Neonatal jaundice is a condition that effects children throughout the world. Pathologic jaundice becomes a serious threat to the well-being of neonates in the context of hemolytic disease which is associated with increased bilirubin production. Our laboratory's approach to this problem is to monitor bilirubin production, and assess the efficacy of therapeutic agents that inhibit the activity of key enzymes, heme oxygenase isoenzymes 1 and 2 (HO-1,2), in the catalyses of heme to bilirubin. Expression of the HO-1 isoenzyme varies both in culture and in vivo in response to metabolic cues such as changes in heme concentrations. Metalloporphyrins, heme analogs, are clinically relevant inhibitors of HO enzymatic activity, but some have also been shown to increase HO-1 expression at the level of transcription which may offset therapeutic uses. Here we propose to address the regulation of HO transcription in culture and living animals in the presence and absence of enzyme inhibitors. This proposal contains three specific aims. First, full length, truncated, and condensed HO-1 promoters will be placed upstream of the luciferase coding sequence, and stable cell lines will be generated from this set of promoter-reporter gene fusions. The activity of the HO-1 promoter will be assessed in culture and compared to previously described patterns of expression to map regions of this promoter that respond to specific stimuli. Second, a selected series of metalloporphyrins with potential clinical use will be tested for effects on HO-1 transcription and enzyme activity in culture. Lastly, using our recently developed in vivo monitoring method, modulators of HO gene expression will be evaluated in living animals to determine the in vivo effects of inhibitors of HO enzymatic activity in real time. Differential regulation of both HO isoenzymes will be compared, first in culture and then in living animals, using luciferase reporters with two different colors of emission. An inability to correlate in vitro or cell culture data with in vivo observations is a familiar problem in biological chemistry. Here we attempt to address this issue using an integrated approach where the same set of reporter constructs is used in vitro and in vivo, and similarly monitored in both environments. As such, this proposal describes analyses of HO expression that will allow more precise hypotheses about gene expression and specific pathway inhibition. We can then combine this data without knowledge of pharmacologic properties of HO inhibitors to select compounds that control hyperbilirubinemia and prevent or treat neonatal jaundice.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL058013-03
Application #
6184350
Study Section
Human Embryology and Development Subcommittee 1 (HED)
Project Start
1998-07-10
Project End
2002-06-30
Budget Start
2000-07-01
Budget End
2001-06-30
Support Year
3
Fiscal Year
2000
Total Cost
$146,242
Indirect Cost
Name
Stanford University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305
Cohen, Ronald S; Wong, Ronald J; Stevenson, David K (2010) Understanding neonatal jaundice: a perspective on causation. Pediatr Neonatol 51:143-8
Stevenson, David K; Wong, Ronald J (2010) Metalloporphyrins in the management of neonatal hyperbilirubinemia. Semin Fetal Neonatal Med 15:164-8
Vreman, Hendrik J; Knauer, Yuri; Wong, Ronald J et al. (2009) Dermal carbon monoxide excretion in neonatal rats during light exposure. Pediatr Res 66:66-9
Morisawa, Takeshi; Wong, Ronald J; Bhutani, Vinod K et al. (2008) Inhibition of heme oxygenase activity in newborn mice by azalanstat. Can J Physiol Pharmacol 86:651-9
Oh, Joo Yeun; Giles, Niroshini; Landar, Aimee et al. (2008) Accumulation of 15-deoxy-delta(12,14)-prostaglandin J2 adduct formation with Keap1 over time: effects on potency for intracellular antioxidant defence induction. Biochem J 411:297-306
Abate, Aida; Zhao, Hui; Wong, Ronald J et al. (2007) The role of Bach1 in the induction of heme oxygenase by tin mesoporphyrin. Biochem Biophys Res Commun 354:757-63
Lin, Yong; Vreman, Hendrik J; Wong, Ronald J et al. (2007) Heme oxygenase-1 stabilizes the blood-spinal cord barrier and limits oxidative stress and white matter damage in the acutely injured murine spinal cord. J Cereb Blood Flow Metab 27:1010-21
Vreman, Hendrik J; Wong, Ronald J; Chan, Miu L et al. (2006) Transcutaneous bilirubinometry: a noninvasive tool for studying newborn jaundiced rats before and after exposure to light. Pediatr Res 59:203-9
Kinobe, Robert T; Vlahakis, Jason Z; Vreman, Hendrik J et al. (2006) Selectivity of imidazole-dioxolane compounds for in vitro inhibition of microsomal haem oxygenase isoforms. Br J Pharmacol 147:307-15
DeSandre, Glenn H; Wong, Ronald J; Morioka, Ichiro et al. (2006) The effectiveness of oral tin mesoporphyrin prophylaxis in reducing bilirubin production after an oral heme load in a transgenic mouse model. Biol Neonate 89:139-46

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