Two-hour methyl isocyanate inhalation exposure and 91-day recovery: a preliminary description of pathologic changes in F344 rats.

Bucher, John R.; Boorman, Gary A.; Gupta, B. N.; Uraih, Linda C.; Hall, L B; Stefanski, Steven A.

doi:10.1289/ehp.877271

Cited by 27 publications

(18 citation statements)

References 18 publications

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“…This exposure pattern was chosen to mimic in duration and result the December 3, 1984, release of methyl isocyanate from a storage tank at an agricultural chemical plant in Bhopal, India. The results of this study (1)(2)(3) demonstrated that the lung and upper respiratory tract were the primary targets of methyl isocyanate injury and suggested that damage to the respiratory tract was severe enough to account for the observed mortality. Results of the previous study also demonstrated a very steep dose response for lethality of inhaled methyl isocyanate, with concentrations of 10 ppm causing few or no deaths in rats or mice, but concentrations of 20 to 30 ppm being lethal to 60 to 80% of exposed animals.…”

Section: Introductionmentioning

confidence: 70%

The toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. II. Repeated exposure and recovery studies.

Bucher¹,

Thompson²,

Adkins³

et al. 1987

Environ Health Perspect

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F344/N rats and B6C3F1 mice were exposed to 0, 1, 3, or 6 ppm methyl isocyanate by inhalation for 6 hr on 4 consecutive days. Deaths of rats were observed following 3 ppm exposures, and mice died after exposures to 6 ppm. Deaths appeared to be related to severe respiratory distress. Survivors in high dose groups lost weight initially, then gained weight at rates equal to controls throughout a 91-day recovery period. Lung weights increased significantly in male and female rats exposed to 3 ppm, but no persistent changes in brain, kidney, thymus, spleen, liver, or testis weights were seen in either mice or rats.Blood and serum from male and female rats were taken for clinical pathology and hematology assessments on day 7 of postexposure, the day prior to the first observed deaths of these animals. No changes or only slight changes were seen in measures of serum alanine aminotransferase, sorbitol dehydrogenase, alkaline phosphatase, or in blood and brain cholinesterase activities. However, serum creatine kinase increased with dose in both males and females. Blood urea nitrogen, creatinine, and methemoglobin were unchanged. No changes were seen in counts ofred blood cells or platelets, or in red cell indicies. Hemoglobin concentrations and hematocrits were slightly elevated. No changes were noted in absolute leukocyte counts, but counts of segmented neutrophils increased and lymphocytes decreased. These changes are consistent with slight hemoconcentration and a stress-related leukogram, as seen in acute exposure studies. These studies provide toxicity information for further NIEHS studies of immunotoxicity, reproductive toxicity, and genetic toxicity using this repeated exposure regimen, which are also reported in this issue. The results indicate that the respiratory system is the primary site of injury following repeated inhalations of lethal and sublethal concentrations of methyl isocyanate, and give little evidence of direct effects on nonrespiratory tissues.

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Section: Introductionmentioning

confidence: 70%

The toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. II. Repeated exposure and recovery studies.

Bucher¹,

Thompson²,

Adkins³

et al. 1987

Environ Health Perspect

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“…Changes in absolute organ weights and in organ- to-body weight ratios for brain, liver, kidney, spleen, and testis (not shown) were statistically significant at certain time points in certain experimental groups, but the differences were not consistent between groups, and did not suggest a selective toxicity to any of these organs. With the exception of mild cytoplasmic vacuolization of the liver in mice, significant pathologic changes were not found in these organs (6,7). However, changes in lung-and thymus-to-body weight ratios were consistent and were dose-related in mice and rats.…”

Section: Body and Organ Weightsmentioning

confidence: 85%

“…Within 3 hr following the exposures (day 0), and again on days 1, 3, 7, 14, 49 and 91 after exposure, five predesignated animals per group were killed by pentobarbital overdose and given a complete gross necropsy. The lungs, brain, liver, kidney, thymus, testis, and spleen were weighed prior to fixation for histopathologic analysis [see accompanying papers (6,7)]. The right apical lobe of the lung was removed from male rats killed on days 0, 1, 3 and 7, weighed, and allowed to dry to constant weight for determination of wet-to-dry weight ratio.…”

Section: Methodsmentioning

confidence: 99%

Toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. I. Acute exposure and recovery studies.

Bucher¹,

Adkins²,

Thompson³

et al. 1987

Environ Health Perspect

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Male and female F344/N rats and B6C3F1 mice were exposed to lethal and sublethal concentrations of methyl isocyanate by inhalation. Mortality, clinical signs, body and organ weights, and changes in clinical pathology and hematology were monitored immediately after 2-hr exposures and during the ensuing 3 months. Additional studies investigated the possible involvement of cyanide in the toxicity of methyl isocyanate. During exposures, signs of restlessness, lacrimation, and a reddish discharge from the nose and mouth were evident in rats and mice. Following exposures, rats and mice were dyspneic and weak. Deaths of rats and mice exposed to lethal concentrations (20 to 30 ppm) began within 15-18 hr, with males more prone to early death than females. A second wave of deaths occurred after 8 to 10 days, affecting primarily female rats and mice exposed to 20 to 30 ppm of methyl isocyanate, and male and female rats exposed to 10 ppm. Most deaths occurred during the first month following the exposures and were preceded by periods of severe respiratory distress. Body weights decreased in proportion to dose early, but then weight gain resumed in survivors at control rates. The only organ with a consistent, dose-related weight change was the lung, which was heavier throughout the studies in animals exposed to high concentrations of methyl isocyanate. No significant clinical pathology, or hematologic changes were observed in exposed rats. Blood and brain cholinesterase were not inhibited. Studies attempting to measure cyanide in the blood of methyl isocyanate-exposed rats, and attempting to affect lethality with a cyanide antidote (sodium nitrite and sodium thiosulfate) gave negative results. The findings indicate that at these doses, methyl isocyanate inhalation causes deaths and persistent pulmonary changes, but no evidence of extrapulmonary toxicity in rodents. Cyanide does not appear to be involved in methyl isocyanate toxicity.

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“…Exposure to these concentrations resulted in a severe necrotizing effect on the olfactory and respiratory epithelium lining the respiratory tract; no effect was observed in those areas of the nose lined with stratified squamous epithelium (9). Stratified squamous epithelium also covers the anterior portion of the cornea, and the apparent lower sensitivity of this cell type to MIC-induced damage may account at least in part for our negative findings.…”

Section: Discussionmentioning

confidence: 65%

Effect of Methyl Isocyanate (MIC) Gas on the Eyes of Fischer 344 Rats

Gupta¹,

Stefanski²,

Bucher³

et al. 1987

Environmental Health Perspectives

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Two-hour methyl isocyanate inhalation exposure and 91-day recovery: a preliminary description of pathologic changes in F344 rats.

Cited by 27 publications

References 18 publications

The toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. II. Repeated exposure and recovery studies.

The toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. II. Repeated exposure and recovery studies.

Toxicity of inhaled methyl isocyanate in F344/N rats and B6C3F1 mice. I. Acute exposure and recovery studies.

Effect of Methyl Isocyanate (MIC) Gas on the Eyes of Fischer 344 Rats

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