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溴氰菊酯和高效氯氰菊酯体外代谢的种属差异:人和大鼠的氧化及水解代谢差异

Species differences in the in vitro metabolism of deltamethrin and esfenvalerate: differential oxidative and hydrolytic metabolism by humans and rats.

作者信息

Godin Stephen J, Scollon Edward J, Hughes Michael F, Potter Philip M, DeVito Michael J, Ross Matthew K

机构信息

Curriculum in Toxicology, University of North Carolina at Chapel Hill, Chapel Hill, NC, USA.

出版信息

Drug Metab Dispos. 2006 Oct;34(10):1764-71. doi: 10.1124/dmd.106.010058. Epub 2006 Jul 19.

Abstract

Pyrethroids are neurotoxic pesticides whose pharmacokinetic behavior plays a role in their potency. This study examined the elimination of esfenvalerate and deltamethrin from rat and human liver microsomes. A parent depletion approach in the presence and absence of NADPH was used to assess species differences in biotransformation pathways, rates of elimination, and intrinsic hepatic clearance. Esfenvalerate was eliminated primarily via NADPH-dependent oxidative metabolism in both rat and human liver microsomes. The intrinsic hepatic clearance (CL(INT)) of esfenvalerate was estimated to be 3-fold greater in rodents than in humans on a per kilogram body weight basis. Deltamethrin was also eliminated primarily via NADPH-dependent oxidative metabolism in rat liver microsomes; however, in human liver microsomes, deltamethrin was eliminated almost entirely via NADPH-independent hydrolytic metabolism. The CL(INT) for deltamethrin was estimated to be 2-fold more rapid in humans than in rats on a per kilogram body weight basis. Metabolism by purified rat and human carboxylesterases (CEs) were used to further examine the species differences in hydrolysis of deltamethrin and esfenvalerate. Results of CE metabolism revealed that human carboxylesterase 1 (hCE-1) was markedly more active toward deltamethrin than the class 1 rat CEs hydrolase A and B and the class 2 human CE (hCE-2); however, hydrolase A metabolized esfenvalerate 2-fold faster than hCE-1, whereas hydrolase B and hCE-1 hydrolyzed esfenvalerate at equal rates. These studies demonstrate a significant species difference in the in vitro pathways of biotransformation of deltamethrin in rat and human liver microsomes, which is due in part to differences in the intrinsic activities of rat and human carboxylestersases.

摘要

拟除虫菊酯是具有神经毒性的杀虫剂,其药代动力学行为决定了它们的效力。本研究检测了大鼠和人肝脏微粒体中乙氰菊酯和溴氰菊酯的消除情况。采用在有和没有烟酰胺腺嘌呤二核苷酸磷酸(NADPH)存在的情况下母体药物消耗法,来评估生物转化途径、消除速率和肝脏固有清除率的种属差异。在大鼠和人肝脏微粒体中,乙氰菊酯主要通过依赖NADPH的氧化代谢而被消除。以每千克体重计算,乙氰菊酯的肝脏固有清除率(CL(INT))在啮齿动物中比在人类中高3倍。在大鼠肝脏微粒体中,溴氰菊酯也主要通过依赖NADPH的氧化代谢而被消除;然而,在人肝脏微粒体中,溴氰菊酯几乎完全通过不依赖NADPH的水解代谢而被消除。以每千克体重计算,溴氰菊酯的CL(INT)在人类中比在大鼠中快2倍。用纯化的大鼠和人羧酸酯酶(CEs)进行代谢研究,以进一步检测溴氰菊酯和乙氰菊酯水解的种属差异。CE代谢结果显示,人羧酸酯酶1(hCE-1)对溴氰菊酯的活性明显高于1类大鼠CE水解酶A和B以及2类人CE(hCE-2);然而,水解酶A代谢乙氰菊酯的速度比hCE-1快2倍,而水解酶B和hCE-1以相同的速率水解乙氰菊酯。这些研究表明,大鼠和人肝脏微粒体中溴氰菊酯生物转化的体外途径存在显著的种属差异,这部分归因于大鼠和人羧酸酯酶固有活性的差异。

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