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1 Cardiovascular Institute and 2 Department of Molecular Genetics and 3 Center for Biological Imaging, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania 15213, and 4 Laboratory for Cancer Research, College of Pharmacy, Rutgers University, Piscataway, New Jersey 08854
Eph receptors constitute the
largest family of receptor tyrosine kinases. Multiple transcripts of
ephrin-A5, the cognate ligand of the EphA3 receptor, were found in
neonatal rat cardiomyocytes. Two cDNA clones encoding the full-length
ephrin-A5 (ephrin-A5
) and a 27-amino acid deletion form
(ephrin-A5
) were isolated. To examine the role of ephrin-A5 in
cardiomyocytes, the cDNAs were inserted into adenoviral vectors, termed
Ad.ephrin-A5
and Ad.ephrin-A5
, respectively, and overexpressed in
cardiomyocytes. The effect of ephrin-A5 on cardiomyocyte gene
expression was investigated using a cDNA expression array and Western
blot analysis. The results showed that both ephrin-A5
and
ephrin-A5
downregulated cyclin D2, cyclin-dependent kinase-4
proteins, and their cognate receptor EphA3, which were associated with
reduced bromodeoxyuridine incorporation in cardiomyocytes. Whereas
ephrin-A5
and ephrin-A5
also induced differential gene
expression, only ephrin-A5
significantly upregulated the
transcription of brain natriuretic peptide and downregulated ras-related protein RAB2, protein kinase C inhibitor protein-1, clusterin, and insulin-like growth factor-binding protein. The results suggest that the two forms of ephrin-A5 share similar function
while differ in regulating different sets of genes in cardiomyocytes.
Eph receptor tyrosine kinase; DNA synthesis; adenoviral gene transfer; gene expression array
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