Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.

Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.

The fundamental importance of the proteoglycan versican to early heart formation was clearly demonstrated by the Vcan null mouse called heart defect (hdf). Total absence of the Vcan gene halts heart development at a stage prior to the heart's pulmonary/aortic outlet segment growth. This creates...

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Main Authors: Tara A Burns, Maria T Dours-Zimmermann, Dieter R Zimmermann, Edward L Krug, Susana Comte-Walters, Leticia Reyes, Monica A Davis, Kevin L Schey, John H Schwacke, Christine B Kern, Corey H Mjaatvedt
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3930639?pdf=render
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spelling doaj-f01157296f4d4bc59fa661dd338ebacd2020-11-25T02:15:26ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0192e8913310.1371/journal.pone.0089133Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.Tara A BurnsMaria T Dours-ZimmermannDieter R ZimmermannEdward L KrugSusana Comte-WaltersLeticia ReyesMonica A DavisKevin L ScheyJohn H SchwackeChristine B KernCorey H MjaatvedtThe fundamental importance of the proteoglycan versican to early heart formation was clearly demonstrated by the Vcan null mouse called heart defect (hdf). Total absence of the Vcan gene halts heart development at a stage prior to the heart's pulmonary/aortic outlet segment growth. This creates a problem for determining the significance of versican's expression in the forming valve precursors and vascular wall of the pulmonary and aortic roots. This study presents data from a mouse model, Vcan ((tm1Zim)), of heart defects that results from deletion of exon 7 in the Vcan gene. Loss of exon 7 prevents expression of two of the four alternative splice forms of the Vcan gene. Mice homozygous for the exon 7 deletion survive into adulthood, however, the inability to express the V2 or V0 forms of versican results in ventricular septal defects, smaller cushions/valve leaflets with diminished myocardialization and altered pulmonary and aortic outflow tracts. We correlate these phenotypic findings with a large-scale differential protein expression profiling to identify compensatory alterations in cardiac protein expression at E13.5 post coitus that result from the absence of Vcan exon 7. The Vcan ((tm1Zim)) hearts show significant changes in the relative abundance of several cytoskeletal and muscle contraction proteins including some previously associated with heart disease. These alterations define a protein fingerprint that provides insight to the observed deficiencies in pre-valvular/septal cushion mesenchyme and the stability of the myocardial phenotype required for alignment of the outflow tract with the heart ventricles.http://europepmc.org/articles/PMC3930639?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Tara A Burns
Maria T Dours-Zimmermann
Dieter R Zimmermann
Edward L Krug
Susana Comte-Walters
Leticia Reyes
Monica A Davis
Kevin L Schey
John H Schwacke
Christine B Kern
Corey H Mjaatvedt
spellingShingle Tara A Burns
Maria T Dours-Zimmermann
Dieter R Zimmermann
Edward L Krug
Susana Comte-Walters
Leticia Reyes
Monica A Davis
Kevin L Schey
John H Schwacke
Christine B Kern
Corey H Mjaatvedt
Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
PLoS ONE
author_facet Tara A Burns
Maria T Dours-Zimmermann
Dieter R Zimmermann
Edward L Krug
Susana Comte-Walters
Leticia Reyes
Monica A Davis
Kevin L Schey
John H Schwacke
Christine B Kern
Corey H Mjaatvedt
author_sort Tara A Burns
title Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
title_short Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
title_full Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
title_fullStr Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
title_full_unstemmed Imbalanced expression of Vcan mRNA splice form proteins alters heart morphology and cellular protein profiles.
title_sort imbalanced expression of vcan mrna splice form proteins alters heart morphology and cellular protein profiles.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description The fundamental importance of the proteoglycan versican to early heart formation was clearly demonstrated by the Vcan null mouse called heart defect (hdf). Total absence of the Vcan gene halts heart development at a stage prior to the heart's pulmonary/aortic outlet segment growth. This creates a problem for determining the significance of versican's expression in the forming valve precursors and vascular wall of the pulmonary and aortic roots. This study presents data from a mouse model, Vcan ((tm1Zim)), of heart defects that results from deletion of exon 7 in the Vcan gene. Loss of exon 7 prevents expression of two of the four alternative splice forms of the Vcan gene. Mice homozygous for the exon 7 deletion survive into adulthood, however, the inability to express the V2 or V0 forms of versican results in ventricular septal defects, smaller cushions/valve leaflets with diminished myocardialization and altered pulmonary and aortic outflow tracts. We correlate these phenotypic findings with a large-scale differential protein expression profiling to identify compensatory alterations in cardiac protein expression at E13.5 post coitus that result from the absence of Vcan exon 7. The Vcan ((tm1Zim)) hearts show significant changes in the relative abundance of several cytoskeletal and muscle contraction proteins including some previously associated with heart disease. These alterations define a protein fingerprint that provides insight to the observed deficiencies in pre-valvular/septal cushion mesenchyme and the stability of the myocardial phenotype required for alignment of the outflow tract with the heart ventricles.
url http://europepmc.org/articles/PMC3930639?pdf=render
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