grant HL36153 ; and S.I.B., by the National Institutes of Health grants AR43396 and GM32443 .

PY - 2011/12/9

Y1 - 2011/12/9

N2 - While mutations in the myosin subfragment 1 motor domain can directly disrupt the generation and transmission of force along myofibrils and lead to myopathy, the mechanism whereby mutations in the myosin rod influences mechanical function is less clear. Here, we used a combination of various imaging techniques and molecular dynamics simulations to test the hypothesis that perturbations in the myosin rod can disturb normal sarcomeric uniformity and, like motor domain lesions, would influence force production and propagation. We show that disrupting the rod can alter its nanomechanical properties and, in vivo, can drive asymmetric myofilament and sarcomere formation. Our imaging results indicate that myosin rod mutations likely disturb production and/or propagation of contractile force. This provides a unifying theory where common pathological cascades accompany both myosin motor and specific rod domain mutations. Finally, we suggest that sarcomeric inhomogeneity, caused by asymmetric thick filaments, could be a useful index of myopathic dysfunction.

AB - While mutations in the myosin subfragment 1 motor domain can directly disrupt the generation and transmission of force along myofibrils and lead to myopathy, the mechanism whereby mutations in the myosin rod influences mechanical function is less clear. Here, we used a combination of various imaging techniques and molecular dynamics simulations to test the hypothesis that perturbations in the myosin rod can disturb normal sarcomeric uniformity and, like motor domain lesions, would influence force production and propagation. We show that disrupting the rod can alter its nanomechanical properties and, in vivo, can drive asymmetric myofilament and sarcomere formation. Our imaging results indicate that myosin rod mutations likely disturb production and/or propagation of contractile force. This provides a unifying theory where common pathological cascades accompany both myosin motor and specific rod domain mutations. Finally, we suggest that sarcomeric inhomogeneity, caused by asymmetric thick filaments, could be a useful index of myopathic dysfunction.

KW - electron microscopy

KW - molecular dynamics

KW - myopathy

KW - myosin

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Structural basis for myopathic defects engendered by alterations in the myosin rod

Abstract

Keywords

ASJC Scopus subject areas

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