Coexpression of Mutant p53 and p193 Renders Embryonic Stem Cell-Derived Cardiomyocytes Responsive to the Growth-Promoting Activities of Adenoviral E1A

doi:10.1161/hh1001.090878

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Circulation Research. 2001;88:1004-1011
Published online before print May 10, 2001, doi: 10.1161/hh1001.090878

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	Apoptosis
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(Circulation Research. 2001;88:1004.)
© 2001 American Heart Association, Inc.

Molecular Medicine

Coexpression of Mutant p53 and p193 Renders Embryonic Stem Cell–Derived Cardiomyocytes Responsive to the Growth-Promoting Activities of Adenoviral E1A

Kishore B. S. Pasumarthi, Shih-Chong Tsai, Loren J. Field

From the Wells Center for Pediatric Research and Krannert Institute of Cardiology, Indiana University School of Medicine, Indianapolis, Ind. Present address of S.-C.T. is Institute of Biomedical Sciences, Academia Sinica, Taipei, Taiwan, Republic of China.

Correspondence to Dr Loren J. Field, Herman B Wells Center for Pediatric Research, James Whitcomb Riley Hospital for Children, 702 Barnhill Dr, Room 2600, Indianapolis, IN 46202-5225. E-mail ljfield{at}iupui.edu

Abstract—Expression of adenoviral E1A in cardiomyocytesresults in the activation of DNA synthesis followed by apoptosis.In contrast, expression of simian virus 40 large T antigen inducessustained cardiomyocyte proliferation. Previous studies haveshown that T antigen binds to 2 proapoptotic proteins in cardiomyocytes,namely the p53 tumor suppressor and p193 (a new member of theBH3-only proapoptosis subfamily). Structure-function analysesidentified a p193 C-terminal truncation mutant that encodesprosurvival activity. This mutant was used to test the roleof p193 in E1A-induced cardiomyocyte apoptosis. E1A inducedapoptosis in cardiomyocytes derived from differentiating embryonicstem cells. Expression of the prosurvival p193 mutant aloneor a mutant p53 alone did not block E1A-induced apoptosis. Incontrast, combinatorial expression of mutant p193 and mutantp53 blocked E1A-induced apoptosis, resulting in a proliferativeresponse indistinguishable from that seen with T antigen. Theseresults confirm the hypothesis that there are 2 proapoptoticpathways, encoded by p53 and p193, respectively, which restrictcardiomyocyte cell cycle activity in differentiating embryonicstem cell cultures. Furthermore, these results explain in molecularterms the phenotypic differences of E1A versus T-antigen genetransfer in cardiomyocytes.

Key Words: cardiomyocyte proliferation • cardiac myocyte apoptosis • heart regeneration

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