TY - JOUR
T1 - Reactivation of cardiomyocyte cell cycle
T2 - A potential approach for myocardial regeneration
AU - McMullen, Nichole M.
AU - Gaspard, Gerard J.
AU - Pasumarthi, Kishore B.S.
PY - 2005
Y1 - 2005
N2 - Regulation of cardiomyocyte cell cycle appears to be more complex in mammals compared to the lower vertebrates. Cardiomyocytes from the adult newt and zebrafish can proliferate in response to myocardial injury and regenerate the damaged area. In contrast, cardiomyocytes in the mammalian heart cease to proliferate soon after birth. This limits the ability of the mammalian heart to regenerate the damaged myocardium following heart disease. It is believed that increasing the number of myocytes in a diseased heart can decrease scar formation and improve myocardial function. To this end, reactivation of cell cycle in the surviving myocardium may have therapeutic value in the treatment of heart disease. Here we provide a summary of studies describing myocyte cell cycle activity during development and disease, mechanisms of cell cycle exit in the adult heart and genetic modulations affecting cardiomyocyte cell cycle activity. Further, we discuss the potential utility of myocyte cell cycle reactivation in cardiac regeneration as well as improvement of myocardial function.
AB - Regulation of cardiomyocyte cell cycle appears to be more complex in mammals compared to the lower vertebrates. Cardiomyocytes from the adult newt and zebrafish can proliferate in response to myocardial injury and regenerate the damaged area. In contrast, cardiomyocytes in the mammalian heart cease to proliferate soon after birth. This limits the ability of the mammalian heart to regenerate the damaged myocardium following heart disease. It is believed that increasing the number of myocytes in a diseased heart can decrease scar formation and improve myocardial function. To this end, reactivation of cell cycle in the surviving myocardium may have therapeutic value in the treatment of heart disease. Here we provide a summary of studies describing myocyte cell cycle activity during development and disease, mechanisms of cell cycle exit in the adult heart and genetic modulations affecting cardiomyocyte cell cycle activity. Further, we discuss the potential utility of myocyte cell cycle reactivation in cardiac regeneration as well as improvement of myocardial function.
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U2 - 10.1002/sita.200400050
DO - 10.1002/sita.200400050
M3 - Review article
AN - SCOPUS:23844520335
SN - 1615-4053
VL - 5
SP - 126
EP - 141
JO - Signal Transduction
JF - Signal Transduction
IS - 3
ER -