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静脉注射脂质体苯硝唑作为杀锥虫剂:增加药物向肝脏的递送是不够的。

Intravenous liposomal benznidazole as trypanocidal agent: increasing drug delivery to liver is not enough.

作者信息

Morilla M J, Montanari J A, Prieto M J, Lopez M O, Petray P B, Romero E L

机构信息

Laboratorio de Diseño de Transportadores de Drogas, Universidad Nacional de Quilmes, Roque Saenz Peña 180, Bernal, B1876BXD Buenos Aires, Argentina.

出版信息

Int J Pharm. 2004 Jul 8;278(2):311-8. doi: 10.1016/j.ijpharm.2004.03.025.

Abstract

With the aim of investigating if delivery of benznidazole (BNZ) to liver could be increased by incorporating the drug in multilamellar liposomes, single bolus of free BNZ or liposomal BNZ formulations (MLV-BNZ) composed of HSPC:DSPG:Chol 2:1:2 (mol/mol/mol) at 0.7% (w/w) drug/total lipid ratio, were injected by intramuscular (i.m.), subcutaneous (s.c.) and intravenous (i.v.) routes, at 0.2 mg BNZ/kg, in rats. The resulting blood concentrations were followed along 9 h post-injection (p.i.) and drug accumulation in liver was determined after 4 and 9 h p.i. Only upon i.v. injection of MLV-BNZ, a threefold higher BNZ accumulation in liver was obtained, together with blood BNZ concentrations of 1.1 microg/ml (30% lower than the blood BNZ concentration achieved upon i.v. administration of free drug) occurred 4 h p.i. However, such increased liver uptake of BNZ, raised twice a week had no effect on parasitaemia levels of mice infected with the RA strain of Trypanosoma cruzi. Our results indicate that the relationship between increased selectivity for an infected tissue and therapeutic effect is not always straightforward, at least for the MLV-BNZ regimen used in the present study.

摘要

为了研究将苯硝唑(BNZ)包裹在多层脂质体中是否能增加其在肝脏中的递送量,以0.2mg BNZ/kg的剂量,通过肌肉注射(i.m.)、皮下注射(s.c.)和静脉注射(i.v.)途径,给大鼠注射单次推注的游离BNZ或由HSPC:DSPG:Chol 2:1:2(摩尔/摩尔/摩尔)组成、药物/总脂质比为0.7%(w/w)的脂质体BNZ制剂(MLV-BNZ)。在注射后(p.i.)9小时内监测血药浓度,并在注射后4小时和9小时测定肝脏中的药物蓄积量。仅在静脉注射MLV-BNZ时,肝脏中BNZ的蓄积量提高了三倍,且在注射后4小时血中BNZ浓度为1.1μg/ml(比静脉注射游离药物时达到的血中BNZ浓度低30%)。然而,每周两次提高BNZ在肝脏中的摄取量,对感染克氏锥虫RA株的小鼠的寄生虫血症水平没有影响。我们的结果表明,至少对于本研究中使用的MLV-BNZ方案,对感染组织选择性增加与治疗效果之间的关系并非总是直接的。

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