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孕期接触全氟辛酸(PFOA)对老鼠生殖的影响。

Effects of perfluorooctanoic acid (PFOA) exposure to pregnant mice on reproduction.

机构信息

Department of Forensic Medicine and Toxicology, Faculty of Veterinary Medicine, Assiut University, Assiut, Egypt.

出版信息

J Toxicol Sci. 2010 Aug;35(4):527-33. doi: 10.2131/jts.35.527.

DOI:10.2131/jts.35.527
PMID:20686339
Abstract

Perfluorooctanoic acid (PFOA) has similar characteristics to perfluorooctane sulfonate (PFOS) in reproduction toxicity featured by neonatal death. We found that PFOS exposure to mice during pregnancy led to intracranial blood vessel dilatation of fetuses accompanied by severe lung collapse which caused neonatal mortality. Thus, we adopted the corresponding experimental design to PFOS in order to characterize the neonatal death by PFOA. Pregnant ICR mice were given 1, 5 and 10 mg/kg PFOA daily by gavage from gestational day (GD) 0 to 17 and 18 for prenatal and postnatal evaluations, respectively. Five to nine dams per group were sacrificed on GD 18 for prenatal evaluation; other 10 dams were left to give birth. No maternal death was observed. The liver weight increased dose-dependently, with hepatocellular hypertrophy, necrosis, increased mitosis and mild calcification at 10 mg/kg. PFOA at 10 mg/kg increased serum enzyme activities (GGT, ALT, AST and ALP) with hypoproteinemia and hypolipidemia. PFOA treatment reduced the fetal body weight at 5 and 10 mg/kg. Teratological evaluation showed delayed ossification of the sternum and phalanges and delayed eruption of incisors at 10 mg/kg, but did not show intracranial blood vessel dilatation. Postnatal evaluation revealed that PFOA reduced the neonatal survival rate at 5 and 10 mg/kg. At 5 mg/kg pups were born alive and active and 16% died within 4 days observation, while all died within 6 hr after birth at 10 mg/kg without showing intracranial blood vessel dilatation. The cause of neonatal death by PFOA may be different from PFOS.

摘要

全氟辛酸(PFOA)在生殖毒性方面具有类似于全氟辛烷磺酸(PFOS)的特征,表现为新生儿死亡。我们发现,PFOS 在妊娠期间暴露于小鼠体内会导致胎儿颅内血管扩张,同时伴有严重的肺塌陷,从而导致新生儿死亡。因此,我们采用了相应的实验设计来研究 PFOA 导致的新生儿死亡。将怀孕的 ICR 小鼠从妊娠第 0 天到第 17 天每天通过灌胃给予 1、5 和 10mg/kg 的 PFOA,第 18 天进行产前和产后评估。每组 5-9 只孕鼠用于产前评估;其余 10 只孕鼠则用于分娩。未观察到母体死亡。肝脏重量呈剂量依赖性增加,10mg/kg 时出现肝细胞肥大、坏死、有丝分裂增加和轻度钙化。PFOA 在 10mg/kg 时会增加血清酶活性(GGT、ALT、AST 和 ALP),同时伴有低蛋白血症和低脂质血症。PFOA 处理会降低 5mg/kg 和 10mg/kg 时的胎儿体重。致畸学评估显示,10mg/kg 时胸骨和指骨的骨化延迟,门齿迟萌,但未显示颅内血管扩张。产后评估显示,PFOA 降低了 5mg/kg 和 10mg/kg 时的新生儿存活率。5mg/kg 组的幼鼠出生时存活且活跃,16%在 4 天观察期内死亡,而 10mg/kg 组的所有幼鼠在出生后 6 小时内死亡,且未显示颅内血管扩张。PFOA 导致的新生儿死亡的原因可能与 PFOS 不同。

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