Desenvolvimento e avaliação da atividade e farmacocinética de nanopartículas lipídicas sólidas contendo a associação de quinina e doxiciclina / Development and evaluation of the activity and pharmacokinetics of solid lipid nanoparticles loaded with the association of Quinine and Doxycycline

AUTOR(ES)
FONTE

IBICT - Instituto Brasileiro de Informação em Ciência e Tecnologia

DATA DE PUBLICAÇÃO

2011

RESUMO

Malaria is one of the most devastating tropical diseases caused by intracellular protozoan parasites of the genus Plasmodium. More than 3 billion people live in malarial endemic regions. Five species of Plasmodium (falciparum, vivax, ovale, malariae and knowlesi) cause disease in humans and infection with P. falciparum, the most deadly of these parasites, results in more than 1 million deaths annually. The development of resistance to traditional antimalarial drugs leads to the use of drug combinations such as quinine (QN)/doxycycline (DOX). In this context, the aims of this work were to develop and characterize solid lipid nanoparticles (SLN) loaded with QN/ DOX, to evaluate their efficacy in an in vivo model of berghei malaria, and to determine their pharmacokinetics and erythrocyte partition coefficient compared to the non-encapsulated (free) drug association. The SLN were prepared by high pressure homogenization technique using polysorbate 80 and Lipoid® as emulsifiers and cetyl palmitate as lipid matrix. In the preliminary stability study, QN/DOX-loaded SLN (2.0/0.2 mg/mL) presented adequate particle size (152.8 ± 5.26 nm), polydispersion index (0.173 ± 0.006), zeta potential (-38.6 ± 1.82 mV), high drug content (95.9% ± 0.70/94.1% ± 2.41) and appropriate encapsulation efficiency (94.2% ± 1.14/83.0% ± 2.52) after 21 days of storage at room temperature. For the assay analysis, a fast and specific liquid chromatography-tandem mass spectrometry (LC-MS/MS) method was developed and validated for the simultaneous determination of QN and DOX. The LC-MS/MS method was carried out on a Sun Fire Waters C18 column (50 mm x 3.0 mm I.D.) and the mobile phase consisted of acetonitrile:0.1% formic acid (75:25, v/v), run at a flow rate of 0.45 mL/min (split 1:3). The injection volume was 10 ¿L. Plasmodium berghei infected Wistar rats were used to evaluate the efficacy of QN/DOX-loaded SLN using different dosing regimens. The effective QN/DOX-loaded SLN i.v. (75/7.5 mg/kg/day) and oral (105/10.5 mg/kg/day) doses represent an almost 30% reduction compared to the free drugs in association. Plasma pharmacokinetics was evaluated after administration of free or nanoencapsulated QN/DOX by i.v. (10/1 mg/kg) and oral (25/2.5 mg/kg) routes to infected Wistar rats. For the quantification of the rat plasma samples, a fast, sensitive and specific LC-MS-MS method was developed and validated for the determination of QN and DOX. QN, DOX and cimetidine (internal standard, IS) were extracted from the plasma by protein precipitation and the mobile phase consisted of methanol/formic acid 0.1% (70:30, v/v), run at a flow rate of 0.5 mL/min (split 1:3). Detection was carried out by positive Electrospray Ionization in multiple reaction monitoring mode, monitoring the transitions 325.0>307.0, 445.0>428.1 and 252.8>159.0, for QN, DOX and IS, respectively. The analysis was carried out in 2.0 min and the method was linear in the plasma concentration range of 5-5000 ng/mL. No significant alteration of pharmacokinetic parameters was observed for both drugs and routes of dosing after nanoencapsulation. QN partition coefficient into P. berghei infected erythrocyte was increased (5.53 ± 0.28) when the QN/DOX-loaded SLN was used in comparison with the free drugs in association (3.81 ± 0.23). No significant alteration on DOX erythrocyte partition coefficient was observed. In summary, the results showed that QN/DOX nanoencapsulation into SLN allows the reduction of the effective antimalarial dose being an interesting alternative to be investigated for the treatment of falciparum resistant malaria.

ASSUNTO(S)

quinina quinine doxiciclina doxycycline nanoparticulas solid lipid nanoparticles plasmodium berghei malária malaria farmacocinética pharmacokinetics erythrocyte partition coefficient lc-ms/ms

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