Electrohydrodynamic encapsulation of cisplatin in poly (lactic-co-glycolic acid) nanoparticles for controlled drug delivery
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Single step electrohydrodynamic atomization was used to produce cisplatin encapsulated PLGA polymer particles.

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The versatility of the method in controlling the size and drug loading of the particles by variation of drug:polymer ratios and operating conditions was demonstrated.

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Compared to conventional nanoparticle production methods, particles generated by electrohydrodynamic atomization proved to have higher encapsulation efficiencies (> 70%).

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The distribution of the drug with various concentrations within the polymeric particles was further studied with SEM-TEM/EDX methods and compared against the unloaded particles.

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In-vitro release data were analysed and it was shown that all the formulations tested exhibited an initial burst release followed by a sustained release period.

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While the release data fit best with the Ritger-Peppas model, it was shown that it is not possible to attribute the largest difference in initial release rate entirely to particle size.

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This study highlights the enhanced functionality due to particle morphology and drug concentration, which enables the potential for high cisplatin encapsulation and tunable release.

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