Using transdermal iontophoresis to increase granisetron delivery across skin in vitro and in vivo: effect of experimental conditions and a comparison with other enhancement strategies.

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RESEARCH PRODUCT

Using transdermal iontophoresis to increase granisetron delivery across skin in vitro and in vivo: effect of experimental conditions and a comparison with other enhancement strategies.

Yogeshvar N. Kalia Alicia López-castellano Adriana Ganem-rondero Virginia Merino David Quintanar-guerrero Jennyfer Cázares-delgadillo

subject

Male medicine.drug_class Swine Pharmaceutical Science Iontophoresis/methods Pharmacology In Vitro Techniques Granisetron Administration Cutaneous High-performance liquid chromatography Granisetron Pharmacokinetics In vivo Limit of Detection Granisetron/administration & dosage/pharmacokinetics Skin/metabolism Medicine Antiemetic Animals Rats Wistar Chromatography High Pressure Liquid Transdermal Skin ddc:615 Iontophoresis business.industry Half-life Iontophoresis Antiemetics/administration & dosage/pharmacokinetics Rats Serotonin Antagonists/administration & dosage/pharmacokinetics Area Under Curve Antiemetics Serotonin Antagonists business medicine.drug Half-Life

description

The objectives of the study were (i) to investigate the effect of experimental parameters on the iontophoretic transport of granisetron, (ii) to identify the relative contributions of electromigration (EM) and electroosmosis (EO), (iii) to determine the feasibility of delivering therapeutic amounts of drug for the treatment of chemotherapy-induced nausea and vomiting and (iv) to test the in vitro results in a simple animal model in vivo. Preliminary in vitro studies using aqueous granisetron formulations investigating the effect of drug concentration (5, 10, 20 and 40 mM) and current density (0.1, 0.2, 0.3 mA cm(-2)) were performed using porcine ear skin. As expected, cumulative delivery in vitro at the 20 and 40 mM concentrations was significantly greater than that at 5 and 10mM, which were not statistically different (p<0.05). Increasing the applied current density from 0.1 to 0.3 mA cm(-2) resulted in a approximately 4.2-fold increase in iontophoretic flux. Furthermore, in the absence of Na(+) in the formulation, no dependence of iontophoretic flux on drug concentration was reported (at a granisetron concentration of 40 mM, the transport rate was 2.93+/-0.62 microg cm(-2)min(-1)). Co-iontophoresis of acetaminophen was used to show that EM was the predominant transport mechanism accounting for 71-86% of total granisetron delivery. In vivo studies in Wistar rats (40 mM granisetron; application of 0.3 mA cm(-2) for 5h with Ag/AgCl electrodes and salt bridges) showed an average iontophoretic input rate (k(input)) of 0.83+/-0.26 microg min(-1) and a maximum plasma concentration (C(max)) of 0.092+/-0.004 microg ml(-1). Based on these results and given the known pharmacokinetics, transdermal iontophoresis could achieve therapeutic drug levels for the management of chemotherapy-induced emesis using a reasonably sized (4-6 cm(2)) patch.

year	journal	country	edition	language
2010-03-01	European journal of pharmaceutical sciences : official journal of the European Federation for Pharmaceutical Sciences

10.1016/j.ejps.2010.01.008 https://pubmed.ncbi.nlm.nih.gov/20096354