Progression of Lung Inflammation and Damage in Rats After Cessation of Silica Inhalation

Porter, Dale W.; Hubbs, Ann F.; Mercer, Robert R.; Robinson, Victor A.; Ramsey, Dawn; McLaurin, Jeff; Khan, Amir; Battelli, Lori; Brumbaugh, Kurt; Teass, Alexander W.; Castranova, Vincent

doi:10.1093/toxsci/kfh110

Cited by 111 publications

(119 citation statements)

References 33 publications

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“…Silica exposure results in the induction of inflammation (Chen et al, 1999b;Fubini and Hubbard, 2003;Porter et al, 2004), and a definite role for inflammation in many of the toxic effects of silica has been demonstrated Porter et al, 2002). Induction of pulmonary inflammation, as evidenced from a significant increase in the number of AMs and PMNs as well as the activities of pro-inflammatory cytokines, MCP1 and MIP-2, was noticed in the rat lung tissue samples which were used in the current study to determine gene expression profile by microarray analysis (Sellamuthu et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

Mechanisms of crystalline silica-induced pulmonary toxicity revealed by global gene expression profiling

Sellamuthu¹,

Umbright²,

et al. 2011

Inhalation Toxicology

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A proper understanding of the mechanisms underlying crystalline silica-induced pulmonary toxicity has implications in the management and potential prevention of the adverse health effects associated with silica exposure including silicosis, cancer and several auto-immune diseases. Human lung type II epithelial cells and rat lungs exposed to crystalline silica were employed as experimental models to determine global gene expression changes in order to understand the molecular mechanisms underlying silica-induced pulmonary toxicity. The differential gene expression profile induced by silica correlated with its toxicity in the A549 cells. The biological processes perturbed by silica exposure in the A549 cells and rat lungs, as identified by the bioinformatics analysis of the differentially expressed genes, demonstrated significant similarity. Functional categorization of the differentially expressed genes identified cancer, cellular movement, cellular growth and proliferation, cell death, inflammatory response, cell cycle, cellular development, and genetic disorder as top ranking biological functions perturbed by silica exposure in A549 cells and rat lungs. Results of our study, in addition to confirming several previously identified molecular targets and mechanisms involved in silica toxicity, identified novel molecular targets and mechanisms potentially involved in silica-induced pulmonary toxicity. Further investigations, including those focused on the novel molecular targets and mechanisms identified in the current study may result in better management and, possibly, reduction and/or prevention of the potential adverse health effects associated with crystalline silica exposure.

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Section: Discussionmentioning

confidence: 99%

Mechanisms of crystalline silica-induced pulmonary toxicity revealed by global gene expression profiling

Sellamuthu¹,

Umbright²,

et al. 2011

Inhalation Toxicology

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“…It has been reported that nodular changes in the interstitium, lipoproteinosis and fibrosis are induced by intratracheal instillation of α -quartz to rats at higher dose levels than 1 mg 15,35) or by repeated inhalation exposure of rats to α -quartz at 15 mg/m 3 for 60 d 36) . However, no such lesions except fibrosis with alveolar wall thickening were found to occur in the lung of 160 m g quartz-dosed rats.…”

Section: Discussionmentioning

confidence: 99%

Pulmonary Toxicity of Intratracheally Instilled Multiwall Carbon Nanotubes in Male Fischer 344 Rats

et al. 2010

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“…Sacrifice was at the end of exposure and after 36 days' recovery. Pulmonary inflammation and PAP increased during the recovery period in rats exposed for 40 and 60 days but not 20 days; fibrosis developed even when exposure was stopped prior to its initial development (Porter et al 2004). Several inhalation studies in rats with various quartz molecules, and with exposure from 5 days to 13 weeks (Absher et al 1989;Arts et al 2007;Baggs, Ferin, and Oberdörster 1997;Driscoll et al 1991;Henderson et al 1995;Vallyathan et al 1995), one 4-week inhalation study in mice (Velan, Kumar, and Cohen 1993), and the 11-week study in guinea pigs mentioned above (Heppleston 1986) did not demonstrate PAP but showed inflammation and fibrosis.…”

Section: Silicon Dioxide/silica/quartzmentioning

confidence: 99%

Particle-induced Pulmonary Alveolar Proteinosis and Subsequent Inflammation and Fibrosis: A Toxicologic and Pathologic Review

Bomhard¹

2017

Toxicol Pathol

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This review analyzes the published data on cases of pulmonary alveolar proteinosis (PAP) in workers inhaling crystalline aluminum, indium, silicon, and titanium particles and possible sequelae, that is, inflammation and fibrosis, and compares these findings with those from animal experiments. In inhalation studies in rodents using crystalline indium and gallium compounds, pronounced PAP followed by inflammation and fibrosis down to very low concentration ranges have been reported. Crystalline aluminum, silicon, and titanium compounds also induced comparable pulmonary changes in animals, though at higher exposure levels. Laboratory animal species appear to react to the induction of PAP with varying degrees of sensitivity. The sensitivity of humans to environmental causes of PAP seems to be relatively low. Up to now, no cases of PAP, or other pulmonary diseases in humans, have been described for gallium compounds. However, a hazard potential can be assumed based on the results of animal studies. Specific particle properties, responsible for the induction of PAP and its sequelae, have not been identified. This review provides indications that, both in animal studies and in humans, PAP is not often recognized due to the absence of properly directed investigation or is concealed behind other forms of lung pathology.

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Progression of Lung Inflammation and Damage in Rats After Cessation of Silica Inhalation

Cited by 111 publications

References 33 publications

Mechanisms of crystalline silica-induced pulmonary toxicity revealed by global gene expression profiling

Mechanisms of crystalline silica-induced pulmonary toxicity revealed by global gene expression profiling

Pulmonary Toxicity of Intratracheally Instilled Multiwall Carbon Nanotubes in Male Fischer 344 Rats

Particle-induced Pulmonary Alveolar Proteinosis and Subsequent Inflammation and Fibrosis: A Toxicologic and Pathologic Review

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