In vivo pharmacokinetics of ginsenoside compound K mediated by gut microbiota

Author:

Deng Ming-Si,Huang Su-tian-zi,Xu Ya-Ni,Shao Li,Wang Zheng-GuangORCID,Chen Liang-Jian,Huang Wei-Hua

Abstract

Ginsenoside Compound K (GCK) is the main metabolite of natural protopanaxadiol ginsenosides with diverse pharmacological effects. Gut microbiota contributes to the biotransformation of GCK, while the effect of gut microbiota on the pharmacokinetics of GCK in vivo remains unclear. To illustrate the role of gut microbiota in GCK metabolism in vivo, a systematic investigation of the pharmacokinetics of GCK in specific pathogen free (SPF) and pseudo-germ-free (pseudo-GF) rats were conducted. Pseudo-GF rats were treated with non-absorbable antibiotics. Liquid chromatography tandem mass spectrometry (LC–MS/MS) was validated for the quantification of GCK in rat plasma. Compared with SPF rats, the plasma concentration of GCK significantly increased after the gut microbiota depleted. The results showed that GCK absorption slowed down, Tmax delayed by 3.5 h, AUC0-11 increased by 1.3 times, CLz/F decreased by 0.6 times in pseudo-GF rats, and Cmax was 1.6 times higher than that of normal rats. The data indicated that gut microbiota played an important role in the pharmacokinetics of GCK in vivo.

Funder

the National Natural Scientific Foundation of China

the Hunan Provincial Natural Science Foundation of China

the Scientific Research Program of Furong laboratory

the Scientific Research Project of Department of Education of Hunan Province

Publisher

Public Library of Science (PLoS)

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