Limited Role for the Bilirubin-Biliverdin Redox Amplification Cycle in the Cellular Antioxidant Protection by Biliverdin Reductase

Maghzal, Ghassan J.; Leck, Meng-Choo; Collinson, Emma J.; Li, Cheng; Stocker, Roland

doi:10.1074/jbc.m109.037119

Cited by 88 publications

(65 citation statements)

References 48 publications

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“…We propose the idea that GPS pathophysiology may be in part related to a suppressed hBVR activity and/or expression in the affected tissues that would result both in an attenuated ability to temper GPBP kinase activity and to generate the quencher of oxygen radicals, bilirubin (30). ROS have been shown to expose cryptic epitopes associated with autoimmune GPS (35) Furthermore, GPBP has been identified as a product of a human-specific TNF-␣-responsive transcriptional unit (4) and has been implicated in apoptotic pro-autoimmune signaling (44).…”

Section: Discussionmentioning

confidence: 99%

Human Biliverdin Reductase Suppresses Goodpasture Antigen-binding Protein (GPBP) Kinase Activity

Miralem

Gibbs

Revert

et al. 2010

Journal of Biological Chemistry

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The Ser/Thr/Tyr kinase activity of human biliverdin reductase (hBVR) and the expression of Goodpasture antigenbinding protein (GPBP), a nonconventional Ser/Thr kinase for the type IV collagen of basement membrane, are regulated by tumor necrosis factor (TNF-␣). The pro-inflammatory cytokine stimulates kinase activity of hBVR and activates NF-B, a transcriptional regulator of GPBP mRNA. Increased GPBP activity is associated with several autoimmune conditions, including Goodpasture syndrome. Here we show that in HEK293A cells hBVR binds to GPBP and down-regulates its TNF-␣-stimulated kinase activity; this was not due to a decrease in GPBP expression. Findings with small interfering RNA to hBVR and to the p65 regulatory subunit of NF-B show the hBVR role in the initial stimulation of GPBP expression by TNF-␣-activated NF-B; hBVR was not a factor in mediating GPBP mRNA stability. The interacting domain was mapped to the 281 CX 10 C motif in the C-terminal 24 residues of hBVR. A 7-residue peptide, KKRILHC 281 , corresponding to the core of the consensus D(␦)-Box motif in the interacting domain, was as effective as the intact 296-residue hBVR polypeptide in inhibiting GPBP kinase activity. GPBP neither regulated hBVR expression nor TNF-␣ dependent NF-B expression. Collectively, our data reveal that hBVR is a regulator of the TNF-␣-GPBP-collagen type IV signaling cascade and uncover a novel biological interaction that may be of relevance in autoimmune pathogenesis. Goodpasture syndrome (GPS)2 is a disorder mediated by autoantibody attack against the C-terminal noncollagenous-1 (NC1) domain of the ␣3 chain of the type IV collagen of basement membrane (␣3(IV)NC1) (Goodpasture antigen (GPA)). The NC1 domain initiates the braiding of the collagenous domains into a triple helical structure (protomer) and then mediates the assembly of two individual protomers yielding a quaternary structure known as the hexamer. The autoantibody epitope is cryptic in the hexamer, and the mechanism for its immunological exposure remains unknown. The autoimmune reaction results in deposits of autoantibodies along alveolar and glomerular basement membranes, causing lung hemorrhage and rapidly progressive glomerulonephritis, the two cardinal clinical manifestations of GPS (1, 2).Goodpasture antigen-binding protein (GPBP) is a nonconventional TNF-␣-inducible Ser/Thr kinase that targets the ␣3(IV)NC1 domain and regulates basement membrane collagen organization (3-6). Cells express at least two GPBP isoforms of 77 and 91 kDa. The 77-kDa GPBP polypeptide (GPBP in this report) interacts with type IV collagen, whereas the 91-kDa isoform associates with the cellular membrane and regulates extracellular levels of the 77-kDa polypeptide (7). In the present study we concentrated on the interaction of hBVR with the 77-kDa form of GPBP by transfecting cells with an expression plasmid encoding this form and using the cytoplasmic fraction of the cell lysate; hBVR is a soluble protein. GPBP phosphorylates GPA at its N terminus (6). Alterations in protein phosp...

