PDF herunterladen
Planta Med 2007; 73(14): 1429-1435
DOI: 10.1055/s-2007-990256
Pharmacology
Original Paper
© Georg Thieme Verlag KG Stuttgart · New York

The Effect of Silymarin on Oral Nifedipine Pharmacokinetics

Uwe Fuhr1 , Svane Beckmann-Knopp1 , Alexander Jetter1 , 4 , Hendrik Lück2 , Ulrich Mengs3
  • 1Department of Pharmacology, University Hospital, University of Cologne, Cologne, Germany
  • 2ITECRA Institute for Tailored Early Clinical Research and Advice GmbH & Co. KG, Cologne, Germany;
  • 3Madaus GmbH, Cologne, Germany
  • 4Division of Clinical Pharmacology and Toxicology, Department of Internal Medicine, University Hospital Zurich, Zürich, Switzerland
Weitere Informationen

Publikationsverlauf

Received: May 29, 2007 Revised: September 24, 2007

Accepted: October 2, 2007

Publikationsdatum:
30. Oktober 2007 (online)

    Lizenzen und Reprints

Abstract

Silibinin, the main component of silymarin (a milk thistle extract used for treatment of liver injury), has been shown to inhibit CYP3A4 in human liver microsomes. The present study was conducted to examine whether inhibition of CYP3A4 by silymarin is also present in vivo. Immediate release nifedipine (10 mg) was administered as a CYP3A4 test drug either alone or with co-administration of silymarin (280 mg administered 10 hours and 1.5 hours prior to the administration of nifedipine) to 16 healthy male volunteers (mean age 27 years, mean body weight 77 kg). Nifedipine and silibinin concentrations were quantified by HPLC, heart rate and blood pressure were monitored for safety reasons. Pharmacokinetic parameters were calculated by non-compartmental methods, and the potential interaction by silymarin was handled as an equivalence problem. We found that nifedipine AUC was 1.13-fold higher (90 % CI, 0.97- to 1.32-fold) in the silymarin period, Cmax values were 0.70-fold (90 % CI, 0.39- to 1.27-fold) of those of the reference period, with a trend to delayed absorption in the silymarin period. Intraindividual variability especially for Cmax (intrasubject CV 120 %) was unexpectedly high. There was no meaningful effect on hemodynamic parameters. In conclusion, our data suggest that co-administration of silymarin does not considerably change the extent of absorption or metabolism of nifedipine but may decrease the absorption rate. Silymarin thus is not a potent CYP3A4 inhibitor in vivo.

Key words:

Silybum marianum (L.) Gaertn. - Asteraceae - silymarin - silibinin - milk thistle extract - nifedipine - CYP3A4 - drug-drug interaction

