Preparation, Characterization and in vitro Release Studies of Enoxaparin in Nanoparticle form and Enterically Coated Tablets Containing Different Enhancers

In the past decade, many strategies have been developed to enhance oral drug delivery. differenttechniques were investigated, amongst those the use of permeation enhancers such surfactants and biodegradable polymers were studied more extensively. chitosan derivatives have been studied as permeation enhancer in free soluble form and as nanoparticulate systems. the aim of the currentwork was to develop a nanoparticulate system based on ionic interaction between trimethyl chitosan (tmc) and enoxaparin as well as enterically coated enoxaparin tablets containingsurfactants such as tween 80 and sodium lauryl sulfate (sls) as permeation enhancer. theprepared nanoparticles were characterized for size, zeta potential, loading capacity and in vitrorelease. the tablets were enterically coated using acryl-eze®, characterized physically and wereassayed for their content. the release of enoxaparin was studied in pbs ph 6.8 corresponding tothe ph of small intestine. the result suggested that the nanoparticles were positively charged witha diameter of about 120 nm and loading capacity of around 95%. the tablets contained 60 mg ofenoxaparin, 10 mg of surfactants as enhancer. the in vitro release from tablets showed almost 100% enoxaparin release in 2 hours; whereas in nanoparticles there was a 67.5% release in 24 hours. the result suggests that the enhancing effect of the systems may be useful for oral enoxaparin tablets. in order to better evaluate the enhancing effect of the polymer with the surfactants as well as the oral tablets with nanoparticulate systems further ex vivo and in vivo studies are required.