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对2,3,7,8-四氯二苯并对二恶英短期高剂量毒性作用具有抗性和半抗性的大鼠产后抗药性的发展

Postnatal development of resistance to short-term high-dose toxic effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin in TCDD-resistant and -semiresistant rats.

作者信息

Simanainen Ulla, Tuomisto Jouni T, Pohjanvirta Raimo, Syrjälä Paula, Tuomisto Jouko, Viluksela Matti

机构信息

Laboratory of Toxicology, Department of Environmental Health, National Public Health Institute, FIN-70701 Kuopio, Finland.

出版信息

Toxicol Appl Pharmacol. 2004 Apr 1;196(1):11-9. doi: 10.1016/j.taap.2003.11.025.

Abstract

Despite great interspecies differences in adult 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) sensitivity, the toxic potency of TCDD is similar across species in fetal mortality. Han/Wistar (Kuopio; H/W) rats are exceptionally resistant to acute toxicity of TCDD, but show sensitivity to embryotoxicity and teratogenicity. The resistance of adult H/W rats to acute TCDD toxicity is based on a point mutation in the transactivation domain of the aryl hydrocarbon receptor (AHR) and to an unknown gene "B". This study investigated the time course of postnatal development of resistance to TCDD and the significance of genotypic variation in resistance development. H/W, line A (a new line with the H/W-type mutated AHR), and line B rats (a line with normal AHR but moderately resistant because of gene "B") were exposed to a single dose of TCDD 2-56 days after birth. H/W and line A rats received 1000 microg/kg; male and female B rats received 200 and 100 microg/kg, respectively. Survival was monitored for 42 days. Interestingly, although TCDD ceased growth and weight gain in all TCDD groups, the younger dosed animals did not seem to reach the body weight of the older dosed animals even in 100 days. The survival results after 42 days showed that line A rats are fairly resistant to TCDD immediately after birth, and their full TCDD resistance develops during the first week of life. The moderate resistance of line B rats develops approximately at the time of weaning. This difference in the time course of resistance development suggests that there are basic differences in pathways mediating resistance in lines A and B rats.

摘要

尽管成年动物对2,3,7,8-四氯二苯并对二恶英(TCDD)的敏感性存在很大的种间差异,但TCDD在胎儿死亡率方面的毒性效力在不同物种间相似。Han/Wistar(库奥皮奥;H/W)大鼠对TCDD的急性毒性具有极强的抗性,但对胚胎毒性和致畸性敏感。成年H/W大鼠对TCDD急性毒性的抗性基于芳烃受体(AHR)反式激活结构域中的一个点突变以及一个未知基因“B”。本研究调查了出生后对TCDD抗性的发育时间进程以及抗性发育中基因型变异的意义。H/W、A系(具有H/W型突变AHR的新品系)和B系大鼠(AHR正常但因基因“B”而具有中等抗性的品系)在出生后2 - 56天接受单次剂量的TCDD。H/W和A系大鼠接受1000微克/千克;雄性和雌性B系大鼠分别接受200和100微克/千克。监测存活42天。有趣的是,尽管TCDD使所有TCDD处理组的生长和体重增加停止,但即使在100天内,较年幼的给药动物似乎也未达到较年长给药动物的体重。42天后的存活结果表明,A系大鼠出生后立即对TCDD具有相当的抗性,其对TCDD的完全抗性在出生后的第一周内形成。B系大鼠的中等抗性大约在断奶时形成。抗性发育时间进程的这种差异表明,A系和B系大鼠介导抗性的途径存在基本差异。

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