Chronic Inhalation Toxicity of Size-Separated Glass Fibers in Fischer 344 Rats
Autor: | P. Thevenaz, E. E. McConnell, J. G. Hadley, T. W. Hesterberg, R. Anderson, J. Chevalier, David M. Bernstein, W. C. Miiller |
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Rok vydání: | 1993 |
Předmět: |
Lung Diseases
Male Ceramics Pathology medicine.medical_specialty Lung Neoplasms Asbestos Serpentine Pulmonary Fibrosis Toxicology medicine.disease_cause Asbestos Pulmonary fibrosis Chrysotile Parenchyma medicine Animals Mesothelioma Particle Size Aerosols Lung Inhalation Chemistry medicine.disease Rats Inbred F344 Rats medicine.anatomical_structure Toxicity Body Burden Glass |
Zdroj: | Fundamental and Applied Toxicology. 20:464-476 |
ISSN: | 0272-0590 |
Popis: | Chronic Inhalation Toxicity of Size Separated Glass Fibers in Fischer 344 Rats. Hesterberg, T. W., Muller, W. C., McConnell E. E., Chevalier, J., Hadley, J. G., Bernstein, D. M., Thevenaz, P., and Anderson, R. (1993). Fundam. Appl. Toxicol. 20, 464-476. This is study was initiated to determine the chronic biological effects in Fisher 344 rats of inhaled size-separated respirable fractions of fibrous glass (FG) having compositions representative of common building insulation wools. Rats were exposed using nose-only inhalation chambers, 6 hr/day, 5 days/week, for 24 months to three concentrations(3, 16, and 30mg/m3)of two different compositions of FG (designated MMVF 10 and MMVF 11), or to filtered air (negative control). Fibrous glass findings were compared to those from a concurrent inhalation study of chrysotile asbestos and refractory ceramic fiber (RCF). The FGs used in this study were size selected to be largely respirable in the rat and the aerosol generation technique did not alter the dimensions of the fibers. Interim euthanizations look place at 3- to 6-month intervals to monitor progression of pulmonary changes. Fibers were recovered from digested lung tissue for determination of changes in fiber number and morphology. In animals exposed to 30 mg/m3 of MMVF 10 or MMVF 11, 4.2 ± 0.9 × 105 and 6.4 ±3. 1 × 105 fibers/mg dry lung tissue, respectively, were recovered after 24 months of exposure. Exposure to chrysotile asbestos (10 mg/m3) and to a lesser extent RCF (30 mg/m3) resulted in pulmonary fibrosis as well as mesothelioma and significant increases in lung tumors. FG exposure was associated with a nonspecific inflammatory response (macrophase response) in the lungs that did not appear to progress after 6-12 months of exposure. These cellular changes are reversible and are similar to the effects observed after inhalation of an inert dust. No lung fibrosis was observed in the FG-exposed animals. Further, FG exposure resulted in no mesotheliomas and no statistically significant increase in lung tumor incidence when compared to that of the negative control group. These findings, along with previous inhalation studies, suggest that respirable fibrous glass does not represent a significant hazard for fibrotic or neoplastic lung disease in humans. |
Databáze: | OpenAIRE |
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