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DOI: 10.1055/s-2006-947198
© Georg Thieme Verlag KG Stuttgart · New York
Antiviral Effect of Artemisinin from Artemisia annua against a Model Member of the Flaviviridae Family, the Bovine Viral Diarrhoea Virus (BVDV)
Publication History
Received: April 29, 2006
Accepted: June 20, 2006
Publication Date:
10 August 2006 (online)
Abstract
The antiviral activity versus flaviviruses of artemisinin, a safe drug obtained from Artemisia annua and commonly used to treat malaria, has been investigated using as an in vitro model bovine epithelial cells from embryonic trachea (EBTr) infected with the cytopathic strain Oregon C24V, of bovine viral diarrhoea virus (BVDV), which is a member of the Flaviviridae family. Antiviral activity was estimated by the degree of protection against the cytopathic effect of BVDV on host cells and by the reduction in BVDV-RNA release to the culture medium. To induce an intermediate cytopathic effect in non-treated cells, EBTr cells were first exposed to BVDV for 48 h and then incubated with virus-free medium for 72 h. Ribavirin and artemisinin (up to 100 µM) induced no toxicity in host cells, whereas a slight degree of toxicity was observed for IFN-α at concentrations above 10 U/mL up to 100 U/mL. Treatment of infected cells with IFN-α, ribavirin and artemisinin markedly reduced BVDV-induced cell death. A combination of these drugs resulted in an additive protective effect. These drugs induced a significant reduction in the production/release of BVDV virions by infected EBTr cells; there was also an additive effect when combinations of them were assayed. These results suggest a potential usefulness of artemisinin in combination with current pharmacological therapy for the treatment of human and veterinary infections by flaviviruses.
Abbreviations
BVDV:Bovine Viral Diarrhoea Virus
HCV:Hepatitis C Virus
IFN:Interferon
Key words
EBTr - Hepacivirus - Hepatitis - Interferon - Liver - Malaria - Ribavirin
References
- 1 Buckwold V E, Beer B E, Donis R O. Bovine viral diarrhea virus as a surrogate model of hepatitis C virus for the evaluation of antiviral agents. Antiviral Res. 2003; 60 1-15
- 2 Zeisel M B, Baumert T F. Production of infectious hepatitis C virus in tissue culture: A breakthrough for basic and applied research. J Hepatol. 2006; 44 436-9
- 3 Behrens S E, Grassmann C W, Thiel H J, Meyers G, Tautz N. Characterization of an autonomous subgenomic pestivirus RNA replicon. J Virol. 1998; 72 2364-72
- 4 Greiser-Wilke I, Haas L, Dittmar K, Liess B, Moennig V. RNA insertions and gene duplications in the nonstructural protein p125 region of pestivirus strains and isolates in vitro and in vivo . Virology. 1993; 193 977-80
- 5 Meyers G, Tautz N, Stark R, Brownlie J, Dubovi E J, Collett M S. et al . Rearrangement of viral sequences in cytopathogenic pestiviruses. Virology. 1992; 191 368-86
- 6 Qi F, Ridpath J F, Lewis T, Bolin S R, Berry E S. Analysis of the bovine viral diarrhea virus genome for possible cellular insertions. Virology. 1992; 189 285-92
- 7 Meshnick S R. Artemisinin: mechanism of action, resistance and toxicity. Int J Parasitol. 2002; 32 1655-60
- 8 Yamey G. Treating Plasmodium falciparum malaria with artemisinin derivatives. PLoS Med. 2005; 2 e414
- 9 Romero M R, Efferth T, Serrano M A, Castano B, Macias R IR, Briz O. et al . Effect of artemisinin/artesunate as inhibitors of hepatitis B virus production in an ”in vitro” replicative system. Antiviral Res. 2005; 68 75-83
- 10 Efferth T, Marschall M, Wang X, Huong S M, Hauber I, Olbrich A. et al . Antiviral activity of artesunate towards wild-type, recombinant, and gancyclovir-resistant human cytomegaloviruses. J Mol Med. 2002; 80 233-42
