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Enhancement of Oral Bioavailability of Pentoxifylline by Solid Lipid Nanoparticles Publisher Pubmed



Varshosaz J1 ; Minayian M2 ; Moazen E1
Authors
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Authors Affiliations
  1. 1. Department of Pharmaceutics, Isfahan University of Medical Science, Isfahan Pharmaceutical Sciences Research Center, 81746-73461, Isfahan, Hezar Jarib St., Iran
  2. 2. Isfahan Pharmaceutical Sciences Research Center, Isfahan, Iran

Source: Journal of Liposome Research Published:2010


Abstract

Pentoxifylline (PTX) is a highly water-soluble, hemorheologic drug that undergoes first-pass effect with 20% bioavailability. The solid lipid nanoparticles (SLNs) of PTX were prepared to enhance its oral bioavailability by homogenization, followed by the sonification method. Seven different variables, each at two levels, were studied: lipid type, surfactant type and concentration, speed of homogenizer, acetone:dichloromethane (DCM) ratio, lecithin:lipid ratio, and sonication time. The mean particle size and size distribution, drug entrapment efficiency (EE%), zeta potential, and drug release of the SLNs were investigated. A pharmacokinetic study was conducted in male Wistar rats after oral administration of 10mg kg -1 PTX in the form of free drug or SLNs. The z-average particle size, zeta potential, and EE% of the SLNs were at least 250nm,-30.2 mV, and 70%, respectively. Among the studied factors, the lipid type, surfactant type, and percentage had a significant effect on the particle size. Zeta potential was more affected by lipid type, acetone:DCM ratio, and sonication time. Speed of homogenizer and acetone:DCM ratio had a significant effect on the EE%. The optimized SLN was prepared by 80mg of cetyl alcohol, 10mg of lecithin, acetone:DCM ratio (1:2), 30-second sonication, 3% Tween 20, and a mixing rate of 800rpm. In vitro drug release lasted for about 5 hours. It was found that the relative bioavailability of PTX in SLNs was significantly increased, compared to that of the PTX solution. SLNs offer a promising approach to improve the oral bioavailability of PTX that is affected by a high first-pass effect. © 2010 Informa UK Ltd.
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