EXCEED THE SPACE- PROVIDED. The broad objective of this proposal is to investigate the mechanisms by which growth hormone (GH) regulates | the sexually dimorphic expression of hepatic isoforms of cytochrome P450 (CYP), which impacts on concerns regarding the gender-effectiveness of therapeutic agents. Having identified the basic elements in the masculine: 'episodic' and feminine 'continuous' plasma GH profiles that selectively 'signal' the expression of 8 constitutive sex-dependent rat CYPs, we now propose to examine the mechanisms by which the hepatocyte discriminates between these numerous GH signals and transduces their messages to the nucleus. We hypothesize that each extracellular signal in the circulating GH profiles activates a different signal transduction pathway or different components in a signal transduction web, responsible for the induction or suppression of each isoform. We propose to identify the different signal transduction pathways mediating GH regulation of CYPs by both infusing GH-devoid rats and exposing primary rat hepatocytes to individual GH signals known to regulate expression of each CYP isoform. Similar experiments will be conducted to identify GH-dependent CYP isoforms in human hepatocytes and the signal transduction pathways mediating their action. Expression levels of hepatic CYPs are gender-dependent in the adult rat (as well as in every other species examined), and regardless of the treatment, males can not be induced to express the full female pattern of hepatic CYPs nor can females be treated to express the normal male pattern. We propose to investigate whether the sexually dimorphic CYP isoforms are permanently imprinted by determining the degree of CYP sex reversal in gender crossed (male to female and female to male) hepatocyte transplants as well as in rat and human hepatocyte cultures exposed to the GH profiles of the opposite sex. Follow-up studies will examine gender-based imprinting differences in the signal transduction responses to GH signals. I PERFORMANCE SITE ========================================Section End===========================================
Showing the most recent 10 out of 40 publications