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CF-1小鼠在产前暴露于双酚A后生殖器官的正常发育。

Normal reproductive organ development in CF-1 mice following prenatal exposure to bisphenol A.

作者信息

Cagen S Z, Waechter J M, Dimond S S, Breslin W J, Butala J H, Jekat F W, Joiner R L, Shiotsuka R N, Veenstra G E, Harris L R

机构信息

Shell Chemical Co., Houston, Texas, USA.

出版信息

Toxicol Sci. 1999 Jul;50(1):36-44. doi: 10.1093/toxsci/50.1.36.

Abstract

Bisphenol A (BPA) is a monomer used in the manufacture of a multitude of chemical products, including epoxy resins and polycarbonate. The objective of this study was to evaluate the effects of BPA on male sexual development. This study, performed in CF-1 mice, was limited to the measurement of sex-organ weights, daily sperm production (DSP), epididymal sperm count, and testis histopathology in the offspring of female mice exposed to low doses of BPA (0, 0.2, 2, 20, or 200 microg/kg/day), by deposition in the mouth on gestation days 11-17. Male sexual development determinations were made in offspring at 90 days-of-age. Since this study was conducted to investigate and clarify low-dose effects reported by S. C. Nagel et al., 1997, Environ. Health Perspect. 105, 70-76, and F. S. vom Saal et al., 1998, Toxicol. Indust. Health 14, 239-260, our study protocol purposely duplicated the referenced studies for all factors indicated as critical by those investigators. An additional group was dosed orally with 0.2 microg/kg/day of diethylstilbestrol (DES), which was selected based on the maternal dose reported to have maximum effect on the prostate of developing offspring, by F. S. vom Saal (1996, personal communication), vom Saal et al. (1997, Proc. Natl. Acad. Sci. U S A 94, 2056-2061). Tocopherol-stripped corn oil was used as the vehicle for BPA and DES, and was administered alone to control animals. No treatment-related effects on clinical observations, body weight, or food consumption were observed in adult females administered any dose of BPA or DES. Similarly, no treatment-related effects on growth or survival of offspring from dams treated with BPA or DES were observed. The total number of pups born per litter was slightly lower in the 200-microg/kg/day BPA group when compared to controls, but this change was not considered treatment-related since the litter size was within the normal range of historical controls. There were no treatment-related effects of BPA or DES on testes histopathology, daily sperm production, or sperm count, or on prostate, preputial gland, seminal vesicle, or epididymis weights at doses previously reported to affect these organs or at doses an order of magnitude higher or lower. In conclusion, under the conditions of this study, the effects of low doses of BPA reported by S. C. Nagel et al., 1997 (see above) and F. S. vom Saal et al., 1998 (see above), or of DES reported by F. S. vom Saal et al., 1997 (see above) were not observed. The absence of adverse findings in the offspring of dams treated orally with DES challenges the "low-dose hypothesis" of a special susceptibility of mammals exposed perinatally to ultra-low doses of even potent estrogenic chemicals. Based on the data in the present study and the considerable body of literature on effects of BPA at similar and much higher doses, BPA should not be considered as a selective reproductive or developmental toxicant.

摘要

双酚A(BPA)是一种用于制造多种化学产品的单体,包括环氧树脂和聚碳酸酯。本研究的目的是评估双酚A对雄性性发育的影响。这项在CF-1小鼠身上进行的研究,仅限于测量在妊娠第11至17天经口给予低剂量双酚A(0、0.2、2、20或200微克/千克/天)的雌性小鼠后代的性器官重量、每日精子生成量(DSP)、附睾精子计数和睾丸组织病理学。在90日龄的后代中进行雄性性发育测定。由于本研究旨在调查和阐明S.C. Nagel等人(1997年,《环境健康展望》105卷,70 - 76页)以及F.S. vom Saal等人(1998年,《毒理学与工业卫生》14卷,239 - 260页)所报告的低剂量效应,我们的研究方案特意重复了那些研究者指出的所有关键因素的参考研究。另外一组经口给予0.2微克/千克/天的己烯雌酚(DES),这是根据F.S. vom Saal(1996年,个人交流)、vom Saal等人(1997年,《美国国家科学院院刊》94卷,2056 - 2061页)报告的对发育中后代前列腺有最大影响的母体剂量选择的。生育酚去除的玉米油用作双酚A和己烯雌酚的载体,并单独给予对照动物。给予任何剂量双酚A或己烯雌酚的成年雌性动物在临床观察、体重或食物消耗方面未观察到与处理相关的影响。同样,在用双酚A或己烯雌酚处理的母鼠后代的生长或存活方面未观察到与处理相关的影响。与对照组相比,200微克/千克/天双酚A组每窝出生的幼崽总数略低,但由于窝仔数在历史对照的正常范围内,这种变化不被认为与处理相关。在先前报告的影响这些器官的剂量或高一个数量级或低一个数量级的剂量下,双酚A或己烯雌酚对睾丸组织病理学、每日精子生成量、精子计数或前列腺、包皮腺、精囊或附睾重量均无与处理相关的影响。总之,在本研究条件下,未观察到S.C. Nagel等人(1997年,见上文)和F.S. vom Saal等人(1998年,见上文)所报告的低剂量双酚A的影响,或F.S. vom Saal等人(1997年,见上文)所报告的确己烯雌酚的影响。经口给予己烯雌酚的母鼠后代未出现不良发现,这对哺乳动物在围产期暴露于超低剂量甚至强效雌激素化学物质时具有特殊易感性的“低剂量假说”提出了挑战。基于本研究的数据以及关于双酚A在相似和更高剂量下影响的大量文献,双酚A不应被视为选择性生殖或发育毒物。

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