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多菌灵对大鼠和仓鼠生殖发育及功能的影响。

Carbendazim-induced alterations of reproductive development and function in the rat and hamster.

作者信息

Gray L E, Ostby J, Linder R, Goldman J, Rehnberg G, Cooper R

机构信息

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

出版信息

Fundam Appl Toxicol. 1990 Aug;15(2):281-97. doi: 10.1016/0272-0590(90)90055-o.

Abstract

We are developing a data base that will allow us to select endpoints that would be useful in the detection of reproductive toxicity in a multigenerational test. In this effort, carbendazim (MBC), a known reproductive toxicant, was administered to male and female rats from weaning, through puberty, gestation, and lactation. A similar study was conducted with hamsters. In rats, MBC was administered at 0, 50, 100, 200, or 400 mg/kg/day. Hamsters were dosed at 0 or 400 mg/kg/day. In the parent (P0) generation, landmarks of puberty were measured. In females, estrous cyclicity, litter size, the number of implants, organ weights, and histology were assessed. Our assessment of the male rat included organ weights, testicular and epididymal sperm counts, a quantitative measure of sperm motility, sperm morphology, testicular histology, and endocrine measures. The growth, viability, and reproductive function of the offspring (F1) were observed during a 4-month period of continuous breeding. In the P0 of both species. MBC did not alter pubertal development, growth, or viability. The reproductive potential of the rats treated with MBC at 200 and 400 mg/kg/day was reduced due to effects on sperm production and fetal viability. In the male rat, MBC treatment markedly altered sperm morphology, testicular and epididymal weights, and sperm numbers and testicular histology. Fertility, sperm motility, and hormonal levels were altered, primarily in the males with very low sperm counts. The ability to conceive did not appear to involve a female factor. In P0 female rats, MBC administration caused postimplantation losses in the high-dosage groups and a few malformed rat pups were found in the litters from the 100 and 200 treatment groups. MBC was less toxic to the hamster than the rat. The only reproductive effects induced by MBC treatment were on sperm measures. Fertility of the P0 generation and fetal and neonatal (F1) viability were not decreased by MBC administration. In the male rat, testis weight, sperm numbers in the cauda epididymis and testis and sperm morphology were sensitive to the effects of MBC. In females, counting implantation scars at necropsy was useful, as this information allowed us to confirm pregnancy and identify postimplantation losses induced by MBC administration.

摘要

我们正在开发一个数据库,该数据库将使我们能够选择在多代试验中对检测生殖毒性有用的终点指标。在这项工作中,多菌灵(MBC)是一种已知的生殖毒物,从断奶期开始,经青春期、妊娠期和哺乳期对雄性和雌性大鼠给药。对仓鼠进行了类似的研究。在大鼠中,多菌灵的给药剂量为0、50、100、200或400毫克/千克/天。仓鼠的给药剂量为0或400毫克/千克/天。在亲代(P0)代中,测量了青春期的标志性指标。在雌性中,评估了发情周期、产仔数、着床数、器官重量和组织学。我们对雄性大鼠的评估包括器官重量、睾丸和附睾精子计数、精子活力的定量测量、精子形态、睾丸组织学和内分泌指标。在连续繁殖的4个月期间观察了后代(F1)的生长、活力和生殖功能。在两个物种的P0代中,多菌灵均未改变青春期发育、生长或活力。由于对精子生成和胎儿活力的影响,以200和400毫克/千克/天剂量处理的大鼠的生殖潜力降低。在雄性大鼠中,多菌灵处理显著改变了精子形态、睾丸和附睾重量、精子数量和睾丸组织学。生育力、精子活力和激素水平发生了改变,主要是在精子计数极低的雄性大鼠中。受孕能力似乎不涉及雌性因素。在P0代雌性大鼠中,高剂量组给药后出现着床后损失,在100和200处理组的窝仔中发现了一些畸形幼鼠。多菌灵对仓鼠的毒性比对大鼠的毒性小。多菌灵处理诱导的唯一生殖效应是对精子指标的影响。多菌灵给药并未降低P0代的生育力以及胎儿和新生儿(F1)的活力。在雄性大鼠中,睾丸重量、附睾尾和睾丸中的精子数量以及精子形态对多菌灵的影响敏感。在雌性中,尸检时计数着床瘢痕很有用,因为这些信息使我们能够确认妊娠并识别多菌灵给药引起的着床后损失。

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