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Matches in Nanopublications for { ?s ?p ?o <http://www.tkuhn.ch/bel2nanopub/RA0vXTsdUHDr0pea4XSfyYr8dfo-YMnHV-xZpzaNsBleA#provenance>. }

• _4 label "Selventa" provenance.
• large_corpus.bel rights "Copyright (c) 2011-2012, Selventa. All rights reserved." provenance.
• _3 value "With the use of fibroblasts, hepatoma cells, and macrophages in culture, NO has been shown to increase IRP RNA-binding activity, resulting in increased TfR-1 expression and reduced ferritin translation.1-5 The mechanism behind this increase in IRP RNA- binding activity may be a result of the NO-mediated depletion of cellular iron or the ability of NO to directly disassemble the [4Fe-4S] cluster of IRP-1 to increase RNA-binding activity.1,2 However, these studies con- flict with other investigations involving macrophages showing that inflammation or incubation with interferon /lipopolysaccharide leads to marked NO production that stimulates ferritin synthesis and decreases TfR-1 mRNA levels.6-10 This effect was caused by NO as inhibitors of nitric oxide synthase prevented the response. 10 Moreover, the increase in ferritin and decrease in TfR-1 expression were mediated by IRP-2, evidenced by a marked decrease in its RNA-binding activity.8-10 The findings of recent studies9,10 have suggested that the different effects of NO described above are a result of the various redox-related states of this molecule generated under different conditions, eg, the nitrosonium ion [NO+] and nitric oxide [NO-]. For instance, the effect of NO in mediating increased IRP RNA binding activity may be mediated by NO-; as it avidly binds iron and could result in iron release from IRP-1 and the cell.10 Exposure of macrophages to inflammatory cytokines may generate NO, which then S-nitrosylates IRP-2 and results in its degradation, leading to increased ferritin translation.10 However, further studies are required to confirm this hypothesis, as there is no direct evidence that IRP-2 is S-nitrosylated by NO The effects of hypoxia on iron metabolism can also be at least partly linked to the changes in RNA-binding activity of the IRPs. Indeed, IRP-1 RNA-binding activity has been shown to decrease in macrophages and hepatoma cells during hypoxia,11,12 and these conditions are known to increase ferritin expression.13" provenance.
• _3 wasQuotedFrom 12761471 provenance.
• assertion hadPrimarySource 12761471 provenance.
• large_corpus.bel title "BEL Framework Large Corpus Document" provenance.
• large_corpus.bel description "Approximately 61,000 statements." provenance.
• assertion wasDerivedFrom large_corpus.bel provenance.
• assertion wasDerivedFrom _3 provenance.
• large_corpus.bel authoredBy _4 provenance.
• large_corpus.bel version "20131211" provenance.