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In vivo behavior of MIL-100 nanoparticles at early times after intravenous administration

体内分布 纳米载体 药代动力学 体内 药理学 药物输送 间隙 化学 药品 脾脏 分布(数学) 医学 内科学 生物 生物技术 有机化学 泌尿科 数学分析 数学
作者
Teresa Simón‐Yarza,Tarek Baâti,Fadoua Neffati,Leïla Njim,Patrick Couvreur,Christian Serre,Ruxandra Gref,Mohamed Fadhel Najjar,Abdelfatteh Zakhama,Patricia Horcajada
出处
期刊:International Journal of Pharmaceutics [Elsevier BV]
卷期号:511 (2): 1042-1047 被引量:76
标识
DOI:10.1016/j.ijpharm.2016.08.010
摘要

Metal-organic frameworks have shown interesting features for biomedical applications, such as drug delivery and imaging agents. The benchmarked mesoporous iron(III) trimesate MIL-100 MOF nanocarrier combines progressive release of high drug cargoes with absence of visible in vivo toxicity. Although in a previous study pharmacokinetics and biodistribution of MIL-100 nanoparticles were evaluated in the long term (from 24 h to 1 month), the crucial times for drug targeting and delivery applications are shorter (up to 24 h). Thus, this work aims to study the blood circulating profile and organ accumulation of MIL-100 nanocarrier at early times after administration. For this purpose, after intravenous administration to rats, both constitutive components of MIL-100 (trimesate and iron) were quantified by high performance liquid chromatography and a spectrophotometric method, respectively. The pharmacokinetic profile suggested that the nanoparticles act as a depot in the blood stream during the first hours before being cleared. Accumulation took mainly place in the liver and, in some extent, in the spleen. Nevertheless, histological studies demonstrated the absence of morphological alterations due to the presence of the particles in these organs. Liver function was however slightly altered as reflected by the increased plasma aspartate aminotransferase concentrations. Finally trimesate was progressively eliminated in urine.
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