Toxicity of chlorpyrifos and chlorpyrifos oxon in a transgenic mouse model of the human paraoxonase (PON1) Q192R polymorphism

Cole, Toby B; Walter, Betsy J; Shih, Diana M; Tward, Aaron D; Lusis, Aldons J; Timchalk, Chuck; Richter, Rebecca J; Costa, Lucio G; Furlong, Clement E

doi:10.1097/01.fpc.0000167327.08034.d2

Title: Toxicity of chlorpyrifos and chlorpyrifos oxon in a transgenic mouse model of the human paraoxonase (PON1) Q192R polymorphism

Journal Article · Mon Aug 01 00:00:00 EDT 2005 · Pharmacogenetics and Genomics

DOI:https://doi.org/10.1097/01.fpc.0000167327.08034.d2· OSTI ID:876953

Cole, Toby B; Walter, Betsy J; Shih, Diana M; Tward, Aaron D; Lusis, Aldons J; Timchalk, Chuck; Richter, Rebecca J; Costa, Lucio G; Furlong, Clement E

The Q192R polymorphism of paraoxonase (PON1) has been shown to affect hydrolysis of organophosphorus compounds. The Q192 and R192 alloforms exhibit equivalent catalytic efficiencies of hydrolysis for diazoxon, the oxon form of the pesticide (DZ). However, the R192 alloform has a higher catalytic efficiency of hydrolysis than does the Q192 alloform for chlorpyrifos oxon (CPO), the oxon form of the pesticide chlorpyrifos (CPS). The current study examined the relevance of these observations for in-vivo exposures to chlorpyrifos and chlorpyrifos oxon. Methods Using a transgenic mouse model we examined the relevance of the Q192R polymorphism for exposure to CPS and CPO in vivo. Transgenic mice were generated that expressed either human PON1Q192 or PON1R192 at equivalent levels, in the absence of endogenous mouse PON1. Dose-response and time course experiments were performed on adult mice exposed dermally to CPS or CPO. Morbidity and acetylcholinesterase (AChE) activity in the brain and diaphragm were determined in the first 24 h following exposure. Results Mice expressing PON1Q192 were significantly more sensitive to CPO, and to a lesser extent CPS, than were mice expressing PON1R192. The time course of inhibition following exposure to 1.2 mg/kg CPO revealed maximum inhibition of brain AChE at 6?12 h, with PON1R192, PON1Q192, and PON1? /? mice exhibiting 40, 70 and 85% inhibition, respectively, relative to control mice. The effect of PON1 removal on the dose?response curve for CPS exposure was remarkably consistent with a PBPK/PD model of CPS exposure. Conclusion These results indicate that individuals expressing only the PON1Q192 allele would be more sensitive to the adverse effects of CPO or CPS exposure, especially if they are expressing a low level of plasma PON1Q192.

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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:: 876953

Report Number(s):: PNWD-SA-7056; TRN: US200608%%29

Journal Information:: Pharmacogenetics and Genomics, Vol. 58, Issue 8

Country of Publication:: United States

Language:: English

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60 APPLIED LIFE SCIENCES
ADULTS
BRAIN
DIAPHRAGM
DISEASE INCIDENCE
HYDROLYSIS
IN VIVO
PESTICIDES
TOXICITY
TRANSGENIC MICE
paraoxonase
PON1
chlorpyrifos
chlorpyrifos oxon
mice

Title: Toxicity of chlorpyrifos and chlorpyrifos oxon in a transgenic mouse model of the human paraoxonase (PON1) Q192R polymorphism

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