Iron and infection: the heart of the matter

Bullen, J. J.; Rogers, H. J.; Spalding, Paul B.; Ward, C. Gillon

doi:10.1016/j.femsim.2004.11.010

Cited by 243 publications

(224 citation statements)

References 26 publications

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“…Although IV iron has been theoretically implicated as a cause of increased infections. 70,71 Hoen et al 72 prospectively examined 985 dialysis patients receiving IV iron as part of the regimen for dialysisassociated anemia and found that, while central venous catheters, history of bacteremia, arteriovenous grafts, and immunosuppression were associated with increased risk of infections, ferritin levels and total dose of IV iron administration were not. Furthermore, in the Anker study, patients with heart failure (a relatively high-risk group)-including approximately 40% with CKD in a 6-month placebo-controlled trial-had improvements in quality of life and functional status without an increase in infections.…”

Section: Potential Negative Effects Of IV Ironmentioning

confidence: 99%

Clinical Use of Intravenous Iron: Administration, Efficacy, and Safety

2010

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This section reviews the history, pharmacology, administration, efficacy, and toxicity of intravenous iron. Intravenous iron offers advantages over oral iron for the treatment of iron deficiency anemia across a wide range of disease states associated with absolute and functional iron deficiency. However, there remain concerns about the acute safety profiles of the available preparations and the potential for long-term toxicity with their repeated administration. Seven intravenous iron formulations are available. Confusion concerning the relative toxicities of the different formulations abounds. The similarities and differences are discussed. Iron repletion has been associated with adverse outcomes in infections. The relationship, if any, between intravenous iron administration and infections is reviewed. The potential advantages of total dose infusion (TDI), complete repletion in a single setting, are highlighted. A new paradigm for iron replacement therapy in iron deficiency anemia is presented.

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Section: Potential Negative Effects Of IV Ironmentioning

confidence: 99%

Clinical Use of Intravenous Iron: Administration, Efficacy, and Safety

2010

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“…A variety of serotypes have been identified among APEC, and strains of the same O-types (O1, 2, 4, 6, 7, 8, 16, 18 and 75) are also noticeably involved in UTIs Oelschlaeger et al, 2002;Bullen et al, 2005). The common presence of a set of virulence-associated genes among APEC and UPEC strains as well as similar disease patterns and phylogenetic background indicate a genetic relationship between APEC and UPEC isolates (Kaper et al, 2004;Moulin-Schouleur et al, 2006;Ron, 2006).…”

Section: Introductionmentioning

confidence: 99%

Comparison of virulence factors and expression of specific genes between uropathogenic Escherichia coli and avian pathogenic E. coli in a murine urinary tract infection model and a chicken challenge model

et al. 2009

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Avian pathogenic Escherichia coli (APEC) and uropathogenic E. coli (UPEC) establish infections in extraintestinal habitats of different hosts. As the diversity, epidemiological sources and evolutionary origins of extraintestinal pathogenic E. coli (ExPEC) are so far only partially defined, in the present study,100 APEC isolates and 202 UPEC isolates were compared by their content of virulence genes and phylogenetic groups. The two groups showed substantial overlap in terms of their serogroups, phylogenetic groups and virulence genotypes, including their possession of certain genes associated with large transmissible plasmids of APEC. In a chicken challenge model, both UPEC U17 and APEC E058 had similar LD 50 , demonstrating that UPEC U17 had the potential to cause significant disease in poultry. To gain further information about the similarities between UPEC and APEC, the in vivo expression of 152 specific genes of UPEC U17 and APEC E058 in both a murine urinary tract infection (UTI) model and a chicken challenge model was compared with that of these strains grown statically to exponential phase in rich medium. It was found that in the same model (murine UTI or chicken challenge), various genes of UPEC U17 and APEC E058 showed a similar tendency of expression. Several iron-related genes were upregulated in the UTI model and/or chicken challenge model, indicating that iron acquisition is important for E. coli to survive in blood or the urinary tract. Based on these results, the potential for APEC to act as human UPEC or as a reservoir of virulence genes for UPEC should be considered. Further, this study compared the transcriptional profile of virulence genes among APEC and UPEC in vivo.

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“…This phenomenon is considered to be a defense reaction depriving bacteria of iron. 13 Though mitochondrial function during sepsis and endotoxic shock has been studied extensively, results are contradictory. Mitochondrial function during septic/endotoxic shock depends on: (i) the source of mitochondria, (ii) the experimental induction of septic/endotoxic shock, and (iii) the phase of illness.…”

Section: Introductionmentioning

confidence: 99%

A novel endotoxin-induced pathway: upregulation of heme oxygenase 1, accumulation of free iron, and free iron-mediated mitochondrial dysfunction

Duvigneau

Piskernik

Haindl

et al. 2008

Laboratory Investigation

100

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Mitochondria are involved in the development of organ failure in critical care diseases. However, the mechanisms underlying mitochondrial dysfunction are not clear yet. Inducible hemoxygenase (HO-1), a member of the heat shock protein family, is upregulated in critical care diseases and considered to confer cytoprotection against oxidative stress. However, one of the products of HO-1 is Fe 2 þ which multiplies the damaging potential of reactive oxygen species catalyzing Fenton reaction. The aim of this study was to clarify the relevance of free iron metabolism to the oxidative damage of the liver in endotoxic shock and its impact on mitochondrial function. Endotoxic shock in rats was induced by injection of lipopolysaccharide (LPS) at a dose of 8 mg/kg (i.v.). We observed that the pro-inflammatory cytokine TNF-a and the liver necrosis marker aspartate aminotransferase were increased in blood, confirming inflammatory response to LPS and damage to liver tissue, respectively. The levels of free iron in the liver were significantly increased at 4 and 8 h after onset of endotoxic shock, which did not coincide with the decrease of transferrin iron levels in the blood, but rather with expression of the inducible form of heme oxygenase (HO-1). The proteins important for sequestering free iron (ferritin) and the export of iron out of the cells (ferroportin) were downregulated facilitating the accumulation of free iron in cells. The temporarily increased concentration of free iron in the liver correlated with the temporary impairment of both mitochondrial function and tissue ATP levels. Addition of exogenous iron ions to mitochondria isolated from control animals resulted in an impairment of mitochondrial respiration similar to that observed in endotoxic shock in vivo. Our data suggest that free iron released by HO-1 causes mitochondrial dysfunction in pathological situations accompanied by endotoxic shock.

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Iron and infection: the heart of the matter

Cited by 243 publications

References 26 publications

Clinical Use of Intravenous Iron: Administration, Efficacy, and Safety

Clinical Use of Intravenous Iron: Administration, Efficacy, and Safety

Comparison of virulence factors and expression of specific genes between uropathogenic Escherichia coli and avian pathogenic E. coli in a murine urinary tract infection model and a chicken challenge model

A novel endotoxin-induced pathway: upregulation of heme oxygenase 1, accumulation of free iron, and free iron-mediated mitochondrial dysfunction

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