References

  • 1 Leng-Peschlow E, Strenge-Hesse A. Die Mariendistel (Sylibum marianum) und Silymarin als Lebertherapeutikum.  Z Phytother. 1991;  12 162-74.
    PubMedGoogle Scholar
  • 2 Flora K, Hahn M, Rosen H, Benner K. Milk thistle (Silybum marianum) for the therapy of liver disease.  Am J Gastroenterol. 1998;  93 139-43.
    CrossrefPubMedGoogle Scholar
  • 3 Gazak R, Walterova D, Kren V. Silybin and silymarin - new and emerging applications in medicine.  Curr Med Chem. 2007;  14 315-38.
    CrossrefPubMedGoogle Scholar
  • 4 Saller R, Melzer J, Reichling J, Brignoli R, Meier R. An updated systematic review of the pharmacology of silymarin.  Forsch Komplementarmed. 2007;  14 70-80.
    PubMedGoogle Scholar
  • 5 Beckmann-Knopp S, Rietbrock S, Weyhenmeyer R, Bocker R H, Beckurts K T, Lang W. et al . Inhibitory effects of silibinin on cytochrome P-450 enzymes in human liver microsomes.  Pharmacol Toxicol. 2000;  86 250-6.
    CrossrefPubMedGoogle Scholar
  • 6 Böcker R H, Guengerich F P. Oxidation of 4-aryl- and 4-alkyl-substituted 2,6-dimethyl-3,5-bis(alkoxycarbonyl)-1,4-dihydropyridines by human liver microsomes and immunochemical evidence for the involvement of a form of cytochrome P-450.  J Med Chem. 1986;  29 1596-603.
    CrossrefPubMedGoogle Scholar
  • 7 Sridar C, Goosen T C, Kent U M, Williams J A, Hollenberg P F. Silybin inactivates cytochromes P450 3A4 and 2C9 and inhibits major hepatic glucuronosyltransferases.  Drug Metab Dispos. 2004;  32 587-94.
    CrossrefPubMedGoogle Scholar
  • 8 Zuber R, Modriansky M, Dvorak Z, Rohovsky P, Ulrichova J, Simanek V. et al . Effect of silybin and its congeners on human liver microsomal cytochrome P450 activities.  Phytother Res. 2002;  16 632-8.
    CrossrefPubMedGoogle Scholar
  • 9 Weyhenmeyer R, Mascher H, Birkmayer J. Study on dose-linearity of the pharmacokinetics of silibinin diastereomers using a new stereospecific assay.  Int J Clin Pharmacol Ther Toxicol. 1992;  30 134-8.
    PubMedGoogle Scholar
  • 10 Lorenz D, Lucker P W, Mennicke W H, Wetzelsberger N. Pharmacokinetic studies with silymarin in human serum and bile.  Methods Find Exp Clin Pharmacol. 1984;  6 655-61.
    PubMedGoogle Scholar
  • 11 Schandalik R, Gatti G, Perucca E. Pharmacokinetics of silybin in bile following administration of silipide and silymarin in cholecystectomy patients.  Arzneimittelforschung. 1992;  42 964-8.
    PubMedGoogle Scholar
  • 12 Schandalik R, Perucca E. Pharmacokinetics of silybin following oral administration of silipide in patients with extrahepatic biliary obstruction.  Drugs Exp Clin Res. 1994;  20 37-42.
    PubMedGoogle Scholar
  • 13 Fuhr U. Drug interactions with grapefruit juice. Extent, probable mechanism and clinical relevance.  Drug Saf. 1998;  18 251-72.
    CrossrefPubMedGoogle Scholar
  • 14 Watkins P B. Noninvasive tests of CYP3A enzymes.  Pharmacogenetics. 1994;  4 171-84.
    CrossrefPubMedGoogle Scholar
  • 15 Fuhr U, Jetter A, Kirchheiner J. Appropriate phenotyping procedures for drug metabolizing enzymes and transporters in humans and their simultaneous use in the ”cocktail” approach.  Clin Pharmacol Ther. 2007;  81 270-83.
    CrossrefPubMedGoogle Scholar
  • 16 Shen D D, Kunze K L, Thummel K E. Enzyme-catalyzed processes of first-pass hepatic and intestinal drug extraction.  Adv Drug Deliv Rev. 1997;  27 99-127.
    CrossrefPubMedGoogle Scholar
  • 17 Galetin A, Ito K, Hallifax D, Houston J B. CYP3A4 substrate selection and substitution in the prediction of potential drug-drug interactions.  J Pharmacol Exp Ther. 2005;  314 180-90.
    CrossrefPubMedGoogle Scholar
  • 18 Bailey D G, Spence J D, Munoz C, Arnold J M. Interaction of citrus juices with felodipine and nifedipine.  Lancet. 1991;  337 268-9.
    CrossrefPubMedGoogle Scholar
  • 19 Venkatakrishnan K, von Moltke L L, Greenblatt D J. Effects of the antifungal agents on oxidative drug metabolism: clinical relevance.  Clin Pharmacokinet. 2000;  38 111-80.
    PubMedGoogle Scholar
