The Effect of Route, Vehicle, and Divided Doses on the Pharmacokinetics of Chlorpyrifos and its Metabolite Trichloropyridinol in Neonatal Sprague-Dawley Rats

Marty, M S; Domoradzki, J Y; Hansen, S C; Timchalk, Chuck; Bartels, M J; Mattsson, Joel L

doi:10.1093/toxsci/kfm239

Title: The Effect of Route, Vehicle, and Divided Doses on the Pharmacokinetics of Chlorpyrifos and its Metabolite Trichloropyridinol in Neonatal Sprague-Dawley Rats

Journal Article · Sat Dec 01 00:00:00 EST 2007 · Toxicological Sciences, 100(2):360-373

DOI:https://doi.org/10.1093/toxsci/kfm239· OSTI ID:921564

Marty, M S; Domoradzki, J Y; Hansen, S C; Timchalk, Chuck; Bartels, M J; Mattsson, Joel L

There is a paucity of data on neonatal systemic exposure using different dosing paradigms. Male CD (Sprague-Dawley derived) rats at postnatal day (PND) 5 were dosed with chlorpyrifos (CPF, 1 mg/kg) using different routes of exposure, vehicles, and single vs. divided doses. Blood concentrations of CPF and its primary metabolite, trichloropyridinol (TCP), were measured at multiple times through 24 h. Groups included: single gavage bolus vs. divided gavage doses in corn oil (1 vs 3 times in 24 h), single gavage bolus vs. divided gavage doses in rat milk, and subcutaneous administration in DMSO. These data were compared with lactational exposure of PND 5 pups from dams exposed to CPF in the diet at 5 mg/kg/day for four weeks or published data from dams exposed to daily gavage with CPF at 5 mg/kg/day. Maternal blood CPF levels were an order of magnitude lower from dietary exposure than gavage (1.1 vs 14.8 ng/g), and blood CPF levels in PND 5 pups that nursed dietary-exposed or gavage-exposed dams were below the limit of detection. Single gavage doses of 1 mg/kg CPF in corn oil vehicle in pups resulted in CPF blood levels of 49 ng/g, and in milk vehicle about 9 ng/g. Divided doses led to lower peak CPF levels. A bolus dose of 1 mg/kg CPF in DMSO administered sc appeared to have substantially altered pharmacokinetics from orally administered chlorpyrifos. To be meaningful for risk assessment, neonatal studies require attention to the exposure scenario, since route, vehicle, dose and frequency of administration result in different systemic exposure to the test chemical and its metabolites.

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Research Organization:: Pacific Northwest National Lab. (PNNL), Richland, WA (United States)

Sponsoring Organization:: USDOE

DOE Contract Number:: AC05-76RL01830

OSTI ID:: 921564

Report Number(s):: PNWD-SA-7894; TOSCF2; TRN: US200804%%670

Journal Information:: Toxicological Sciences, 100(2):360-373, Vol. 100, Issue 2; ISSN 1096-6080

Country of Publication:: United States

Language:: English

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13 HYDRO ENERGY
BLOOD
CORN OIL
DAMS
DETECTION
DIET
MALES
METABOLITES
MILK
RISK ASSESSMENT
Neonatal rat
chlorpyrifos
trichloropyridinol
gavage
diet
SC DMSO
dose rate
vehicle

Title: The Effect of Route, Vehicle, and Divided Doses on the Pharmacokinetics of Chlorpyrifos and its Metabolite Trichloropyridinol in Neonatal Sprague-Dawley Rats

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