Spinosad Insecticide: Subchronic and Chronic Toxicity and Lack of Carcinogenicity in CD-1 Mice

doi:10.1093/toxsci/65.2.276

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Toxicological Sciences 65, 276-287 (2002)
Copyright © 2002 by the Society of Toxicology

SAFETY EVALUATION

Spinosad Insecticide: Subchronic and Chronic Toxicity and Lack of Carcinogenicity in CD-1 Mice

K. E. Stebbins^*^,1, D. M. Bond^*, M. N. Novilla and M. J. Reasor

^* Toxicology and Environmental Research and Consulting, The Dow Chemical Company, 1803 Building, Midland, Michigan 48674; Lilly Research Laboratories, Eli Lilly and Company, Greenfield, Indiana 46268; and Department of Pharmacology and Toxicology, West Virginia University, Morgantown, West Virginia, 26506

The potential toxicologic and oncogenic effects of spinosad,a natural fermentation product with insecticidal properties,were investigated. The 13-week toxicity study consisted of groupsof 10 CD-1 mice/sex provided diets containing 0, 0.005, 0.015,0.045, or 0.12% spinosad (Study 1). The 0.12% group was terminatedon Test Day 44 due to mortality and overt clinical signs oftoxicity. An 18-month chronic oncogenicity study consisted ofgroups of 50 CD-1 mice/sex provided diets containing 0, 0.0025,0.008, or 0.036% spinosad (Study 2). Two interim groups of 10mice/sex/group were terminated after 3 and 12 months. Femalesgiven 0.036% were terminated on Day 455 due to markedly lowerbody weights and feed consumption, as well as excessive mortality.Because of the early termination of the female high-dose group,additional groups of 10 male and female mice (12-month interimnecrospy) and 50 male and female mice (18-month necropsy) wereprovided diets containing 0, 0.0008, or 0.024% spinosad (Study3) to fully assess potential chronic toxicity and oncogenicity.Standard toxicologic parameters were evaluated consistent withexisting regulatory guidelines. The primary effect in the 13-weekand 18-month studies was intracellular vacuolation of histiocyticand epithelial cells in numerous tissues and organs at dosesof $>=$ 0.015%. The histological vacuolation corresponded to ultrastructurallysosomal lamellar inclusion bodies. This alteration was consistentwith phospholipidosis, a condition that results from accumulationof polar lipids in lysosomes. Lesions with no apparent directrelation to vacuolation were hyperplasia of the glandular mucosaof the stomach, skeletal muscle myopathy, bone marrow necrosis,and anemia with associated splenic hematopoiesis. The incidenceof tumors in mice given spinosad was not increased relativeto controls at any dose level. The no observed effect levelfor the 13-week study was 0.005% (6 mg/kg/day) spinosad, andfor the chronic toxicity/oncogenicity study was 0.008% (11 mg/kg/day)spinosad for male and female CD-1 mice.

Key Words: spinosad; subchronic toxicity; carcinogenicity; lysosomes; phospholipidosis; cationic amphiphilic compounds; mice.

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