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在杂色底鳉胚胎和孵化后幼鱼中细胞色素P-450依赖性单加氧酶系统的诱导

Induction of cytochrome P-450-dependent monooxygenase systems in embryos and eleutheroembryos of the killfish Fundulus heteroclitus.

作者信息

Binder R L, Stegeman J J, Lech J J

出版信息

Chem Biol Interact. 1985 Oct;55(1-2):185-202. doi: 10.1016/s0009-2797(85)80127-7.

Abstract

Microsomal aryl hydrocarbon hydroxylase (AHH) activity was highly inducible by polychlorinated biphenyls (PCBs) in Fundulus embryos, and stages prior to the appearance of the liver rudiment were competent to respond to these inducers. Consistent with previous observations, basal AHH activity in whole eleutheroembryo microsomes was shown to increase about 9-fold within 24 h of hatching. Aminopyrine N-demethylase (APD) activity also increased with time after hatching. However, the increase in APD activity was much less than that of AHH activity, suggesting a post-hatching change in basal cytochrome P-450 isozyme composition. Also associated with hatching was an increase in the sensitivity to PCBs as inducers of AHH activity. The ED50 for induction of AHH activity in eleutheroembryos was estimated to be only one-third to one-fourth that in embryos. This developmental increase in the sensitivity to PCBs was not due to a redistribution of PCBs between the yolk and tissues with yolk absorption, and was not simply age-dependent, but appeared to require hatching. An additional change in the monooxygenase system associated with hatching was that microsomal NADPH-cytochrome c reductase activity was not inducible by PCBs prior to hatching, but was modestly inducible after hatching. High performance liquid chromatographic (HPLC) analysis of benzo[a]-pyrene (BP) metabolites formed by microsomes from control and PCB-treated eleutheroembryos demonstrated production of dihydrodiols in the 7,8- and 9,10-positions of the benzo-ring. The formation of these metabolites was completely inhibited by the epoxide hydrolase (EH) inhibitor, trichloropropene oxide, indicating the presence of EH in Fundulus eleutheroembryos. Furthermore, these results indicate the Fundulus eleutheroembryos probably can activate BP to its ultimate carcinogenic form, the 7,8-dihydrodiol-9,10-epoxide, and induction of AHH activity by PCBs is likely to increase the rate of formation of activated metabolites from BP and related compounds. However, during the most active period of organogenesis, prior to hatching, basal AHH activity was low, and prehatching stages were relatively insensitive to cytochrome P-450 inducers. The combination of these effects may help to protect these stages from damage from activated metabolites.

摘要

在底鳉胚胎中,微粒体芳烃羟化酶(AHH)活性可被多氯联苯(PCBs)高度诱导,并且在肝脏原基出现之前的阶段就能对这些诱导剂产生反应。与之前的观察结果一致,在孵化后24小时内,全游离胚胎微粒体中的基础AHH活性增加了约9倍。氨基比林N-脱甲基酶(APD)活性也随着孵化后的时间增加。然而,APD活性的增加远小于AHH活性的增加,这表明孵化后基础细胞色素P-450同工酶组成发生了变化。与孵化相关的还有对PCBs作为AHH活性诱导剂的敏感性增加。估计在游离胚胎中诱导AHH活性的半数有效剂量(ED50)仅为胚胎中的三分之一到四分之一。这种对PCBs敏感性的发育性增加并非由于随着卵黄吸收PCBs在卵黄和组织之间的重新分布,也不是简单的年龄依赖性,而是似乎需要孵化。与孵化相关的单加氧酶系统的另一个变化是,孵化前微粒体NADPH-细胞色素c还原酶活性不能被PCBs诱导,但孵化后可被适度诱导。对来自对照和PCB处理的游离胚胎的微粒体形成的苯并[a]芘(BP)代谢物进行高效液相色谱(HPLC)分析表明,在苯环的7,8-和9,10-位产生了二氢二醇。这些代谢物的形成被环氧化物水解酶(EH)抑制剂环氧三氯丙烷完全抑制,表明底鳉游离胚胎中存在EH。此外,这些结果表明底鳉游离胚胎可能能够将BP激活为其最终致癌形式7,8-二氢二醇-9,10-环氧化物,并且PCBs对AHH活性的诱导可能会增加BP和相关化合物的活性代谢物的形成速率。然而,在器官发生最活跃的时期,即在孵化前,基础AHH活性较低,孵化前阶段对细胞色素P-450诱导剂相对不敏感。这些效应的综合作用可能有助于保护这些阶段免受活性代谢物的损害。

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