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双酚A对大鼠和小鼠的发育毒性。

The developmental toxicity of bisphenol A in rats and mice.

作者信息

Morrissey R E, George J D, Price C J, Tyl R W, Marr M C, Kimmel C A

出版信息

Fundam Appl Toxicol. 1987 May;8(4):571-82. doi: 10.1016/0272-0590(87)90142-4.

Abstract

Bisphenol A (BPA) was evaluated for developmental toxicity in CD rats (0, 160, 320, or 640 mg/kg/day) and CD-1 mice (0, 500, 750, 1000, or 1250 mg/kg/day) dosed daily by gastric intubation on Gestational Days 6 through 15. Timed-pregnant dams were sacrificed 1 day prior to parturition, the uterine contents were examined, and all fetuses were examined for external, visceral, and skeletal malformations. In rats, maternal weight gain during gestation, weight gain corrected for gravid uterine weight, and weight gain during treatment were significantly reduced at all BPA doses. Gravid uterine weight and average fetal body weight per litter were not affected by BPA. No increase in percentage resorptions per litter or percentage fetuses malformed per litter was detected. In mice, maternal mortality occurred at all BPA doses, reaching 18% at the high dose, which also produced a significant decrease in maternal body weight gain during gestation and treatment. Weight gain corrected for gravid uterine weight was not affected by BPA. Reductions in gravid uterine weight and average fetal body weight were observed with the 1250 mg/kg dose of BPA. Relative maternal liver weight was increased at all doses of BPA. There was a significant increase in the percentage of resorptions per litter with 1250 mg BPA/kg/day. Malformation incidence was not altered by BPA. Thus, BPA treatment at maternally toxic dose levels during organogenesis produced fetal toxicity in mice but not in rats and did not alter fetal morphologic development in either species.

摘要

对双酚A(BPA)进行了发育毒性评估,在妊娠第6至15天通过胃内插管每日给CD大鼠(剂量为0、160、320或640毫克/千克/天)和CD - 1小鼠(剂量为0、500、750、1000或1250毫克/千克/天)给药。在分娩前1天处死定时妊娠的母鼠,检查子宫内容物,并对所有胎儿进行外部、内脏和骨骼畸形检查。在大鼠中,所有双酚A剂量组母鼠在妊娠期的体重增加、校正妊娠子宫重量后的体重增加以及治疗期间的体重增加均显著降低。妊娠子宫重量和每窝胎儿平均体重不受双酚A影响。未检测到每窝吸收百分率或每窝畸形胎儿百分率增加。在小鼠中,所有双酚A剂量组均出现母鼠死亡,高剂量组死亡率达18%,该剂量组还使母鼠在妊娠期和治疗期间的体重增加显著降低。校正妊娠子宫重量后的体重增加不受双酚A影响。观察到1250毫克/千克双酚A剂量组妊娠子宫重量和胎儿平均体重降低。所有双酚A剂量组母鼠肝脏相对重量增加。1250毫克双酚A/千克/天剂量组每窝吸收百分率显著增加。双酚A未改变畸形发生率。因此,在器官形成期给予母体毒性剂量水平的双酚A处理,在小鼠中产生了胎儿毒性,但在大鼠中未产生,且在两个物种中均未改变胎儿形态发育。

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