Publication | Open Access
Evaluation of Metabolic Stability of Kinsenoside, an Antidiabetic Candidate, in Rat and Human Liver Microsomes
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Citations
6
References
2015
Year
GlycobiologyOxidative StressBioanalysisHepatotoxicityHealth SciencesMetabolic StabilityBiochemistryLiver PhysiologyAnoectochilus FormosanusGood Metabolic StabilityHuman Liver MicrosomesAntidiabetic CandidateMetabolomicsPharmacologyDrug-induced Liver InjuryDiabetesPhysiologyMetabolic RegulationMetabolismMedicine
Kinsenoside is a principle bioactive compound of Anoectochilus formosanus. It exhibits various pharmacological effects such as antihyperglycemic, antioxidant, anti-inflammatory, immunostimulating, and hepatoprotective activities and has recently been developed as an antidiabetic drug candidate. In this study, as part of an in vitro pharmacokinetic study, the stability of kinsenoside in rat and human liver microsomes was evaluated. Kinsenoside was found to have good metabolic stability in both rat and human liver microsomes. These results will provide useful information for further in vivo pharmacokinetic and metabolism studies.
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