- 11 Kaptein S J, Efferth T, Leis M, Rechter S, Auerochs S, Kalmer M. et al . The anti-malaria drug artesunate inhibits replication of cytomegalovirus in vitro and in vivo . Antiviral Res. 2006; 69 60-9
- 12 Ouzounov S, Mehta A, Dwek R A, Block T M, Jordan R. The combination of interferon alpha-2b and n-butyl deoxynojirimycin has a greater than additive antiviral effect upon production of infectious bovine viral diarrhea virus (BVDV) in vitro: implications for hepatitis C virus (HCV) therapy. Antiviral Res. 2002; 55 425-35
- 13 Lau J Y, Tam R C, Liang T J, Hong Z. Mechanism of action of ribavirin in the combination treatment of chronic HCV infection. Hepatology. 2002; 35 1002-9
- 14 Durantel D, Carrouee-Durantel S, Branza-Nichita N, Dwek R A, Zitzmann N. Effects of interferon, ribavirin, and iminosugar derivatives on cells persistently infected with noncytopathic bovine viral diarrhea virus. Antimicrob Agents Chemother. 2004; 48 497-504
- 15 Yang Y Z, Little B, Meshnick S R. Alkylation of proteins by artemisinin. Effects of heme, pH and drug structure. Biochem Pharmacol. 1994; 48 569-73
- 16 Zhang F, Gosser D K, Meshnick S R. Hemin-catalyzed decomposition of artemisinin. Biochem Pharmacol. 1992; 43 1805-9
- 17 Liang T J, Rehermann B, Seeff L B, Hoofnagle J H. Pathogenesis, natural history, treatment, and prevention of hepatitis C. Ann Intern Med. 2000; 132 296-305
- 18 Tanikawa K. Pathogenesis and treatment of hepatitis C virus-related liver diseases. Hepatobiliary Pancreat Dis Int. 2004; 3 17-20
- 19 McHutchison J G, Gordon S C, Schiff E R, Shiffman M L, Lee W M, Rustgi V K. et al . Interferon alfa-2b alone or in combination with ribavirin as initial treatment for chronic hepatitis C. Hepatitis Interventional Therapy Group. N Engl J Med. 1998; 339 1485-92
- 20 Coon J T, Ernst E. Complementary and alternative therapies in the treatment of chronic hepatitis C: A systematic review. J Hepatol. 2004; 40 491-500
- 21 Briz O, Serrano M A, Rebollo N, Hagenbuch B, Meier P J, Koepsell H. et al . Carriers involved in targeting the cytostatic bile acid-cisplatin derivatives cis-diammine-chloro-cholylglycinate-platinum(II) and cis-diammine-bisursodeoxycholate-platinum(II) toward liver cells. Mol Pharmacol. 2002; 61 853-60
- 22 Bland M. An introduction to medical statistics. 3rd edition London; Oxford University Press 2000
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- 23 Yanagida K, Baba C, Baba M. Inhibition of bovine viral diarrhea virus (BVDV) by mizoribine: synergistic effect of combination with interferon-alpha. Antiviral Res. 2004; 64 195-201
- 24 Price R, van Vugt M, Phaipun L, Luxemburger C, Simpson J, McGready R. et al . Adverse effects in patients with acute falciparum malaria treated with artemisinin derivatives. Am J Trop Med Hyg. 1999; 60 547-55
- 25 McGready R, Cho T, Cho J J, Simpsom J A, Luxemburger C, Dubowitz L. et al . Artemisinin derivatives in the treatment of falciparum malaria in pregnancy. Trans R Soc Trop Med Hyg. 1998; 92 430-3
- 26 Nosten F, Price R N. New antimalarials. A risk-benefit analysis. Drug Saf. 1995; 12 264-73
- 27 Dayan A D. Neurotoxicity and artemisinin compounds: do the observations in animals justify limitation of clinical use?. Med Trop. 1998; 58 32-7
- 28 Samuel C E. Antiviral actions of interferons. Clin Microbiol Rev. 2001; 14 778-809
- 29 Tam R C, Lau J Y, Hong Z. Mechanisms of action of ribavirin in antiviral therapies. Antivir Chem Chemother. 2001; 12 261-72
Jose J. G. Marin
Department of Physiology and Pharmacology
University of Salamanca
Campus Miguel de Unamuno, E.D. S09
37007 Salamanca
Spain
Phone: +34-923-294-674
Fax: +34-923-294-669
Email: jjgmarin@usal.es