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增效剂胡椒基丁醚和三丁基三硫代磷酸酯对德国小蠊(蜚蠊目:姬蠊科)残杀威药代动力学的影响

Effects of the synergists piperonyl butoxide and S,S,S-tributyl phosphorotrithioate on propoxur pharmacokinetics in Blattella germanica (Blattodea: Blattellidae).

作者信息

Sanchez-Arroyo H, Koehler P G, Valles S M

机构信息

Entomología y Acarología-IFIT-CP, Edo. México CP, Mexico.

出版信息

J Econ Entomol. 2001 Oct;94(5):1209-16. doi: 10.1603/0022-0493-94.5.1209.

Abstract

Effects of the synergists piperonyl butoxide (PBO) and S,S,S-tributyl phosphorotrithioate (DEF) on propoxur pharmacokinetics were examined in the German cockroach, Blattella germanica (L.). Treatment of adult male German cockroaches with the cytochrome P450 monooxygenase inhibitor, PBO, or the esterase inhibitor, DEF, increased propoxur toxicity by 2- and 6.8-fold, respectively, implicating hydrolysis as a major detoxification route of propoxur in the German cockroach. However, significant hydrolytic metabolism could not be demonstrated conclusively in vitro resulting in a conflict between in situ bioassay data and in vitro metabolic studies. In vitro propoxur metabolism with NADPH-fortified microsomes produced at least nine metabolites. Formation of metabolites was NADPH-dependent; no quantifiable metabolism was detected with cytosolic fractions. However, microsomal fractions lacking an NADPH source did produce a low, but detectable, quantity of metabolites (1.6 pmol). PBO inhibited NADPH-dependent propoxur metabolism in a dose-dependent fashion, implicating cytochrome P450 monooxygenases as the enzyme system responsible for the metabolism. Interestingly, DEF also inhibited the NADPH-dependent metabolism of propoxur, albeit to a lower extent. Treatment with PBO or DEF also caused a significant reduction in the cuticular penetration rate of propoxur. The data demonstrate that unanticipated effects are possible with synergists and that caution must be exercised when interpreting synergist results.

摘要

在德国小蠊(Blattella germanica (L.))中研究了增效剂胡椒基丁醚(PBO)和三丁基三硫代磷酸酯(DEF)对残杀威药代动力学的影响。用细胞色素P450单加氧酶抑制剂PBO或酯酶抑制剂DEF处理成年雄性德国小蠊,分别使残杀威毒性提高了2倍和6.8倍,这表明水解是德国小蠊中残杀威的主要解毒途径。然而,在体外无法确凿地证明有显著的水解代谢,这导致原位生物测定数据与体外代谢研究之间存在冲突。用NADPH强化的微粒体进行体外残杀威代谢产生了至少九种代谢产物。代谢产物的形成依赖于NADPH;用胞质部分未检测到可量化的代谢。然而,缺乏NADPH来源的微粒体部分确实产生了少量但可检测到的代谢产物(1.6皮摩尔)。PBO以剂量依赖的方式抑制依赖NADPH的残杀威代谢,这表明细胞色素P450单加氧酶是负责代谢的酶系统。有趣的是,DEF也抑制了依赖NADPH的残杀威代谢,尽管程度较低。用PBO或DEF处理也导致残杀威的表皮渗透速率显著降低。数据表明增效剂可能会产生意想不到的效果,在解释增效剂结果时必须谨慎。

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