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在体和离体评估伊维菌素和丹诺氟沙星在绵羊体内的相互作用。

In vivo and ex vivo assessment of the interaction between ivermectin and danofloxacin in sheep.

机构信息

Laboratorio de Farmacología, Departamento de Fisiopatología, Facultad de Ciencias Veterinarias, Universidad Nacional del Centro, Campus Universitario, Paraje Arroyo Seco, Tandil, Argentina.

出版信息

Vet J. 2012 Jun;192(3):422-7. doi: 10.1016/j.tvjl.2011.09.006. Epub 2011 Nov 12.

Abstract

The impact of an efflux pump-related interaction between ivermectin and danofloxacin on their intestinal transport (ex vivo) and disposition kinetics (in vivo) was assessed. Eighteen male Corriedale sheep were randomly assigned to one of three groups. Animals in Group A received 0.2mg/kg ivermectin by SC injection, those in Group B were given 6 mg/kg danofloxacin SC on two occasions 48 h apart and those in Group C were treated with both compounds at the same rates. Plasma concentrations of ivermectin and danofloxacin were measured by HPLC using fluorescence detection. Ex vivo intestinal drug transport activity was measured by the use of the Ussing chamber technique. Plasma concentrations of ivermectin in the first 6 days after injection tended to be higher in Group C than Group A. Contemporaneous treatment with ivermectin significantly increased systemic exposure to danofloxacin (AUC values were 32-35% higher) and prolonged the elimination half-life of danofloxacin (40-52% longer). Ex vivo, incubation with ivermectin significantly decreased the efflux transport of rhodamine 123, a P-glycoprotein substrate, in sheep intestine, but no significant effect of danofloxacin on transport activity was observed. Evaluation of the interaction of danofloxacin with the breast cancer resistance protein (BCRP) showed that pantoprazole and ivermectin significantly decreased danofloxacin secretion in the rat intestine. Thus, the ivermectin-induced reduction of danofloxacin efflux transport observed in this study may involve BCRP activity but the involvement of P-glycoprotein cannot be ruled out.

摘要

评估了伊维菌素和丹氟沙星之间外排泵相关相互作用对其肠道转运(离体)和处置动力学(体内)的影响。18 只雄性科里代尔羊被随机分配到三组之一。A 组动物经 SC 注射给予 0.2mg/kg 伊维菌素,B 组动物两次 SC 给予 6mg/kg 丹氟沙星,间隔 48 小时,C 组动物以相同速率给予两种化合物。采用荧光检测的 HPLC 法测定伊维菌素和丹氟沙星的血浆浓度。通过使用 Ussing 室技术测量离体肠道药物转运活性。注射后第 6 天,C 组伊维菌素的血浆浓度较 A 组高,有升高趋势。同时给予伊维菌素可显著增加丹氟沙星的全身暴露量(AUC 值增加 32-35%)并延长丹氟沙星的消除半衰期(延长 40-52%)。离体孵育时,伊维菌素显著降低了羊肠中 rhodamine 123 的外排转运,而 rhodamine 123 是 P-糖蛋白的底物,但丹氟沙星对转运活性没有显著影响。评价丹氟沙星与乳腺癌耐药蛋白(BCRP)的相互作用表明,泮托拉唑和伊维菌素可显著减少大鼠肠内丹氟沙星的分泌。因此,本研究中观察到的伊维菌素诱导丹氟沙星外排转运减少可能涉及 BCRP 活性,但不能排除 P-糖蛋白的参与。

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