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Circulation Research. 2004
Published online before print March 4, 2004, doi: 10.1161/01.RES.0000125294.04612.81
A more recent version of this article appeared on April 2, 2004
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Submitted on January 22, 2004
Revised on February 18, 2004
Accepted on February 23, 2004

Evidence for Fusion Between Cardiac and Skeletal Muscle Cells

Hans Reinecke *; Elina Minami ; Veronica Poppa ; and Charles E. Murry

From the Department of Pathology, University of Washington, Seattle, Wash.

* To whom correspondence should be addressed. E-mail: hreineck{at}u.washington.edu.

Cardiomyoplasty with skeletal myoblasts may benefit cardiac function after infarction. Recent reports indicate that adult stem cells can fuse with other cell types. Because myoblasts are "fusigenic" cells by nature, we hypothesized they might be particularly likely to fuse with cardiomyocytes. To test this, neonatal rat cardiomyocytes labeled with LacZ and green fluorescent protein (GFP) were cocultured with unlabeled C2C12 myoblasts. After 3 days, we observed a small population of skeletal myotubes that expressed LacZ and GFP, indicating cell fusion. To test whether such fusion occurred in vivo, LacZ-expressing C2C12 myoblasts were grafted into normal nude mouse hearts. At 2 weeks after grafting, cells at the graft-host interface expressed both LacZ and cardiac-specific myosin light chain 2v (MLC2v). To test more definitively whether fusion between skeletal and cardiac muscle could occur, we used a Cre/lox reporter system that activated LacZ only on cell fusion. When neonatal cardiomyocytes from {alpha}-myosin heavy chain promoter ({alpha}-MHC)-Cre mice were cocultured with myoblasts from floxed-lacZ reporter mice, LacZ was activated in a subset of cells, indicating cell fusion occurred in vitro. Finally, we grafted the floxed-lacZ myoblasts into normal hearts of {alpha}-MHC-Cre+ and {alpha}-MHC-Cre- mice (n=5 each). Hearts analyzed at 4 days and 1 week after transplantation demonstrated activation of LacZ when the skeletal muscle cells were implanted into hearts of {alpha}-MHC-Cre+ mice, but not after implantation into {alpha}-MHC-Cre- mice. These data indicate that skeletal muscle cell grafting gives rise to a subpopulation of skeletal-cardiac hybrid cells with a currently unknown phenotype. The full text of this article is available online at http://circres.ahajournals.org.


Key words: cardiomyoplasty • skeletal myoblast • cell transplantation • cell fusion • Cre/lox




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