Embryo-Fetal Developmental and Reproductive Toxicology of Vinyl Chloride in Rats

doi:10.1093/toxsci/68.1.207

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Toxicological Sciences 68, 207-219 (2002)
Copyright © 2002 by the Society of Toxicology

REPRODUCTIVE AND DEVELOPMENTAL TOXICOLOGY

Embryo-Fetal Developmental and Reproductive Toxicology of Vinyl Chloride in Rats

Suzanne R. Thornton^*, Raymond E. Schroeder, Rodney L. Robison^*, Dean E. Rodwell^*, David A. Penney, Kenneth D. Nitschke and Wendy K. Sherman^¶^,1

^* Huntingdon Life Sciences, Inc., East Millstone, New Jersey 08875; MPI, Mattawan, Michigan 49071; CONDEA Vista Company, Houston, Texas 77079; The Dow Chemical Company, Midland, Michigan 48674; and ^¶ American Chemistry Council, 1300 Wilson Boulevard, Arlington, Virginia 22209

Vinyl chloride (VC) exposure is primarily via inhalation inthe workplace. The primary target organ of VC toxicity is theliver and occupational exposure to VC leads to hepatic angiosarcoma.However, based on epidemiological studies, researchers havebeen unable to ascertain the effect of occupational VC exposureon embryo-fetal development or reproductive function. A limitednumber of animal studies available in the literature have examinedthe effect of VC on embryo-fetal development, however, thereare no published studies on the effect of VC exposure on reproductivecapability. The current study was designed to assess the potentialmaternal and/or embryo-fetal developmental and 2-generationreproductive toxicity of inhaled VC in CD® Sprague-Dawleyrats at exposure levels of 0, 10, 100, and 1100 ppm. In theembryo-fetal/developmental toxicity study, the female rats wereexposed to VC daily from gestation day (GD) 6 through 19. Inthe reproductive toxicity study, the F₀ generation male andfemale rats were exposed to VC for a 10-week premating and 3-weekmating periods. The F₀ generation male rats were exposed toVC until terminal euthanasia. The F₀ generation female ratswere exposed from GD 0 through GD 20 and lactation day (LD)4 through LD 25. Our results indicate that up to 1100 ppm VCexposure did not adversely affect embryo-fetal developmentalor reproductive capability over 2 generations in rats. The primarytarget organ of VC, the liver, was affected as evidenced byan increase in liver weight and/or histologically identifiedcellular alterations, such as centrilobular hypertrophy at 100and 1000 ppm. Based on the results of these studies, the noobserved adverse effect level (NOAEL) for embryo-fetal/developmentis 1100 ppm, and the NOAEL for reproduction is 1100 ppm. Theresults from the current studies, which are a more comprehensiveembryo-fetal/developmental and reproduction study, may be incorporatedinto future risk assessments of occupational exposure to VCwhere concerns regarding the effects of VC exposure remain.

Key Words: vinyl chloride; embryo-fetal; developmental; reproduction; two-generation; rat; Sprague-Dawley.

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