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甲基丙烯腈对斯普拉格-道利大鼠和新西兰白兔发育毒性的评估。

Evaluation of the developmental toxicity of methacrylonitrile in Sprague-Dawley rats and New Zealand white rabbits.

作者信息

George J D, Price C J, Marr M C, Myers C B, Schwetz B A, Heindel J J, Hunter E S

机构信息

Chemistry and Life Sciences, Research Triangle Institute, Research Triangle Park, North Carolina, 27709-2194, USA.

出版信息

Fundam Appl Toxicol. 1996 Dec;34(2):249-59. doi: 10.1006/faat.1996.0194.

Abstract

Timed-pregnant Sprague-Dawley (CD) outbred rats and New Zealand White rabbits were dosed by gavage with methacrylonitrile (MACR) in distilled water during major organogenesis. Rats were dosed on Gestational Days (GD) 6 through 15 (0, 5, 25, or 50 mg MACR/kg/day) and rabbits on GD 6 through 19 (0, 1, 3, or 5 mg MACR/kg/day). Maternal clinical status was monitored daily during treatment. At termination (GD 20, rats; GD 30, rabbits), confirmed-pregnant females (25-26 per group, rats; 17-22 per group, rabbits) were evaluated for clinical status and gestational outcome; each live fetus was examined for external, visceral, and skeletal malformations. In rats, no treatment-related maternal clinical signs or mortality were observed, nor was there any adverse effect on maternal body weight or food or water consumption. At necropsy, absolute, relative, and adjusted maternal liver weight was increased at the mid- and high-dose groups, an effect that may be indicative of induction of hepatic enzymes rather than toxicity. In the absence of any indication of maternal toxicity, the no-observed-adverse-effect level (NOAEL) for maternal toxicity in this study was >/=50 mg MACR/kg/day. The NOAEL for developmental toxicity in rats was also >/=50 mg MACR/kg/day. There was no effect of treatment on postimplantation loss, mean fetal body weight per litter, or morphological development. In rabbits, maternal mortality and clinical signs were not dose related. Maternal food consumption, body weight, and liver weight were not adversely affected by treatment. Thus, the maternal NOAEL was >/=5 mg MACR/kg/day. Maternal toxicity, including death, was observed >/=7.5 mg/kg/day in preliminary studies. The developmental NOAEL was also >/=5 mg MACR/kg/day. There was no adverse effect of treatment on postimplantation loss or fetal body weight. A significant decrease in the percentage male fetuses per litter was observed, although there was no effect on total live litter size, suggesting that the reduction in the ratio of live male fetuses in the high-dose group was not biologically significant. MACR had no adverse effect on morphological development. In summary, oral administration of MACR to rats and rabbits during organogenesis, at doses that did not cause persistent maternal toxicity (50 mg MACR/kg/day, rats; 5 mg MACR/kg/day, rabbits), also did not cause any adverse developmental effects.

摘要

在主要器官形成期,将妊娠特定阶段的斯普拉格-道利(CD)远交群大鼠和新西兰白兔,经口灌胃给予溶于蒸馏水中的甲基丙烯腈(MACR)。大鼠在妊娠第6至15天给药(0、5、25或50毫克MACR/千克/天),兔子在妊娠第6至19天给药(0、1、3或5毫克MACR/千克/天)。在治疗期间每天监测母体的临床状况。在实验结束时(大鼠为妊娠第20天;兔子为妊娠第30天),对确认怀孕的雌性动物(大鼠每组25 - 26只;兔子每组17 - 22只)进行临床状况和妊娠结局评估;检查每只活胎仔的外部、内脏和骨骼畸形情况。在大鼠中,未观察到与治疗相关的母体临床体征或死亡情况,对母体体重、食物或水的消耗量也没有任何不良影响。尸检时,中、高剂量组母体肝脏的绝对重量、相对重量和校正重量均增加,这种效应可能表明肝酶的诱导而非毒性作用。在没有任何母体毒性迹象的情况下,本研究中母体毒性的未观察到不良作用水平(NOAEL)≥50毫克MACR/千克/天。大鼠发育毒性的NOAEL也≥50毫克MACR/千克/天。治疗对着床后丢失、每窝平均胎仔体重或形态发育没有影响。在兔子中,母体死亡率和临床体征与剂量无关。母体食物消耗量、体重和肝脏重量未受到治疗的不利影响。因此,母体NOAEL≥5毫克MACR/千克/天。在初步研究中,观察到≥7.5毫克/千克/天的剂量会出现母体毒性,包括死亡。发育毒性的NOAEL也≥5毫克MACR/千克/天。治疗对着床后丢失或胎仔体重没有不良影响。观察到每窝雄性胎仔百分比显著下降,尽管对每窝活胎仔总数没有影响,这表明高剂量组活雄性胎仔比例的降低在生物学上不显著。MACR对形态发育没有不良影响。总之,在器官形成期给大鼠和兔子经口给予MACR,在未引起持续性母体毒性的剂量下(大鼠为50毫克MACR/千克/天;兔子为5毫克MACR/千克/天),也未引起任何不良发育影响。

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