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Am J Physiol Cell Physiol 294: C1242-C1249, 2008. First published March 12, 2008; doi:10.1152/ajpcell.00529.2007
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RECEPTORS AND SIGNAL TRANSDUCTION

FGF-16 is released from neonatal cardiac myocytes and alters growth-related signaling: a possible role in postnatal development

Shun Yan Lu, David P. Sontag, Karen A. Detillieux, and Peter A. Cattini

Department of Physiology, University of Manitoba, Winnipeg, Manitoba, Canada

Submitted 7 November 2007 ; accepted in final form 10 March 2008

FGF-16 has been reported to be preferentially expressed in the adult rat heart. We have investigated the expression of FGF-16 in the perinatal and postnatal heart and its functional significance in neonatal rat cardiac myocytes. FGF-16 mRNA accumulation was observed by quantitative RT-PCR between neonatal days 1 and 7, with this increased expression persisting into adulthood. FGF-2 has been shown to increase neonatal rat cardiac myocyte proliferative potential via PKC activation. Gene array analysis revealed that FGF-16 inhibited the upregulation by FGF-2 of cell cycle promoting genes including cyclin F and Ki67. Furthermore, the CDK4/6 inhibitor gene Arf/INK4A was upregulated with the combination of FGF-16 and FGF-2 but not with either factor on its own. The effect on Ki67 was validated by protein immunodetection, which also showed that FGF-16 significantly decreased FGF-2-induced Ki67 labeling of cardiac myocytes, although it alone had no effect on Ki67 labeling. Inhibition of p38 MAPK potentiated cardiac myocyte proliferation induced by FGF-2 but did not alter the inhibitory action of FGF-16. Receptor binding assay showed that FGF-16 can compete with FGF-2 for binding sites including FGF receptor 1. FGF-16 had no effect on activated p38, ERK1/2, or JNK/SAPK after FGF-2 treatment. However, FGF-16 inhibited PKC-{alpha} and PKC-{varepsilon} activation induced by FGF-2 and, importantly, IGF-1. Collectively, these data suggest that expression and release of FGF-16 in the neonatal myocardium interfere with cardiac myocyte proliferative potential by altering the local signaling environment via modulation of PKC activation and cell cycle-related gene expression.

fibroblast growth factor; protein kinase C; Ki67


Address for reprint requests and other correspondence: P. Cattini, Dept. of Physiology, Univ. of Manitoba, 730 William Ave., Winnipeg, Manitoba, Canada R3E 3J7 (e-mail: peter_cattini{at}umanitoba.ca)






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