The formation of an inclusion complex between a metabolite of ginsenoside, compound K and γ-cyclodextrin and its dissolution characteristics

Kentaro Igami; Masatoshi Ozawa; Sae Inoue; Daisuke Iohara; Toshitsugu Miyazaki; Masamitsu Shinoda; Makoto Anraku; Fumitoshi Hirayama; Kaneto Uekama

doi:10.1111/jphp.12468

The formation of an inclusion complex between a metabolite of ginsenoside, compound K and γ-cyclodextrin and its dissolution characteristics

J Pharm Pharmacol. 2016 May;68(5):646-54. doi: 10.1111/jphp.12468. Epub 2015 Aug 10.

Authors

Kentaro Igami¹, Masatoshi Ozawa², Sae Inoue², Daisuke Iohara³, Toshitsugu Miyazaki¹, Masamitsu Shinoda², Makoto Anraku³, Fumitoshi Hirayama³, Kaneto Uekama³

Affiliations

¹ Research and Development Center, Nagase & Co., Kobe, Hyogo, Japan.
² Research and Development Dept., Nagase Medicals Co., Itami, Hyogo, Japan.
³ Faculty of Pharmaceutical Sciences, Sojo University, Kumamoto, Japan.

PMID: 26255976
DOI: 10.1111/jphp.12468

Abstract

Objectives: 20S-protopanaxadiol 20-O-β-D-glucopyranoside (compound K), a metabolite of ginsenoside, is only sparingly soluble in water. The aim of this study was to improve the low solubility, slow dissolution rate and low oral bioavailability of compound K by forming an inclusion complex with γ-cyclodextrin (γ-CyD), and to compare the results with those of β-CyD complex.

Methods: The interactions of compound K with β and γ-CyDs were studied by the solubility method and proton nuclear magnetic resonance spectroscopy. Solid forms of compound K/CyD complexes with different molar ratios were prepared by the kneading method, and the resulting complex was characterized by powder X-ray diffractometry. The dissolution rate of the complexes was measured by the rotary disk method. In-vivo absorption studies in rats were carried out, and the serum level of compound K, after its oral administration, was measured by a liquid chromatography-tandem mass spectrometry system.

Key findings: γ-CyD markedly improved the low solubility of compound K at lower CyD concentrations (<0.03 M), whereas the solubility was decreased at higher concentrations (>0.06 m). The enhancement in solubility by γ-CyD at a lower concentration was much higher than the corresponding values for β-CyD. The apparent 1:1 stability constant (1.5 × 10(5) m(-1) ) for the γ-CyD complex was 18-fold larger than that (8.2 × 10(3) m(-1) ) of the β-CyD complex. The dissolution rate of the 1:1 compound K/γ-CyD complex was faster than that for the 1:3 (guest : host) complex. These results suggest that the dissolution rate of the 1:1 complex, in which the drug is partially included, was faster than that of the 1:3 complex, in which the drug was completely included, due to the higher solubility and amorphous property of the former complex compared with the properties of the latter complex. The fast dissolution of the γ-CyD complex was reflected in the maximum plasma level (Cmax ) of the drug and the time (Tmax ) to reach the maximum plasma level after its oral administration to rats.

Conclusions: The effect of γ-CyD on enhancing the solubility of compound K is much higher than that for the β-CyD complex, and the dissolution rate of the guest when it is partially included in the γ-CyD is faster the corresponding value when it is completely included in the cavity.

Keywords: bioavailability; compound K; ginsenoside; inclusion complex; γ-cyclodextrin.

Publication types

Comparative Study

MeSH terms

Administration, Oral
Animals
Biological Availability
Chromatography, High Pressure Liquid
Crystallography, X-Ray
Drug Compounding
Gastrointestinal Absorption
Ginsenosides / administration & dosage
Ginsenosides / blood
Ginsenosides / chemistry*
Ginsenosides / pharmacokinetics
Male
Powder Diffraction
Proton Magnetic Resonance Spectroscopy
Rats, Sprague-Dawley
Solubility
Tandem Mass Spectrometry
Technology, Pharmaceutical / methods
beta-Cyclodextrins / chemistry
gamma-Cyclodextrins / chemistry*

Substances

Ginsenosides
beta-Cyclodextrins
gamma-Cyclodextrins
ginsenoside M1