医療薬学
Online ISSN : 1882-1499
Print ISSN : 1346-342X
ISSN-L : 1346-342X
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生物学的利用能向上を目指したグリチルリチン直腸投与製剤に関する基礎的検討
古閑 健二郎竹腰 久美子鍛治 聡畑 友佳子小倉 勤藤下 修
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2006 年 32 巻 2 号 p. 154-163

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We investigated the usefulness of a suppository containing highly concentrated glycyrrhizin monoammonium (GZ-NH4) solution prepared by pretreatment with clove oil in rats. The aims of this study were to clarify membrane permeability, the bioavailability of GZ-NH4 and the extent of tissue damage. Membrane permeability was evaluated using Ussing-type diffusion chambers, bioavailability assessed through an in vivo absorption study, tissue damage evaluated through observation of hematoxylin-eosin stained tissues and an in vitro release study was carried out to select the suppository base. The formulations used were a GZ-NH4 solution prepared using phosphate buffered solution (control), GZ-NH4 containing 50% labrasol, and GZ-NH4 pretreated with 2% clove oil at 50°C and 70°C. The GZ-NH4 concentrations of all formulations were set to 50 mg/mL. With the GZ-NH4 pretreated with 2% clove oil formulations, the apparent permeability coefficients (Papp) were 1.7- and 1.9-fold higher, respectively, than that of the control formulation. When the various formulations were applied to the rat rectum at a dose of 50 mg/kg of GZ-NH4, the bioavailability of GZ-NH4 pretreated with 2% clove oil at 70°C was 25%, the highest among the four formulations. In the in vivo absorption study, no damage to the epithelial cells of the rectum was observed. These results suggest that GZ-NH4 pretreated with 2% clove oil at 70°C is the most useful formulation for rectal administration. In the in vitro release study to select suppository base, polyethyleneglycol 1000 (PEG 1000) was selected as the hydrophilic base and Witepsol H-15 as the lipophilic base. The initial release of GZ-NH4 was highest for the Witepsol H-15 suppository base. Overall, our results suggest that a lipophilic suppository containing GZ-NH4 pretreating with 2% clove oil at 70°C has the highest release and absorption rates for GZ-NH4 in rectal administration.
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© 2006 日本医療薬学会
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