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在发育过程中接触2,3,7,8-四氯二苯并对二恶英会永久性改变雄性长 Evans 大鼠和仓鼠的生殖功能:雄激素状态正常的后代射精和附睾精子数量减少,性附属腺重量减轻。

Exposure to TCDD during development permanently alters reproductive function in male Long Evans rats and hamsters: reduced ejaculated and epididymal sperm numbers and sex accessory gland weights in offspring with normal androgenic status.

作者信息

Gray L E, Kelce W R, Monosson E, Ostby J S, Birnbaum L S

机构信息

Developmental Reproductive Biology Section, DTD, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina 27711.

出版信息

Toxicol Appl Pharmacol. 1995 Mar;131(1):108-18. doi: 10.1006/taap.1995.1052.

Abstract

Prenatal administration of relatively low doses of TCDD alters reproductive development and fertility of the progeny. Fertility was reduced in the progeny of Wistar rats exposed to 0.5 micrograms TCDD/kg/day from Gestational Day (GD) 6 to GD 15. In a three-generation reproduction study, TCDD reduced fertility of Sprague-Dawley rats in the F1 and F2 but not the F0 (no developmental exposure) generation at 0.01 microgram/kg/day in the diet. Furthermore, administration of TCDD on GD 15 (at 0.064 to 1 microgram/kg) both demasculinized and feminized morphology and behavior of Holtzman male rat offspring. Our objectives were to expand the observations of Mably et al. (1992, Toxicol, Appl. Pharmacol. 114, 97-107, 108-117, 118-126) on the effects of gestational administration of a single dose of TCDD to another strain of rat and another species, the hamster. In the first study, Long Evans (LE) hooded rats were dosed by gavage with 1 microgram TCDD/kg on GD 8 (during the period of major organogenesis) or GD 15 (the gestational day used by Mably et al.). In the second study, pregnant Syrian hamsters, a species relatively insensitive to the lethal effects of TCDD, were dosed on GD 11, equivalent to GD 15 in the rat, with TCDD at 2 micrograms/kg. When LE rats were dosed on GD 15, or when hamsters were dosed on GD 11, puberty (preputial separation) was delayed by about 3 days, ejaculated sperm counts were reduced by at least 58%, and epididymal sperm storage was reduced by 38%. Testicular sperm production was less affected. The sex accessory glands were also reduced in size in LE rat offspring treated on GD 15 despite the fact that serum testosterone (T), T production by the testis in vitro, and androgen receptor (AR) levels were not reduced. Some reproductive measures, such as anogenital distance and male sex behavior, were altered by TCDD treatment in rat but not hamster offspring. Since T and AR levels appeared normal in the sex accessory glands and the epididymis following perinatal TCDD exposure, the alterations in these tissues are not likely to have resulted from an alteration of the androgenic status of the male offspring.

摘要

孕期给予相对低剂量的2,3,7,8-四氯二苯并对二噁英(TCDD)会改变后代的生殖发育和生育能力。从妊娠第6天(GD)至第15天,暴露于0.5微克TCDD/千克/天的Wistar大鼠后代的生育能力降低。在一项三代繁殖研究中,饮食中含有0.01微克/千克/天TCDD时,TCDD降低了F1和F2代Sprague-Dawley大鼠的生育能力,但未降低F0代(无发育暴露)的生育能力。此外,在妊娠第15天给予TCDD(剂量为0.064至1微克/千克)会使Holtzman雄性大鼠后代的形态和行为出现去雄化和雌性化。我们的目标是扩展Mably等人(1992年,《毒理学与应用药理学》114卷,97 - 107页、108 - 117页、118 - 126页)关于孕期给予单剂量TCDD对另一品系大鼠及另一物种仓鼠影响的观察结果。在第一项研究中,Long Evans(LE)带帽大鼠在妊娠第8天(主要器官形成期)或第15天(Mably等人使用的妊娠日)经口灌胃给予1微克TCDD/千克。在第二项研究中,对叙利亚仓鼠(一种对TCDD致死效应相对不敏感的物种)在相当于大鼠妊娠第15天的妊娠第11天给予2微克/千克的TCDD。当LE大鼠在妊娠第15天给药,或仓鼠在妊娠第11天给药时,青春期(包皮分离)延迟约3天,射精精子计数至少减少58%,附睾精子储存量减少38%。睾丸精子生成受影响较小。尽管血清睾酮(T)、睾丸体外T生成以及雄激素受体(AR)水平未降低,但在妊娠第15天接受治疗的LE大鼠后代中,性附属腺的大小也减小了。一些生殖指标,如肛殖距和雄性性行为,在大鼠后代中因TCDD处理而改变,但在仓鼠后代中未改变。由于围产期TCDD暴露后性附属腺和附睾中的T和AR水平似乎正常,这些组织中的改变不太可能是由雄性后代雄激素状态的改变导致的。

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