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产前己烯雌酚会导致雄性和雌性小鼠的外生殖器畸形,并在两种小鼠品系中引发第二代外生殖器持续发育异常。

Prenatal diethylstilbestrol induces malformation of the external genitalia of male and female mice and persistent second-generation developmental abnormalities of the external genitalia in two mouse strains.

作者信息

Mahawong Phitsanu, Sinclair Adriane, Li Yi, Schlomer Bruce, Rodriguez Esequiel, Ferretti Max M, Liu Baomei, Baskin Laurence S, Cunha Gerald R

机构信息

Division of Pediatric Urology, University of California, San Francisco, CA 94143, United States.

Division of Pediatric Urology, University of California, San Francisco, CA 94143, United States.

出版信息

Differentiation. 2014 Sep-Oct;88(2-3):51-69. doi: 10.1016/j.diff.2014.09.005. Epub 2014 Oct 14.

Abstract

Potential trans-generational influence of diethylstilbestrol (DES) exposure emerged with reports of effects in grandchildren of DES-treated pregnant women and of reproductive tract tumors in offspring of mice exposed in utero to DES. Accordingly, we examined the trans-generational influence of DES on development of external genitalia (ExG) and compared effects of in utero DES exposure in CD-1 and C57BL/6 mice injected with oil or DES every other day from gestational days 12 to 18. Mice were examined at birth, and on 5-120 days postnatal to evaluate ExG malformations. Of 23 adult (>60 days) prenatally DES-exposed males, features indicative of urethral meatal hypospadias (see text for definitions) ranged from 18% to 100% in prenatally DES-exposed CD-1 males and 31% to 100% in prenatally DES-exposed C57BL/6 males. Thus, the strains differed only slightly in the incidence of male urethral hypospadias. Ninety-one percent of DES-exposed CD-1 females and 100% of DES-exposed C57BL/6 females had urethral-vaginal fistula. All DES-exposed CD-1 and C57BL/6 females lacked an os clitoris. None of the prenatally oil-treated CD-1 and C57BL/6 male and female mice had ExG malformations. For the second-generation study, 10 adult CD-1 males and females, from oil- and DES-exposed groups, respectively, were paired with untreated CD-1 mice for 30 days, and their offspring evaluated for ExG malformations. None of the F1 DES-treated females were fertile. Nine of 10 prenatally DES-exposed CD-1 males sired offspring with untreated females, producing 55 male and 42 female pups. Of the F2 DES-lineage adult males, 20% had exposed urethral flaps, a criterion of urethral meatal hypospadias. Five of 42 (11.9%) F2 DES lineage females had urethral-vaginal fistula. In contrast, all F2 oil-lineage males and all oil-lineage females were normal. Thus, prenatal DES exposure induces malformations of ExG in both sexes and strains of mice, and certain malformations are transmitted to the second-generation.

摘要

己烯雌酚(DES)暴露的潜在跨代影响随着以下报告而显现:DES治疗的孕妇的孙辈出现了影响,以及子宫内暴露于DES的小鼠后代出现了生殖道肿瘤。因此,我们研究了DES对外部生殖器(ExG)发育的跨代影响,并比较了在妊娠第12天至18天每隔一天注射油或DES的CD - 1和C57BL / 6小鼠子宫内DES暴露的影响。在出生时以及出生后5至120天对小鼠进行检查,以评估ExG畸形。在23只成年(>60天)产前暴露于DES的雄性小鼠中,产前暴露于DES的CD - 1雄性小鼠中指示尿道下裂(定义见正文)的特征发生率在18%至100%之间,产前暴露于DES的C57BL / 6雄性小鼠中为31%至100%。因此,这两个品系在男性尿道下裂的发生率上仅略有差异。91%的暴露于DES的CD - 1雌性小鼠和100%的暴露于DES的C57BL / 6雌性小鼠有尿道阴道瘘。所有暴露于DES的CD - 1和C57BL / 6雌性小鼠都没有阴蒂骨。产前接受油处理的CD - 1和C57BL / 6雄性和雌性小鼠均没有ExG畸形。在第二代研究中,分别来自油处理组和DES暴露组的10只成年CD - 1雄性和雌性小鼠与未处理的CD - 1小鼠配对30天,并对它们的后代进行ExG畸形评估。接受DES处理的F1代雌性均不育。10只产前暴露于DES的CD - 1雄性中有9只与未处理的雌性交配产生后代,产下55只雄性和42只雌性幼崽。在F2代DES谱系成年雄性中,20%有外露的尿道瓣,这是尿道下裂的一个标准。42只(11.9%)F2代DES谱系雌性中有5只患有尿道阴道瘘。相比之下,所有F2代油谱系雄性和所有油谱系雌性均正常。因此,产前DES暴露会在小鼠的两性和品系中诱导ExG畸形,并且某些畸形会传递给第二代。

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