Developmental Toxicity Studies in Rats and Rabbits with 3,5,6-Trichloro-2-pyridinol, the Major Metabolite of Chlorpyrifos

doi:10.1093/toxsci/53.1.100

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Toxicological Sciences 53, 100-108 (2000)
Copyright © 2000 by the Society of Toxicology

Developmental Toxicity Studies in Rats and Rabbits with 3,5,6-Trichloro-2-pyridinol, the Major Metabolite of Chlorpyrifos

Thomas R. Hanley, Jr.^*^,1, Edward W. Carney and E. Marshall Johnson

^* Global Health, Environmental Safety and Regulatory, Dow AgroSciences, L. L. C., 9330 Zionsville Road, Indianapolis, Indiana 46268; Health and Environmental Research Laboratories, The Dow Chemical Company, Midland, Michigan 48674; Jefferson Medical College, Philadelphia, Pennsylvania 19107

3,5,6-Trichloro-2-pyridinol (TCP), the primary metabolite ofchlorpyrifos and chlorpyrifos-methyl, was evaluated for potentialdevelopmental toxicity. Groups of 32–34 bred female Fischer344 rats were given 0, 50, 100, or 150 mg TCP/kg/day by gavageon gestation days 6–15; the fetuses were evaluated ongestation day 21. Similarly, groups of 16 inseminated femaleNew Zealand White rabbits were given 0, 25, 100, or 250 mg TCP/kg/dayby gavage on gestation days 7–19, and fetuses were evaluatedon gestation day 28. No clinical signs of toxicity attributedto TCP were noted in either species. In rats, at 150 mg/kg/day,maternal effects included slight decreases in feed consumption,significantly depressed body weight gain (25% relative to controls)resulting in significantly lower maternal terminal body weights,and increased relative liver weight. At 100 mg/kg/day, maternalbody weight gain in rats was depressed approximately 22%. Amongrabbits, maternal effects were limited to the group given 250mg/kg/day, which lost an average of approximately 70 g duringthe treatment period (vs. 140 g in the controls). There wereno effects on fetal weight or viability, nor were there significantincreases in any fetal alteration in either species. A slightlyhigher (not statistically significant) than usual incidenceof central nervous system anomalies occurred in rabbits, butthese anomalies were found in both treated and control groupsin this study as well as contemporaneous studies of unrelatedcompounds. This, and the fact that these anomalies were notseen with the parent compound, chlorpyrifos, suggest that theirorigin was spontaneous. Thus, TCP was not considered fetotoxicor teratogenic in either rats or rabbits, even at dose levelsthat produced maternal toxicity.

Key Words: TCP; organophosphates; chlorpyrifos; rats; rabbits; developmental toxicity.

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