  • 20 Odou P, Ferrari N, Barthelemy C, Brique S, Lhermitte M, Vincent A. et al . Grapefruit juice-nifedipine interaction: possible involvement of several mechanisms.  J Clin Pharm Ther. 2005;  30 153-8.
    CrossrefPubMedGoogle Scholar
  • 21 Rickling B, Hans B, Kramarczyk R, Krumbiegel G, Weyhenmeyer R. Two high-performance liquid chromatographic assays for the determination of free and total silibinin diastereomers in plasma using column switching with electrochemical detection and reversed-phase chromatography with ultraviolet detection.  J Chromatogr B Biomed Appl. 1995;  670 267-77.
    PubMedGoogle Scholar
  • 22 Steinijans V W, Hartmann M, Huber R, Radtke H W. Lack of pharmacokinetic interaction as an equivalence problem.  Int J Clin Pharmacol Ther Toxicol. 1991;  29 323-8.
    PubMedGoogle Scholar
  • 23 Diletti E, Hauschke D, Steinijans V W. Sample size determination for bioequivalence assessment by means of confidence intervals.  Int J Clin Pharmacol Ther Toxicol. 1991;  29 1-8.
    PubMedGoogle Scholar
  • 24 Gurley B J, Gardner S F, Hubbard M A, Williams D K, Gentry W B, Carrier J. et al . In vivo assessment of botanical supplementation on human cytochrome P450 phenotypes: Citrus aurantium, Echinacea purpurea, milk thistle, and saw palmetto.  Clin Pharmacol Ther. 2004;  76 428-40.
    CrossrefPubMedGoogle Scholar
  • 25 van Erp N P, Baker S D, Zhao M, Rudek M A, Guchelaar H J, Nortier J W. et al . Effect of milk thistle (Silybum marianum) on the pharmacokinetics of irinotecan.  Clin Cancer Res. 2005;  11 7800-6.
    CrossrefPubMedGoogle Scholar
  • 26 Niopas I, Daftsios A C, Xanthakis I, Nikolaidis N. Relative bioavailability study of two nifedipine tablet formulations in healthy male volunteers.  Int J Clin Pharmacol Ther. 2000;  38 309-14.
    PubMedGoogle Scholar
  • 27 Rawashdeh N M, Battah A H, Irshaid Y M, al-Qato M K. Comparative pharmacokinetics of two nifedipine products in capsule form following single oral administration in healthy volunteers.  Eur J Drug Metab Pharmacokinet. 1997;  22 259-64.
    PubMedGoogle Scholar
  • 28 Reitberg D P, Love S J, Quercia G T, Zinny M A. Effect of food on nifedipine pharmacokinetics.  Clin Pharmacol Ther. 1987;  42 72-5.
    CrossrefPubMedGoogle Scholar
  • 29 Bode H, Brendel E, Ahr G, Fuhr U, Harder S, Staib A H. Investigation of nifedipine absorption in different regions of the human gastrointestinal (GI) tract after simultaneous administration of 13C- and 12C-nifedipine.  Eur J Clin Pharmacol. 1996;  50 195-201.
    CrossrefPubMedGoogle Scholar
  • 30 Renwick A G, Ahsan C H, Challenor V F, Daniels R, Macklin B S, Waller D G. et al . The influence of posture on the pharmacokinetics of orally administered nifedipine.  Br J Clin Pharmacol. 1992;  34 332-6.
    PubMedGoogle Scholar
  • 31 Rumble R H, Roberts M S, Denton M J. Effects of posture and sleep on the pharmacokinetics of paracetamol (acetaminophen) and its metabolites.  Clin Pharmacokinet. 1991;  20 167-73.
    PubMedGoogle Scholar
  • 32 Di Carlo G, Autore G, Izzo A A, Maiolino P, Mascolo N, Viola P. et al . Inhibition of intestinal motility and secretion by flavonoids in mice and rats: structure-activity relationships.  J Pharm Pharmacol. 1993;  45 1054-9.
    CrossrefPubMedGoogle Scholar
  • 33 Mahagita C, Grassl S M, Piyachaturawat P, Ballatori N. Human organic anion transporter 1B1 (OATP1B1/OATP-C) and 1B3 (OATP1B3/OATP-8) function as bidirectional carriers and do not mediate GSH-bile acid co-transport. Am J Physiol Gastrointest Liver Physiol 2007: in press.
    Google Scholar
  • 34 Letschert K, Faulstich H, Keller D, Keppler D. Molecular characterization and inhibition of amanitin uptake into human hepatocytes.  Toxicol Sci. 2006;  91 140-9.
    CrossrefPubMedGoogle Scholar

Prof. Dr. Uwe Fuhr

Department of Pharmacology

Clinical Pharmacology

University of Cologne

Gleueler Straße 24

50931 Cologne

Germany

Telefon: +49-221-478-5230

Fax: +49-221-478-7011

eMail: uwe.fuhr@uk-koeln.de

      >