Abstract

The heme metabolic pathway is exquisitely responsive to environmental agents, including metal and porphyrin complexes. Biliverdin reductase (BVR) catalyzes the final step in the pathway. In the past BVR, its substrate, biliverdin, and its product (bilirubin) were considered solely in context of disposal of heme degradation products. Recent findings have alluded to their relevance to a wide range of functions in the cell. Bilirubin is an intracellular antioxidant; biliverdin, product of HO-1 and HO-2 activity, suppresses gene expression and underlies the frequently morbid """"""""green jaundice."""""""" During the past funding period we demonstrated human BVR is a major component of signal transduction pathways: it is a serine/threonine /tyrosine kinase that is activated by phosphorylation in response to oxidative stress and translocates into the nucleus in response to free radicals, cytokines and cAMP, and in tumorigenesis. In the nucleus, BVR functions as a regulator for expression of AP-1 and cAMP target genes that includes HO-1, c-Jun, and ATF-2/CREB.Gene array analysis identifies other genes crucial to signaling and cytoprotection affected by BVR. BVR is a leucine-zipper transcription factor that binds to AP-1 site; biliverdin inhibits its DNA binding. BVR is a substrate for insulin receptor kinase (IRK), is a kinase for IR substrate and, protects against As (III)- mediated apoptosis. Initial studies show: BVR activates PKC, has PKB/Akt activity, binds to PKC and ERK1/2, and promotes cell differentiation; the effects are not cell line specific. Collectively, these findings reveal a previously unrecognized vital component of cell signaling and cytoprotection. The overall objective of this application is to investigate the mechanism and consequences of BVR modulation of cell signaling by the two major arms of insulin receptor/growth factor cascade: the phosphoinositol-3-kinase (PI3-K) and MAPK/ERK pathways, which are linked by PKC. To achieve this objective, 4 aims are proposed: 1) To define role of BVR in the IRK-mediated activation of PI3-K component of insulin/IGF-1 signaling pathway; 2) To examine regulation of MAPK/ERK component of this pathway by BVR; 3) To further define activation of PKC enzymes by BVR; and, 4) To examine in vivo regulation of insulin/IGF signaling by BVR and biliverdin. For this, mice null for BVR gene will be generated to examine effects of phenylhydrazine and As (III), which are diabetogenic and promote cell death, on glucose metabolism and apoptosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
2R01ES004066-20
Application #
7049690
Study Section
Special Emphasis Panel (ZRG1-DIG-F (02))
Program Officer
Maull, Elizabeth A
Project Start
1985-12-06
Project End
2010-11-30
Budget Start
2005-12-19
Budget End
2006-11-30
Support Year
20
Fiscal Year
2006
Total Cost
$372,222
Indirect Cost

  Institution

Name
University of Rochester
Department
Biochemistry
Type
Schools of Dentistry
DUNS #
041294109
City
Rochester
State
NY
Country
United States
Zip Code
14627

  Publications

Miralem, Tihomir; Lerner-Marmarosh, Nicole; Gibbs, Peter E M et al. (2016) Interaction of human biliverdin reductase with Akt/protein kinase B and phosphatidylinositol-dependent kinase 1 regulates glycogen synthase kinase 3 activity: a novel mechanism of Akt activation. FASEB J 30:2926-44
Gibbs, Peter E M; Lerner-Marmarosh, Nicole; Poulin, Amelia et al. (2014) Human biliverdin reductase-based peptides activate and inhibit glucose uptake through direct interaction with the kinase domain of insulin receptor. FASEB J 28:2478-91
Gibbs, Peter E M; Tudor, Cicerone; Maines, Mahin D (2012) Biliverdin reductase: more than a namesake - the reductase, its Peptide fragments, and biliverdin regulate activity of the three classes of protein kinase C. Front Pharmacol 3:31
Miralem, Tihomir; Lerner-Marmarosh, Nicole; Gibbs, Peter E M et al. (2012) The human biliverdin reductase-based peptide fragments and biliverdin regulate protein kinase C? activity: the peptides are inhibitors or substrate for the protein kinase C. J Biol Chem 287:24698-712
Kapitulnik, Jaime; Maines, Mahin D (2012) The role of bile pigments in health and disease: effects on cell signaling, cytotoxicity, and cytoprotection. Front Pharmacol 3:136
Gibbs, Peter E M; Miralem, Tihomir; Lerner-Marmarosh, Nicole et al. (2012) Formation of ternary complex of human biliverdin reductase-protein kinase C?-ERK2 protein is essential for ERK2-mediated activation of Elk1 protein, nuclear factor-?B, and inducible nitric-oxidase synthase (iNOS). J Biol Chem 287:1066-79
Ding, Bo; Gibbs, Peter E M; Brookes, Paul S et al. (2011) The coordinated increased expression of biliverdin reductase and heme oxygenase-2 promotes cardiomyocyte survival: a reductase-based peptide counters *-adrenergic receptor ligand-mediated cardiac dysfunction. FASEB J 25:301-13
Gibbs, Peter E M; Miralem, Tihomir; Maines, Mahin D (2010) Characterization of the human biliverdin reductase gene structure and regulatory elements: promoter activity is enhanced by hypoxia and suppressed by TNF-alpha-activated NF-kappaB. FASEB J 24:3239-54
Maines, Mahin D (2010) Potential application of biliverdin reductase and its fragments to modulate insulin/IGF-1/MAPK/PI3-K signaling pathways in therapeutic settings. Curr Drug Targets 11:1586-94
Miralem, Tihomir; Gibbs, Peter E M; Revert, Fernando et al. (2010) Human biliverdin reductase suppresses Goodpasture antigen-binding protein (GPBP) kinase activity: the reductase regulates tumor necrosis factor-alpha-NF-kappaB-dependent GPBP expression. J Biol Chem 285:12551-8

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