Soluble iron modulates iron oxide particle-induced inflammatory responses via prostaglandin E2 synthesis: In vitro and in vivo studies

doi:10.1186/1743-8977-6-34

Particle and Fibre Toxicology

Volume 6

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Beck-Speier I
Kreyling WG
Maier KL
Dayal N
Schladweiler MC
Mayer P
Semmler-Behnke M
Kodavanti UP

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Kreyling WG
Maier KL
Dayal N
Schladweiler MC
Mayer P
Semmler-Behnke M
Kodavanti UP
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Soluble iron modulates iron oxide particle-induced inflammatory responses via prostaglandin E₂synthesis: In vitro and in vivo studies

Ingrid Beck-Speier¹ , Wolfgang G Kreyling¹^,2 , Konrad L Maier¹ , Niru Dayal¹ , Mette C Schladweiler³ , Paula Mayer¹^,2 , Manuela Semmler-Behnke¹^,2 and Urmila P Kodavanti³

¹Comprehensive Pneumology Center, Institute of Lung Biology and Disease, German Research Center for Environmental Health, D-85764 Neuherberg, Germany

²Focus Network Nanoparticles and Health, Helmholtz Center Munich - German Research Center for Environmental Health, D-85764 Neuherberg, Germany

³Environmental Public Health Division, National Health and Environmental Effects Research Laboratory, US Environmental Protection Agency, Research Triangle Park, NC 27711, USA

author email corresponding author email

Particle and Fibre Toxicology 2009, 6:34doi:10.1186/1743-8977-6-34


Published:	22 December 2009

Abstract

Background

Ambient particulate matter (PM)-associated metals have been shown to play an important role in cardiopulmonary health outcomes. To study the modulation of PM-induced inflammation by leached off metals, we investigated intracellular solubility of radio-labeled iron oxide (⁵⁹Fe₂O₃) particles of 0.5 and 1.5 μm geometric mean diameter. Fe₂O₃particles were examined for the induction of the release of interleukin 6 (IL-6) as pro-inflammatory and prostaglandin E₂(PGE₂) as anti-inflammatory markers in cultured alveolar macrophages (AM) from Wistar Kyoto (WKY) rats. In addition, we exposed male WKY rats to monodispersed Fe₂O₃particles by intratracheal instillation (1.3 or 4.0 mg/kg body weight) to examine in vivo inflammation.

Results

Particles of both sizes are insoluble extracellularly in the media but moderately soluble in AM with an intracellular dissolution rate of 0.0037 ± 0.0014 d^-1for 0.5 μm and 0.0016 ± 0.0012 d^-1for 1.5 μm ⁵⁹Fe₂O₃particles. AM exposed in vitro to 1.5 μm particles (10 μg/mL) for 24 h increased IL-6 release (1.8-fold; p < 0.05) and also PGE₂synthesis (1.9-fold; p < 0.01). By contrast, 0.5 μm particles did not enhance IL-6 release but strongly increased PGE₂synthesis (2.5-fold, p < 0.005). Inhibition of PGE₂synthesis by indomethacin caused a pro-inflammatory phenotype as noted by increased IL-6 release from AM exposed to 0.5 μm particles (up to 3-fold; p < 0.005). In the rat lungs, 1.5 but not 0.5 μm particles (4.0 mg/kg) induced neutrophil influx and increased vascular permeability.

Conclusions

Fe₂O₃particle-induced neutrophilic inflammatory response in vivo and pro-inflammatory cytokine release in vitro might be modulated by intracellular soluble iron via PGE₂synthesis. The suppressive effect of intracellular released soluble iron on particle-induced inflammation has implications on how ambient PM-associated but soluble metals influence pulmonary toxicity of ambient PM.