Absorption, tissue distribution, tissue metabolism and safety of α-mangostin in mangosteen extract using mouse models

Young Hee Choi, Seung Yon Han, You Jin Kim, Young Mi Kim, Young Won Chin

Research output: Contribution to journalArticlepeer-review

49 Scopus citations

Abstract

The commercially available herbal products as the form of extract were usually mixtures containing various compounds. In spite of the purported efficacy in each active constituent, the coexisting constituents in the herbal extract might interfere with the efficacy and safety and affect the pharmacokinetic properties of active constituents. To compare for the pharmacokinetic properties of α-mangostin, a major bioactive compound, in mangosteen extract and pure α-mangostin, the pharmacokinetics as well as tissue distribution, in vitro metabolism, plasma protein binding and safety evaluation were conducted in mice because a mouse model is required a small amount of compounds and useful to develop disease models. The absorption of α-mangostin was increased and hepatic metabolism of α-mangostin was decreased in mice treated with mangosteen extract. However, the intestinal metabolism α-mangostin is comparable and still extensive in mice treated with α-mangostin and mangosteen extract. Intraperitorial LC50 of α-mangostin and mangosteen extract was 150 and 231mg/kg, respectively. These findings may be valuable to explain the different pharmacokinetics and safety of α-mangostin and mangosteen extract. Furthermore, these findings are useful to design the efficacy and safety investigation of α-mangostin or mangosteen extract in mice with disease models or combination therapies to extrapolate into the clinical levels.

Original languageEnglish
Pages (from-to)140-146
Number of pages7
JournalFood and Chemical Toxicology
Volume66
DOIs
StatePublished - Apr 2014

Keywords

  • α-Mangostin
  • Absorption
  • Mangosteen extract
  • Mouse
  • Pharmacokinetics
  • Safety

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