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甲巯咪唑对阿苯达唑口服生物利用度的增强作用及其对小鼠旋毛虫肠外期的驱虫效果:剂量方案的影响

Methimazole-mediated enhancement of albendazole oral bioavailability and anthelmintic effects against parenteral stages of Trichinella spiralis in mice: the influence of the dose-regime.

作者信息

López-García M L, Torrado S, Torrado S, Martínez A R, Bolás F

机构信息

Departamento de Parasitología, Facultad de Farmacia, Universidad Complutense, Madrid, Spain.

出版信息

Vet Parasitol. 1998 Feb 28;75(2-3):209-19. doi: 10.1016/s0304-4017(97)00177-5.

Abstract

The influence of methimazole (MTZ) inhibitor of the microsomal oxidases on the systemic availability of the albendazole sulpho-metabolites (ABZS-MT) albendazole-sulphoxide (ABZSO) and albendazole-sulphone (ABZSO2) and on its anthelmintic effects was investigated in a mouse model for helminthic infections. Plasma concentrations of the ABZS-MT were measured by high performance liquid chromatography (HPLC) following treatment of Swiss CD-1 mice with albendazole (ABZ) alone or ABZ plus MTZ, at both single and repeated doses. The anthelmintic effects were assessed in age-matched mice similarly treated following infection with Trichinella spiralis. MTZ significantly (p < 0.01) increased the ABZS-MT plasma concentrations although the pharmacokinetic profile varied greatly according to the dose of ABZ administered. When ABZ was given at a single dose of 50 mg/kg followed by MTZ at 3 mg/kg, a cumulative effect was observed in the ABZS-MT plasma levels with pharmacokinetic parameters (Tmax = 24 h, Cmax= 30.88 microg/ml and AUC = 1120.80 microg h/ml) significantly ( p < 0.01) higher than those following administration of ABZ alone (Tmax = 3 h, Cmax = 11.00 microg/ml and AUC = 268.03 microg h/ml). This cumulative effect was absent following administration of ABZ at 100 mg/kg where, after reaching a maximum (Cmax = 27.23 microg/ml) at 3 h post-administration (Tmax), the ABZS-MTplasma levels felt down quickly to values under those obtained after administration of ABZ at the same dose, but alone (AUC = 362.15 microg h/ml vs. 340.15 microg h/ml, respectively). When ABZ was given at 50 mg/kg together with MTZ three times every 24 h, a rapid decrease was observed in the ABZS-MT plasma levels following administration of both the second and third doses, respectively. The pharmacokinetic profile of ABZS-MT following administration of each of the three doses of ABZ at 100 mg/kg plus MTZ was the same as that obtained after the single treatment. The rapid decrease of the ABZS-MT plasma levels observed after the sustained treatment or after the single treatment at 100 mg/kg could be due to a microsomal oxidase inductive effect (probably the cytochrome P-450) caused by ABZSO. The co-administration of MTZ significantly (p < 0.01) increased the anthelmintic effects of ABZ against both migrating and encysted larvae of T. spiralis. Repeated treatment did not improve the anthelmintic effects of the single treatment as the efficacies against both stages of the parasite were always lower or identical to those of the single treatment at the corresponding doses.

摘要

在蠕虫感染的小鼠模型中,研究了微粒体氧化酶抑制剂甲巯咪唑(MTZ)对阿苯达唑硫代谢物(ABZS-MT)阿苯达唑亚砜(ABZSO)和阿苯达唑砜(ABZSO2)的全身可用性及其驱虫效果的影响。在用阿苯达唑(ABZ)单独或ABZ加MTZ处理瑞士CD-1小鼠后,通过高效液相色谱法(HPLC)测量单次和重复剂量下ABZS-MT的血浆浓度。在用旋毛虫感染后,对年龄匹配的、接受类似处理的小鼠的驱虫效果进行评估。MTZ显著(p<0.01)提高了ABZS-MT的血浆浓度,尽管药代动力学特征根据ABZ给药剂量的不同而有很大差异。当以50mg/kg的单次剂量给予ABZ,随后以3mg/kg给予MTZ时,在ABZS-MT血浆水平上观察到累积效应,其药代动力学参数(Tmax = 24小时,Cmax = 30.88μg/ml,AUC = 1120.80μg h/ml)显著(p<0.01)高于单独给予ABZ后的参数(Tmax = 3小时,Cmax = 11.00μg/ml,AUC = 268.03μg h/ml)。在以100mg/kg给予ABZ后不存在这种累积效应,给药后3小时(Tmax)达到最大值(Cmax = 27.23μg/ml)后,ABZS-MT血浆水平迅速下降至低于相同剂量但单独给予ABZ后获得的值(AUC分别为362.15μg h/ml和340.15μg h/ml)。当以50mg/kg给予ABZ并每24小时与MTZ一起给药三次时,在分别给予第二剂和第三剂后,观察到ABZS-MT血浆水平迅速下降。在以100mg/kg给予三剂ABZ加MTZ后,ABZS-MT的药代动力学特征与单次治疗后获得的相同。在持续治疗后或在100mg/kg单次治疗后观察到的ABZS-MT血浆水平的迅速下降可能是由于ABZSO引起的微粒体氧化酶诱导作用(可能是细胞色素P-450)。MTZ的共同给药显著(p<0.01)提高了ABZ对旋毛虫迁移期幼虫和包囊期幼虫的驱虫效果。重复治疗并未改善单次治疗的驱虫效果,因为对寄生虫两个阶段的疗效始终低于或等同于相应剂量下单次治疗的疗效。

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