CCAAT/enhancer-binding protein-alpha-dependent transactivation of CYP2C12 in rat hepatocytes

doi:10.1210/me.9.12.1771

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CCAAT/enhancer-binding protein-alpha-dependent transactivation of CYP2C12 in rat hepatocytes

P Tollet, O Lahuna, R Ahlgren, A Mode and JA Gustafsson
Department of Medical Nutrition Karolinska Institute Huddinge University Hospital, Sweden.

Expression of the rat CYP2C12 gene is liver specific and is induced by GH at the transcriptional level. In primary cultures of rat hepatocytes, GH inducibility of CYP2C12 and the presence of C/EBP alpha protein were demonstrated to be equally dependent on attachment of the cells to an extracellular matrix gel (Matrigel). Transient transfection of a C/EBP alpha expression vector into hepatocytes, cultured without Matrigel, increased the cellular P4502C12 messenger RNA levels 10-fold. Cotransfection studies using deletion constructs of the CYP2C12 promoter fused to the luciferase reporter gene localized the C/EBP alpha response to the region -250 to -180. Sequence comparisons and deoxyribonuclease I footprinting using rat liver nuclear extracts indicated two potential C/EBP binding sites in this region. Mutagenesis of the most upstream element (-229 to -207) abolished transactivation by C/EBP alpha. Using gel mobility supershift assays, this element was demonstrated to bind C/EBP alpha and C/EBP beta in liver nuclear extracts and in lysates from hepatocytes cultured on Matrigel. GH treatment of the cells did not alter the C/EBP protein levels or the C/EBP-binding activity to this element. Neither did GH increase the expression of CYP2C12 reporter gene constructs regardless of the presence of different amounts of cotransfected C/EBP alpha. We conclude that C/EBP alpha is a potent transactivator of the CYP2C12 gene and most likely contributes to its liver-specific expression. Although the results presented here do not exclude the possibility of a GH-enhanced transactivating ability of C/EBP alpha, the mechanism of GH-induced levels of P4502C12 is not through increased levels of C/EBP alpha or via enhanced DNA-binding activity of this transcription factor.

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Endocrinology	Endocrine Reviews	J. Clin. End. & Metab.
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				H. Schrem, J. Klempnauer, and J. Borlak Liver-Enriched Transcription Factors in Liver Function and Development. Part II: the C/EBPs and D Site-Binding Protein in Cell Cycle Control, Carcinogenesis, Circadian Gene Regulation, Liver Regeneration, Apoptosis, and Liver-Specific Gene Regulation Pharmacol. Rev., June 1, 2004; 56(2): 291 - 330. [Abstract] [Full Text] [PDF]

				M. C. Garcia, C. Thangavel, and B. H. Shapiro Epidermal Growth Factor Regulation of Female-Dependent CYP2A1 and CYP2C12 in Primary Rat Hepatocyte Culture Drug Metab. Dispos., February 1, 2001; 29(2): 111 - 120. [Abstract] [Full Text]

				M. Rastegar, G. G. Rousseau, and F. P. Lemaigre CCAAT/Enhancer-Binding Protein-{alpha} Is a Component of the Growth Hormone-Regulated Network of Liver Transcription Factors Endocrinology, May 1, 2000; 141(5): 1686 - 1692. [Abstract] [Full Text] [PDF]

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				O. Lahuna, L. Fernandez, H. Karlsson, D. Maiter, F. P. Lemaigre, G. G. Rousseau, J.-A. Gustafsson, and A. Mode Expression of hepatocyte nuclear factor 6�in rat liver is sex-dependent and regulated by growth�hormone PNAS, November 11, 1997; 94(23): 12309 - 12313. [Abstract] [Full Text] [PDF]

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CCAAT/enhancer-binding protein-alpha-dependent transactivation of CYP2C12 in rat hepatocytes