Developing cardiac and skeletal muscle share fast-skeletal myosin heavy chain and cardiac troponin-I expression

Clause, KC and Tchao, J and Powell, MC and Liu, LJ and Huard, J and Keller, BB and Tobita, K (2012) Developing cardiac and skeletal muscle share fast-skeletal myosin heavy chain and cardiac troponin-I expression. PLoS ONE, 7 (7).

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Abstract

Skeletal muscle derived stem cells (MDSCs) transplanted into injured myocardium can differentiate into fast skeletal muscle specific myosin heavy chain (sk-fMHC) and cardiac specific troponin-I (cTn-I) positive cells sustaining recipient myocardial function. We have recently found that MDSCs differentiate into a cardiomyocyte phenotype within a three-dimensional gel bioreactor. It is generally accepted that terminally differentiated myocardium or skeletal muscle only express cTn-I or sk-fMHC, respectively. Studies have shown the presence of non-cardiac muscle proteins in the developing myocardium or cardiac proteins in pathological skeletal muscle. In the current study, we tested the hypothesis that normal developing myocardium and skeletal muscle transiently share both sk-fMHC and cTn-I proteins. Immunohistochemistry, western blot, and RT-PCR analyses were carried out in embryonic day 13 (ED13) and 20 (ED20), neonatal day 0 (ND0) and 4 (ND4), postnatal day 10 (PND10), and 8 week-old adult female Lewis rat ventricular myocardium and gastrocnemius muscle. Confocal laser microscopy revealed that sk-fMHC was expressed as a typical striated muscle pattern within ED13 ventricular myocardium, and the striated sk-fMHC expression was lost by ND4 and became negative in adult myocardium. cTn-I was not expressed as a typical striated muscle pattern throughout the myocardium until PND10. Western blot and RT-PCR analyses revealed that gene and protein expression patterns of cardiac and skeletal muscle transcription factors and sk-fMHC within ventricular myocardium and skeletal muscle were similar at ED20, and the expression patterns became cardiac or skeletal muscle specific during postnatal development. These findings provide new insight into cardiac muscle development and highlight previously unknown common developmental features of cardiac and skeletal muscle. © 2012 Clause et al.

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Details

Item Type:	Article
Status:	Published
Creators/Authors:	Creators Email Pitt Username ORCID Clause, KC Tchao, J Powell, MC Liu, LJ ljl4@pitt.edu LJL4 Huard, J Keller, BB Tobita, K kit3@pitt.edu KIT3
Contributors:	Contribution Contributors Name Email Pitt Username ORCID Editor Goumans, Marie Jose UNSPECIFIED UNSPECIFIED UNSPECIFIED
Centers:	Other Centers, Institutes, Offices, or Units > McGowan Institute for Regenerative Medicine
Date:	10 July 2012
Date Type:	Publication
Journal or Publication Title:	PLoS ONE
Volume:	7
Number:	7
DOI or Unique Handle:	10.1371/journal.pone.0040725
Schools and Programs:	School of Medicine > Developmental Biology School of Medicine > Orthopaedic Surgery Swanson School of Engineering > Bioengineering
Refereed:	Yes
Other ID:	NLM PMC3393685
PubMed Central ID:	PMC3393685
PubMed ID:	22808244
Date Deposited:	05 Oct 2012 19:08
Last Modified:	03 Feb 2019 01:55
URI:	http://d-scholarship.pitt.edu/id/eprint/15587

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