Abstract
Phosphoenolpyruvate carboxykinase (PEPCK) is the rate-limiting enzyme for gluconeogenesis. To investigate underlying mechanisms of corticosteroid (CS) action in regulating glucose, temporal patterns of hepatic PEPCK gene expression, enzyme activity, and cAMP content were examined in adrenalectomized rats receiving acute and chronic methylprednisolone (MPL) treatments. After single MPL intravenous doses, PEPCK mRNA showed a fast increase, reaching a maximum at around 0.75 h, which was followed by an immediate decline to below baseline after 4 h, an apparent acute tolerance/rebound phenomenon. However, PEPCK enzyme showed continuous hyperactivity for over 72 h. This may be the result of generation of cAMP, an important inducer of PEPCK activity, which peaked at around 6 h. During 7-day subcutaneous infusion of MPL, PEPCK mRNA showed profiles consistent with single-dose results, whereas PEPCK activity increased to a comparable maximum followed by a slow decline. However, the extent of cAMP induction was markedly higher during infusion, which could be attributed to amplification of cAMP synthesis and/or a stabilizing effect of MPL on cAMP degradation. A pharmacokinetic/pharmacodynamic model was developed based on receptor/gene mechanisms of CS action. It successfully described the dual effects of MPL on regulating PEPCK message and the post-transcriptional control by cAMP. Our results exemplify the importance of the extent and duration of steroid exposure in mediating pharmacological effects. The model provides quantitation of multiple controlling factors regulating PEPCK and presents insights into its function in glucose metabolism.
Footnotes
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Financial support for this research was provided by Grant GM24211 from the National Institutes of Health.
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DOI: 10.1124/jpet.103.061515.
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ABBREVIATIONS: CS, corticosteroid; GR, glucocorticoid receptor; PK/PD, pharmacokinetic/pharmacodynamic; TAT, tyrosine aminotransferase; PEPCK, phosphoenolpyruvate carboxykinase; ADX, adrenalectomized; MPL, methylprednisolone; GRE, glucocorticoid-responsive element; TC, hypothetical transit biosignal; DR, cytosolic drug-receptor complex; DR(N), drug-receptor complex in nucleus.
- Received October 10, 2003.
- Accepted December 12, 2003.
- The American Society for Pharmacology and Experimental Therapeutics
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