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The Comparative Pulmonary Toxicity of Beryllium Metal and Beryllium Oxide in Cynomolgus Monkeys

 

作者: HaleyP. J.,   PaviaK. F.,   SwaffordD. S.,   DavilaD. R.,   HooverM. D.,   FinchG. L.,  

 

期刊: Immunopharmacology and Immunotoxicology  (Taylor Available online 1994)
卷期: Volume 16, issue 4  

页码: 627-644

 

ISSN:0892-3973

 

年代: 1994

 

DOI:10.3109/08923979409019743

 

出版商: Taylor&Francis

 

数据来源: Taylor

 

摘要:

AbstractInhalation of beryllium (Be) may result in an immune-mediated, chronic granulomatous pulmonary disorder known as chronic beryllium disease (CBD). the physicochemical form of Be may affect the incidence and severity of CBD. We exposed cynomolgus monkeys, by bronchoscopic, intrabronchiolar instillation, to either beryllium oxide (BeO; heat-treated at 500°C) or Be metal at concentrations selected to achieve equimolar concentrations of available Be2+ions dissolving from the particles. Monkeys underwent bronchoalveolar lavage of the right and left diaphragmatic lobes at 14, 30, 60, 90, and 120 days post exposure (dpe). Monkeys were sacrificed at 80 and 180 dpe for evaluation of histopathological pulmonary changes. Numbers of lymphocytes from lung lobes of Be metal-exposed, but not BeO-exposed, monkeys were increased at 14, 30 and 90 dpe. Lung lymphocytes were increased for BeO exposed monkeys only at 60 dpe.In vitro, Be-specific, lung lymphocyte proliferation occurred at 14, 60, and 90 dpe for lymphocytes from Be metal-exposed lung lobes only. At no time were values from BeO-exposed lung lobes different from values from control lobes. Lung lesions in Be metal-exposed monkeys were characterized by focally intense, interstitial fibrosis, marked Type II cell hyperplasia, and variable lymphocyte infiltration. Some Be-metal-exposed monkeys had discrete immune granulomas consisting of tightly organized lymphocytic cuffs surrounding nodular aggregates of epithelioid macrophages. Lesions were rarely present in BeO-exposed monkeys and were much less severe. These data suggest that Be metal produces more severe pulmonary lesions than does BeO and that these lesions are accompanied by Be-specific immune responses.

 

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