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  • Solid dispersion formulations of megestrol acetate with copovidone for enhanced dissolution and oral bioavailability.

Solid dispersion formulations of megestrol acetate with copovidone for enhanced dissolution and oral bioavailability.

Archives of pharmacal research (2011-04-07)
Soon Wook Hong, Bong Sang Lee, Su Jun Park, Hong Ryeol Jeon, Ki Young Moon, Mean Hyung Kang, Sang Han Park, Sung-Up Choi, Woo Heon Song, Jaehwi Lee, Young Wook Choi
ABSTRACT

In order to enhance the dissolution profile and oral bioavailability of megestrol acetate (MA), solid dispersions of MA (MASDs) were formulated with copovidone and crystal sugar as a hydrophilic polymeric carrier and an inert core bead, respectively. Solvent evaporation method and fluidized bed coating technique were employed. MASDs were categorized as crystalline solid dispersion by the characterization of differential scanning calorimetry and X-ray diffraction. The mass-median diameters of MASDs were in a range of 1.4 to 2.6 μm. Based on drug to polymer ratio, MASD (1:1) and (1:2) were considered as optimized formulations, resulting in a smooth-surfaced homogeneously coated layer with enhanced dissolution rate. Dissolution of MASD was gradually increased up to 15 min, after which it reached a plateau. For the initial period, dissolution rates were in the decreasing order of MASD (1:2) ≥ MASD (1:1) > MASD (1:3) > MASD (1:5) > MASD (1:0.5) > MA powder. In the comparative pharmacokinetic study with Megace OS, a reference drug product, MASD (1:1) showed improved bioavailability of over 220% with 2-fold higher C(max) and 30% faster T(max). We conclude that MASD (1:1) is a good candidate for the development of oral solid dosage forms.

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Solvent Green 3, Dye content 95 %