Literature DB >> 30622135

The human innate immune protein calprotectin induces iron starvation responses in Pseudomonas aeruginosa.

Emily M Zygiel1, Cassandra E Nelson2, Luke K Brewer2, Amanda G Oglesby-Sherrouse3,4, Elizabeth M Nolan5.   

Abstract

Most microbial pathogens have a metabolic iron requirement, necessitating the acquisition of this nutrient in the host. In response to pathogen invasion, the human host limits iron availability. Although canonical examples of nutritional immunity are host strategies that limit pathogen access to Fe(III), little is known about how the host restricts access to another biologically relevant oxidation state of this metal, Fe(II). This redox species is prevalent at certain infection sites and is utilized by bacteria during chronic infection, suggesting that Fe(II) withholding by the host may be an effective but unrecognized form of nutritional immunity. Here, we report that human calprotectin (CP; S100A8/S100A9 or MRP8/MRP14 heterooligomer) inhibits iron uptake and induces an iron starvation response in Pseudomonas aeruginosa cells by sequestering Fe(II) at its unusual His6 site. Moreover, under aerobic conditions in which the Fe(III) oxidation state is favored, Fe(II) withholding by CP was enabled by (i) its ability to stabilize this redox state in solution and (ii) the production and secretion of redox-active, P. aeruginosa-produced phenazines, which reduce Fe(III) to Fe(II). Analyses of the interplay between P. aeruginosa secondary metabolites and CP indicated that Fe(II) withholding alters P. aeruginosa physiology and expression of virulence traits. Lastly, examination of the effect of CP on cell-associated metal levels in diverse human pathogens revealed that CP inhibits iron uptake by several bacterial species under aerobic conditions. This work implicates CP-mediated Fe(II) sequestration as a component of nutritional immunity in both aerobic and anaerobic milieus during P. aeruginosa infection.
© 2019 Zygiel et al.

Entities:  

Keywords:  Pseudomonas aeruginosa (P. aeruginosa); bacteria; calprotectin; innate immunity; iron; metal homeostasis; metal sequestration; nutritional immunity; phenazine; virulence

Mesh:

Substances:

Year:  2019        PMID: 30622135      PMCID: PMC6416435          DOI: 10.1074/jbc.RA118.006819

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  63 in total

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  33 in total

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2.  Metal Sequestration and Antimicrobial Activity of Human Calprotectin Are pH-Dependent.

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Review 4.  Nutrient Zinc at the Host-Pathogen Interface.

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5.  Calcium Binding to the Innate Immune Protein Human Calprotectin Revealed by Integrated Mass Spectrometry.

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Review 6.  Multi-metal nutrient restriction and crosstalk in metallostasis systems in microbial pathogens.

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10.  Disruption of Phosphate Homeostasis Sensitizes Staphylococcus aureus to Nutritional Immunity.

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