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Literature DB >> 27619505

Ginsenosides, ingredients of the root of Panax ginseng, are not substrates but inhibitors of sodium-glucose transporter 1.

Shengli Gao¹, Hirotaka Kushida², Toshiaki Makino³.

Abstract

Recent pharmacokinetic studies have revealed that ginsenosides, the major ingredients of ginseng (the roots of Panax ginseng), are present in the plasma collected from subjects receiving ginseng, and speculated that ginsenosides might be actively transported via glucose transporters. We evaluated whether ginsenosides Rb1 and Rg1, and their metabolites from enteric bacteria act as substrates of sodium-glucose cotransporter (SGLT) 1, the major glucose transporter expressed on the apical side of intestinal epithelial cells. First, we evaluated the competing effects of ginseng extract and ginsenosides on the uptake of [14C]methyl-glucose, a substrate of SGLT1, by SGLT1-overexpressing HEK293 cells. A boiling water extract of ginseng inhibited SGLT1 in a concentration-dependent manner with an IC50 value of 0.85 mg/ml. By activity-guided fractionation, we determined that the fraction containing ginsenosides displayed an inhibitory effect on SGLT1. Of the ginsenosides evaluated, protopanaxatriol-type ginsenosides were not found to inhibit SGLT1, whereas protopanaxadiol-type ginsenosides, including ginsenosides Rd, Rg3, Rh2, F2 and compound K, exhibited significant inhibitory effects on SGLT1, with ginsenoside F2 having the highest activity with an IC50 value of 23.0 µM. Next, we measured the uptake of ginsenoside F2 and compound K into Caco-2 cells, a cell line frequently used to evaluate the intestinal absorption of drugs. The uptake of ginsenoside F2 and compound K into Caco-2 cells was not competitively inhibited by glucose. Furthermore, the uptake of ginsenoside F2 and compound K into SGLT1-overexpressing HEK293 cells was not significantly higher than into mock cells. Ginsenoside F2 and compound K did not appear to be substrates of SGLT1, although these compounds could inhibit SGLT1. Ginsenosides might be absorbed by passive diffusion through the intestinal membrane or actively transported via unknown transporters other than SGLT1.

Entities: Chemical Gene Species

Keywords: Diabetes; Ginsenosides; Glucose transporter; Panax ginseng; SGLT1

Mesh：

Substances：

Year: 2016 PMID： 27619505 DOI： 10.1007/s11418-016-1042-9

Source DB: PubMed Journal: J Nat Med ISSN： 1340-3443 Impact factor: 2.343

19 in total

1. Pharmacokinetics of daikenchuto, a traditional Japanese medicine (kampo) after single oral administration to healthy Japanese volunteers.

Authors: Masaya Munekage; Hiroyuki Kitagawa; Kengo Ichikawa; Junko Watanabe; Katsuyuki Aoki; Toru Kono; Kazuhiro Hanazaki
Journal: Drug Metab Dispos Date: 2011-07-01 Impact factor: 3.922

2. An Essential Role of cAMP Response Element Binding Protein in Ginsenoside Rg1-Mediated Inhibition of Na+/Glucose Cotransporter 1 Gene Expression.

Authors: Chun-Wen Wang; Shih-Chieh Su; Shu-Fen Huang; Yu-Chuan Huang; Fang-Na Chan; Yu-Han Kuo; Mei-Whey Hung; Hang-Chin Lin; Wen-Liang Chang; Tsu-Chung Chang
Journal: Mol Pharmacol Date: 2015-10-01 Impact factor: 4.436

3. Ninjin'yoeito and ginseng extract prevent oxaliplatin-induced neurodegeneration in PC12 cells.

Authors: Toshiaki Suzuki; Ayano Yamamoto; Masahiro Ohsawa; Yoshiharu Motoo; Hajime Mizukami; Toshiaki Makino
Journal: J Nat Med Date: 2015-05-27 Impact factor: 2.343

4. Ginsenoside Rb1 promotes browning through regulation of PPARγ in 3T3-L1 adipocytes.

Authors: Qianqian Mu; Xin Fang; Xiaoke Li; Dandan Zhao; Fangfang Mo; Guangjian Jiang; Na Yu; Yi Zhang; Yubo Guo; Min Fu; Jun-Li Liu; Dongwei Zhang; Sihua Gao
Journal: Biochem Biophys Res Commun Date: 2015-09-14 Impact factor: 3.575

5. Bioactivity and bioavailability of ginsenosides are dependent on the glycosidase activities of the A/J mouse intestinal microbiome defined by pyrosequencing.

Authors: Tao Niu; Diane L Smith; Zhen Yang; Song Gao; Taijun Yin; Zhi-Hong Jiang; Ming You; Richard A Gibbs; Joseph F Petrosino; Ming Hu
Journal: Pharm Res Date: 2012-12-20 Impact factor: 4.200

Review 3. Intestinal Saturated Long-Chain Fatty Acid, Glucose and Fructose Transporters and Their Inhibition by Natural Plant Extracts in Caco-2 Cells.

Authors: Katharina Schreck; Matthias F Melzig
Journal: Molecules Date: 2018-10-06 Impact factor: 4.411

3 in total

Ginsenosides, ingredients of the root of Panax ginseng, are not substrates but inhibitors of sodium-glucose transporter 1.

1. Pharmacokinetics of daikenchuto, a traditional Japanese medicine (kampo) after single oral administration to healthy Japanese volunteers.

2. An Essential Role of cAMP Response Element Binding Protein in Ginsenoside Rg1-Mediated Inhibition of Na+/Glucose Cotransporter 1 Gene Expression.

3. Ninjin'yoeito and ginseng extract prevent oxaliplatin-induced neurodegeneration in PC12 cells.

4. Ginsenoside Rb1 promotes browning through regulation of PPARγ in 3T3-L1 adipocytes.

5. Bioactivity and bioavailability of ginsenosides are dependent on the glycosidase activities of the A/J mouse intestinal microbiome defined by pyrosequencing.

6. Degradation of ginsenosides in humans after oral administration.

7. Active absorption of ginsenoside Rg1 in vitro and in vivo: the role of sodium-dependent glucose co-transporter 1.

8. Antiobesity effects of wild ginseng (Panax ginseng C.A. Meyer) mediated by PPAR-gamma, GLUT4 and LPL in ob/ob mice.

Review 9. Ginseng for health care: a systematic review of randomized controlled trials in Korean literature.

10. Biotransformation of ginsenoside Rb1 via the gypenoside pathway by human gut bacteria.

1. Effect of ninjin'yoeito and ginseng extracts on oxaliplatin-induced neuropathies in mice.

Review 2. Therapeutic Potential of Ginsenosides as an Adjuvant Treatment for Diabetes.

Review 3. Intestinal Saturated Long-Chain Fatty Acid, Glucose and Fructose Transporters and Their Inhibition by Natural Plant Extracts in Caco-2 Cells.