Sorbitan ester organogels for transdermal delivery of sumatriptan

The partial phase behavior, theological, and drug release characteristics of an organogel (OG) composed of water, isooctane and sorbitan esters, sorbitan monopalmitate (Span-40) and poly(oxyethylene)sorbitan monostearate (Polysorbate-60) were studied. Phase diagrams showed decreasing areas of optically isotropic organogel region depending on the surfactant ratio, K-W and drug incorporation. The nonbirefringent, clear isotropic solution suggested the reverse micellar/microemulsion nature of the organogel without any molecular ordering. The increase in drug concentration in OGs leads to increase in the viscosity and sol-gel transition temperature (T-g). Fractal dimension (d(f)) values calculated for different compositions suggested that the density of the tubular network increases with increasing drug concentration in OGs. The release rate of the drug from OGs was found to be non-Ficklan through the dialysis membrane. The permeation rate of sumatriptan from pig skin was 0.231 mg/h/cm(2) (781.9 nmol/h/cm(2)). The study indicates potential of OG as a reservoir system for transdermal drug delivery.