Metabolism and Pharmacokinetic Study of Ardipusilloside I in Rats

 

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Abstract

Ardipusilloside I, extracted from Ardisia pusilla A.DC, effectively inhibits the progression of several cancers in animal models and is a potential anti-cancer drug candidate. However, the metabolism and pharmacokinetic characteristics of ardipusilloside I remain unknown. In this study, we developed a highly sensitive liquid chromatography-tandem MS method to determine the ardipusilloside I concentration in rat plasma using ginsenoside Re (whose structure is similar to ardipusilloside I) as the internal standard. After oral administration of ardipusilloside I, its four possible metabolites (M1, M2, M3, and M4, whose structures were determined by MS) were detected in the content from rat small intestine. In rat plasma, however, only M3 and M4 were detected after oral administration of ardipusilloside I. None of the metabolites were detected in plasma samples after intravenous administration of ardipusilloside I to rats. These results indicated that the metabolites, but not the drug itself, were absorbed into plasma after oral administration of ardipusilloside I to rats and that M3 and M4 may be responsible for the antitumor activity of orally administered ardipusilloside I in rat models of cancer.

References

• 1 Tao X J, Wang P X, Yang X J, Yao H, Liu J, Cao Y X. Inhibitory effect of ardipusilloside-I on Lewis pulmonary carcinoma and hepatocarcinoma SMMC-7721.  Zhong Yao Cai. 2005;  28 574-577
  Search in Google Scholar
• 2 Tao X J, Long J W, He J Y, Yao L P, Liu J, Cao Y X. Antitumor and immunological regulation effects of ardipusilloside-I.  Chin Pharmacol Bull. 2005;  21 1070-1073
  Search in Google Scholar
• 3 Cao Y X, Zheng J P, Tao X J, Liu J, Long J W. Effect of ardipusilloside-I on immunological function in immunosuppressed mice induced by cyclophosphamide.  Chin Pharm J. 2005;  40 1553-1555
  Search in Google Scholar
• 4 Zhang Y M, Qu Y L, Zhang J, Wang X J. Ardipusilloside I purified from Ardisia pusilla competitively binds VEGFR and induces apoptosisin NCI-H460 cells.  Phytomedicine. 2010;  17 519-526
  Search in Google Scholar
• 5 Li J, Zhang L, Fei Z, Zhang X, Zhang X N, Zheng H N, Liang J W, Huo J L. Apoptosis of glioma SHG-44 cells induced by ardipusilloside and its mechanism.  Chin J Clin Neurosurg. 2009;  5 57-60
  Search in Google Scholar
• 6 Sun L W, Wang X J, Song J N, Sun W J. ELSD-HPLC determination of ardipusilloside I in Ardisia pusilla A. DC.  Chin J Pharm Anal. 2008;  28 1845-1847
  Search in Google Scholar
• 7 Kim M K, Lee T H, Suh J H, Eom H Y, Min J W, Yeom H, Kim U, Jung H J, Cha K H, Choi Y S, Youm J R, Han S B. Development and validation of a liquid chromatography-tandem mass spectrometry method for the determination of goserelin in rabbit plasma.  J Chromatogr B Analyt Technol Biomed Life Sci. 2010;  878 2235-2242
  Search in Google Scholar
• 8 Giannetti L, Longo F, Buiarelli F, Russo M V, Neri B. Tetracycline residues in royal jelly and honey by liquid chromatography tandem mass spectrometry: validation study according to Commission Decision 2002/657/EC.  Anal Bioanal Chem. 2010;  398 1017-1023
  Search in Google Scholar
• 9 Chen G T, Yang M, Guo D A. Metabolic study of ginsenoside Re in rats.  China J Chin Mater Med. 2009;  24 1540-1543
  Search in Google Scholar
• 10 Qian T, Cai Z, Wong R N, Mak N K, Jiang Z H. In vivo rat metabolism and pharmacokinetic studies of ginsenoside Rg3.  J Chromatogr B Analyt Technol Biomed Life Sci. 2005;  816 223-232
  Search in Google Scholar
• 11 Qian T, Cai Z. Biotransformation of ginsenosides Rb1, Rg3 and Rh2 in rat gastrointestinal tracts.  Chin Med. 2010;  5 19
  Search in Google Scholar
• 12 Yang L, Xu S, Liu C, Su Z. In vivo metabolism study of ginsenoside Re in rat using high-performance liquid chromatography coupled with tandem mass spectrometry.  Anal Bioanal Chem. 2009;  395 1441-1451
  Search in Google Scholar
• 13 Joo K M, Lee J H, Jeon H Y, Park C W, Hong D K, Jeong H J, Lee S J, Lee S Y, Lim K M. Pharmacokinetic study of ginsenoside Re with pure ginsenoside Re and ginseng berry extracts in mouse using ultra performance liquid chromatography/mass spectrometric method.  J Pharm Biomed Anal. 2010;  51 278-283
  Search in Google Scholar
• 14 Akao T, Hayashi T, Kobashi K, Kanaoka M, Kato H, Kobayashi M, Takeda S, Oyama T. Intestinal bacterial hydrolysis is indispensable to absorption of 18 beta-glycyrrhetic acid after oral administration of glycyrrhizin in rats.  J Pharm Pharmacol. 1994;  46 135-137
  Search in Google Scholar
• 15 Akao T, Kida H, Kanaoka M, Hattori M, Kobashi K. Intestinal bacterial hydrolysis is required for the appearance of compound K in rat plasma after oral administration of ginsenoside Rb1 from Panax ginseng.  J Pharm Pharmacol. 1998;  50 1155-1160
  Search in Google Scholar
• 16 Akao T, Kanaoka M, Kobashi K. Appearance of compound K, a major metabolite of ginsenoside Rb1 by intestinal bacteria, in rat plasma after oral administration–measurement of compound K by enzyme immunoassay.  Biol Pharm Bull. 1998;  21 245-249
  Search in Google Scholar
• 17 Bae E A, Han M J, Choo M K, Park S Y, Kim D H. Metabolism of 20(S)- and 20(R)-ginsenoside Rg3 by human intestinal bacteria and its relation to in vitro biological activities.  Biol Pharm Bull. 2002;  25 58-63
  Search in Google Scholar

Dr. Si-Yuan Zhou

Department of Pharmaceutics
School of Pharmacy
Fourth Military Medical University

17 Changle West Road

Xi'an, 710032

China

Phone: +86 29 84 77 67 83

Fax: +86 29 84 77 92 12

Email: zhousy@fmmu.edu.cn

Dr. Yi Gu

Department of Pharmacy
School of Stomatology
Fourth Military Medical University

17 Changle West Road

Xi'an, 710032

China

Phone: +86 29 84 77 67 83

Fax: +86 29 84 77 92 12

Email: guyi@fmmu.edu.cn

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