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http://dx.doi.org/10.5142/JGR.2005.29.1.037

The Inhibitory Effects of Korean Red Ginseng Saponins on 5- HT3A Receptor Channel Activity Are Coupled to Anti-Nausea and Anti-Vomiting Action  

Kim Jong-Hoon (Research Laboratory for the Study of Ginseng Signal Transduction and Dept. of Physiology College of Veterinary Medicine, Konkuk University)
Lee Byung-Hwan (Research Laboratory for the Study of Ginseng Signal Transduction and Dept. of Physiology College of Veterinary Medicine, Konkuk University)
Jeong Sang Min (Research Laboratory for the Study of Ginseng Signal Transduction and Dept. of Physiology College of Veterinary Medicine, Konkuk University)
Nah Seung-Yeol (Research Laboratory for the Study of Ginseng Signal Transduction and Dept. of Physiology College of Veterinary Medicine, Konkuk University)
Publication Information
Journal of Ginseng Research / v.29, no.1, 2005 , pp. 37-43 More about this Journal
Abstract
We performed in vitro and in vivo studies to know whether the inhibitory effects of ginsenosides on $5-HT_{3A}$ receptor channel acctivity are coupled to anti-nausea and anti-vomiting action. In vitro study, we investigated the effect of compound K (CK) and M4, which are ginsenoside metabolites, on human $5-HT_{3A}$ receptor channel activity expressed in Xenopus oocytes using two-electrode voltage clamp technique. Treatment of CK or M4 themselves had no effect in both oocytes injected with $H_2O\;and\;5-HT_{3A}$ receptor cRNA. In oocytes injected with $5- HT_{3A}$ receptor cRNA, M4 treatment inhibited more potently 5-HT-induced inward peak current $(I_{5-HT})$ than CK with dose-dependent and reversible manner. The half-inhibitory concentrations $(IC_{50})$ of CK and M4 were $36.9\;\pm\;10.1\;and\;7.3\;\pm\;2.2\;{\mu}M$, respectively. The inhibition of $I_{5-HT}$ by M4 was non-competitive and voltage-independent. These results indicate that M4 might regulate $5-HT_{3A}$ receptors. In vivo experiments, injection of cisplatin (7.5 mg/kg, i.v.) induced both nausea and vomiting with 1 h latency. These episodes reached to peak after 2 h and persisted for 4 h. Pre-treatment of GTS (500 mg/kg, p.o.) significantly reduced cisplatin-induced nausea and vomiting by $51\;\pm\;8.4\;and\;48.8\;\pm\;6.4\%$ during 4 h compared to GIS­untreated group, respectively. These results show the possibility that in vitro inhibition of $5-HT_{3A}$ receptor channel activity by ginsenosides might be coupled to in vivo anti-emetic activity.
Keywords
Panax ginseng; ginsenoside metabolites; 5-HT_{3A} receptor; cisplatin; emesis;
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