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Section: Discussionmentioning

confidence: 99%

Human Biliverdin Reductase Suppresses Goodpasture Antigen-binding Protein (GPBP) Kinase Activity

Miralem

Gibbs

Revert

et al. 2010

Journal of Biological Chemistry

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“…34 Oxidation of bilirubin partly yields biliverdin, which is rapidly reduced back to bilirubin, but irreversible oxidation to other products also occurs. 35 These compounds, which are thought to promote vasospasm, are rapidly excreted in the urine. 36 However, in the present study, there was no distinct correlation with the inflammation marker hsCRP (Tables 4 and 5).…”

Section: Discussionmentioning

confidence: 99%

Plasma Bilirubin and UGT1A1*28 Are Not Protective Factors Against First-Time Myocardial Infarction in a Prospective, Nested Case–Referent Setting

Ekblom

Marklund

Jansson³

et al. 2010

Circ Cardiovasc Genet

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Background-Bilirubin, an effective antioxidant, shows a large variation in levels between individuals and has been positively associated with reduced cardiovascular disease risk. A major reason for the variability is a common promoter polymorphism, UGT1A1*28, which reduces the transcription of the enzyme that conjugates bilirubin, UDPglucuronosyltransferase 1A1. The aim of the study was to evaluate a possible protective effect of plasma bilirubin and the UGT1A1*28 polymorphism against myocardial infarction in a prospective case-referent setting. Methods and Results-Subjects (nϭ618) with a first-ever myocardial infarction (median event age, 60.5 years; median lag time, 3.5 years) and 1184 matched referents were studied. Plasma bilirubin was lower in cases versus referents. Despite a strong gene-dosage effect on bilirubin levels in both cases and referents, the UGT1A1*28 polymorphism did not influence the risk of myocardial infarction. Among multiple other variables, serum iron showed one of the strongest associations with bilirubin levels. Conclusions-We found no evidence for a protective effect of the UGT1A1*28 polymorphism against myocardial infarction and consequently neither for bilirubin. The lower bilirubin levels in cases might be caused by decreased production, increased degradation, or increased elimination. (Circ Cardiovasc Genet. 2010;3:340-347.)

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“…A multitude of studies have implicated Nrf2 in the induction of HO-1 during oxidative stress (Alam et al, 2003;Gong and Cederbaum, 2006a;Gong and Cederbaum, 2006b;Sun Jang et al, 2009). Finally, in two studies looking at the effects of oxidative stress (by hydrogen peroxide treatment), it was found that cell viability was only marginally affected (Baranano et al, 2002) or not affected at all (Maghzal et al, 2009) by silencing BVR (with interference RNA). The latter study also showed that BVR induction and over-expression also did not provide protection to the cells exposed to hydrogen peroxide.…”

Section: Anti-oxidant Protectionmentioning

confidence: 99%

“…Thus, BVR may have an important role in extending the antioxidant potency of bilirubin. It should be noted that a recent study concluded that the cytoprotective role of this redox cycle was limited as BVR overexpression and inhibition of BVR expression with antisense RNA did not seem to influence hydrogen peroxide-mediated cytotoxicity (Maghzal et al, 2009). It is now known that BVR also functions as a dual-specific kinase of serine/threonine and tyrosine residues in proteins, and in this capacity, BVR affects the signaling and cellular responses to a variety of stimuli (Reviewed in (Kapitulnik and Maines, 2009)).…”

Section: Bvr-catalyzed Redox Cycle With Lipid Peroxidesmentioning

confidence: 99%

Elucidating the Role of Biliverdin Reductase in the Expression of Heme Oxygenase-1 as a Cytoprotective Response to Stress

Reed¹

2012

Pharmacology

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Limited Role for the Bilirubin-Biliverdin Redox Amplification Cycle in the Cellular Antioxidant Protection by Biliverdin Reductase

Cited by 88 publications

References 48 publications

Human Biliverdin Reductase Suppresses Goodpasture Antigen-binding Protein (GPBP) Kinase Activity

Human Biliverdin Reductase Suppresses Goodpasture Antigen-binding Protein (GPBP) Kinase Activity

Plasma Bilirubin and UGT1A1*28 Are Not Protective Factors Against First-Time Myocardial Infarction in a Prospective, Nested Case–Referent Setting

Elucidating the Role of Biliverdin Reductase in the Expression of Heme Oxygenase-1 as a Cytoprotective Response to Stress

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