EVALUATION OF A TWO-GENERATION REPRODUCTION TOXICITY STUDY ADDING ENDOPOINTS TO DETECT ENDOCRINE DISRUPTING ACTIVITY USING VINCLOZOLIN
スポンサーリンク
概要
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A two-generation reproduction toxicity study in rats adding extra endpoints to detect endocrine disrupting activity was conducted using vinclozolin by dietary administration at 0, 40, 200, and 1000 ppm, for investigation of its utility. The extra endpoints included anogenital distance (AGD), nipple development, sexual maturation (vaginal opening and preputial separation), estrous cycle, spermatogenesis, sex organ weights, and blood hormone concentrations (thyroid and sex hormones). Hepatic drugmetabolizing enzyme activities were also measured. The results revealed changes due to vinclozolin in the AGD, nipple development, sexual maturation, sex organ weights, and blood sex hormone concentrations in males of both parental animals and offspring, even at the lowest dose of 40 ppm, confirmed by results for the classical endpoints of histopathological examination at 200 ppm and mating at 1000 ppm. The effects on parental males included increased pituitary and testis weights, and decreased epididymis weights at 1000 ppm in both generations, and decreased prostate and epididymis weights at 200 and 1000 ppm and seminal vesicle weights at 1000 ppm in F1 males. Histopathological examination revealed hypertrophy of the basophilic cells in the pituitary at these two doses, and diffuse hyperplasia of the testicular interstitial cells and atrophy of the seminal vesicle mucosa at 1000 ppm in F0 and F1 males. In addition, F1 males demonstrated decrease in prostate fluid at 200 and 1000 ppm. Blood hormone analysis revealed increases in LH, FSH, testosterone, and DHT in F0 and F1 males at 1000 ppm. General toxicological effects included suppressed body weight gain in F0 and F1 females and in F1 males, and reduced food consumption in F0 and F1 females at 1000 ppm. Histopathological examination revealed centrilobular hepatocellular hypertrophy in males at 200 and 1000 ppm and in females at 1000 ppm, increased lipid droplets in the adrenal zona fasciculata and zona glomerulosa in males at 200 and 1000 ppm and in females at 40 ppm and above, and hyperplasia of ovarian interstitial cells and vacuolation of lutein cells in females at 1000 ppm in both generations. Almost all the tissue changes were accompanied by changes in weights. Decreases in T3 and/or T4 were observed in both sexes and generations at 1000 ppm and in F0 females at 200 ppm. However, these were presumed to be secondary to induction of hepatic drugmetabolizing enzymes, activities being increased for a range of enzymes in both sexes and generations at 1000 ppm. Rise in BROD activity was the most prominent, suggesting that vinclozolin mainly induces CYP2B. As for effects on reproductive function, a marked decrease in the fertility index caused by male infertility was observed in F1 animals at 1000 ppm. However, no effects on spermatogenesis were seen in either F0 or F1 males. Since cleft prepuce and penile hypoplasia were observed in infertile males, it is probable that the cause of infertility in F1 males was related to morphological abnormalities in the external genitalia. Vinclozolin did not affect the estrous cycle, mating, fertility, pregnancy, parturition, or nursing behavior in either F0 or F1 females. In offspring, in addition to suppressed body weight gain in F1 males and females at 1000 ppm, neonatal toxicity caused by antiandrogen activity of vinclozolin was observed in F1 and F2 males. Effects included shortened AGD in F1 males at 1000 ppm and in F2 males at 200 and 1000 ppm, and nipple/areola remnants in F1 males at 200 and 1000 ppm and in F2 males at 40 ppm and above. In addition, decreased epididymis weights at weaning and morphological abnormalities of the external genitalia, including cleft prepuce, penile hypoplasia, and vaginal pouch, were seen in F1 and F2 males at 1000 ppm. Post-weaning examination of F1 offspring further revealed a delay in preputial separation in males at 200 and 1000 ppm. In females, no changes suggesting endocrine disruptive effects were detected with any of the examinations. In conclusion, effects of vinclozolin were detected via the extra endpoints added to this study even at 40 ppm, close to the lowest dose reported to induce endocrine disrupting effects of vinclozolin, with marked reproductive impairment in males of the succeeding generation at 1000 ppm. These results suggest that this test protocol is useful as a two-generation reproduction study method that includes the assessment of endocrine disrupting effects. This work was conducted as part of a project of the Ministry of Environment, though this paper does not contain any opinions of the Ministry.
- 日本トキシコロジー学会の論文
- 2006-02-22
著者
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TSUCHITANI Minoru
Mitsubishi Chemical Safety Institute Ltd.
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Tsuchitani Minoru
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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Toyota Naoto
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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WAKO Yumi
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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Ikeda Yasuo
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Wako Yumi
三菱化学安全科学研究所鹿島研究所
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Wako Yumi
Mitsubishi Chemical Safety Institute Ltd.
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MATSUURA Ikuo
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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SAITOH Tetsuji
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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ASHINA Michiko
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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IWATA Hiroshi
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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ISHIZUKA Yoshihito
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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NAMIKI Masato
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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HOSHINO Nobuhito
Kashima Laboratory, Mitsubishi Chemical Safety Institute Ltd.
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Namiki Masato
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Matsuura Ikuo
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Ashina Michiko
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Saitoh Tetsuji
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Hoshino Nobuhito
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Ishizuka Yoshihito
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Tsuchitani M
Mitsubishi Chemical Safety Institute Ltd.
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Tuchitani Minoru
Mitsubishi Chemical Safety Institute Ltd.
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Wako Yumi
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd
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Tsuchitani Minoru
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Iwata Hiroshi
Kashima Laboratory Mitsubishi Chemical Safety Institute Ltd.
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Tsuchitani Minoru
Nonclinical Research Center Drug Development Service Segment Mitsubishi Chemical Medience Corporatio
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Wako Yumi
Nonclinical Research Center Drug Development Service Segment Mitsubishi Chemical Medience Corporatio
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Tsuchitani Minoru
Kashima Laboratory Mitsubishi Chemical Safery Institute Ltd.
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Tsuchitani Minoru
Nonclinical Research Center Drug Development Service Segment Mitsubishi Chemical Medience Corporation
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