Sage Journals: Discover world-class research

Abstract

The effects of mismatched double-stranded RNA (m-dsRNA) and 1 -(2′-deoxy-2′-fluoro-β-D-arabinofuranosyl)-5-methyl-uracil (D-FMAU) on the replication of duck hepatitis B virus (DHBV) were examined in duck primary hepatocytes infected with DHBV. The 50% inhibitory doses of m-dsRNA and D-FMAU for the replication of DHBV DNA were 0.34±0.06 and 0.007±0.001 μg mL-1, respectively. Mismatched dsRNA slightly inhibited the intermediate DHBV DNA at a concentration as high as 1.0 μg mL-1, whereas the DHBV replicative form was markedly suppressed in the presence of 0.1 μg mL-1 of D-FMAU. On the other hand, m-dsRNA inhibited DHBV DNA replication even after the compound was removed from the culture medium, while the efficacy of D-FMAU did not persist after the cessation of treatment. The analysis of DHBV RNA revealed that m-dsRNA markedly inhibited DHBV RNA transcription, while D-FMAU only marginally suppressed the transcription of viral RNA. These results indicate that m-dsRNA inhibits DHBV RNA transcription rather than DHBV DNA replication and that this suppression of DHBV RNA transcription may produce persistent inhibition of DHBV replication.

Keywords

DHBV hepadnavirus antiviral effect-mismatched double-stranded RNA FMAU duck primary hepatocytes

References

Abbruzzese

J.L.

, Schmidt

, Raber

M.N.

, Levy

J.K.

, Castellanos

A.M.

, Legha

S.S.

, & Krakoff

I.H.

(1989) Phase I trial of l-(2′-deoxy-2′-fluoro-1-beta-D-arabinofuranosyl)-5-methyluracil (FMAU) terminated by severe neurologic toxicity. Investigational New Drugs 7: 195-201.

Chomczynski

, & Sacchi

(1987) Single-step method of RNA isolation by acid guanidinium thiocyanate-phenol-chloroform extraction. Analytical Biochemistry 162: 156-159.

Chu

C.K.

, Ma

, Shanmuganathan

, Wang

, Xiang

, Pai

S.B.

, Yao

G-Q

, Sommadossi

J-P

, & Cheng

Y-C

(1995) Use of 2′-fluoro-5-methyl-β-L-arabinofuranosyluracil as a novel antiviral agent for hepatitis B virus and Epstein–Barr virus. Antimicrobial Agents and Chemotherapy 39: 979-981.

Fourel

, Hantz

, Watanabe

K.A.

, Jacquet

, Chomel

, Fox

J.J.

, & Trepo

(1995) Inhibitory effects of 2′-fluorinated arabinosyl-pyrimidine nucleosides on woodchuck hepatitis virus replication in chronically infected woodchucks. Antimicrobial Agents and Chemotherapy 34: 473-475.

Fourel

, Li

, Hantz

, Jacquet

, Fox

J.J.

, & Trepo

(1992) Effects of 2′-fluorinated arabinosyl-pyrimidine nucleosides on duck hepatitis B virus DNA level in serum and liver of chronically infected ducks. Journal of Medical Virology 37: 122-126.

Hayashi

, & Koike

(1989) Interferon inhibits hepatitis B virus replication in a stable expression system of transfected viral DNA. Journal of Virology 63: 2936-2940.

Ijichi

, Mitamura

, Ida

, Machida

, & Shimada

(1994) In vivo antiviral effects of mismatched double-stranded RNA on duck hepatitis B virus. Journal of Medical Virology 43: 161-165.

Niu

, Wang

, Dixon

, Bowden

, Qiao

, Einck

, & Locarnini

(1993) The use of ampligen alone and in combination with ganciclovir and coumermycin A1 for the treatment of ducks congenitally-infected with duck hepatitis B virus. Antiviral Research 21: 155-171.

Sells

M.A.

, Chen

M-L

, & Acs

(1987) Production of hepatitis B virus particles in HepG2 cells transfected with cloned hepatitis B virus DNA. Proceedings of the National Academy of Sciences, USA 84: 1005-1009.

10.

Summers

(1981) Three recently described animal virus models for human hepatitis B virus. Hepatology 1: 179-183.

11.

Tiollais

, Pourcel

, & Dejean

(1985) The hepatitis B virus Nature 317: 489-495.

12.

Tsurimoto

, Fujiwara

, & Matsubara

(1987) Stable expression and replication of hepatitis B virus genome in an integrated state in a human hepatoma cell line transfected with the cloned viral DNA. Proceedings of the National Academy of Sciences, USA 84: 444-448.

13.

Tur-Kaspa

, Teicher

, Laub

, Itin

, Dagan

, Bloom

B.R.

, & Shafritz

D.A.

(1995) Alpha interferon suppresses hepatitis B virus enhancer activity and reduces viral gene transcription. Journal of Virology 64: 1821-1824.

14.

Tuttleman

J.S.

, Pugh

J.C.

, & Summers

J.W.

(1986) In vitro experimental infection of primary duck hepatocyte cultures with duck hepatitis B vims. Journal of Virology 58: 17-25.

15.

Uchida

, Suzuki

, Etsumi

, Arii

, & Shikata

(1987) Occurrence and ultrastructural localization of duck hepatitis B virus in the liver of ducks after experimental infection. Hepatology 7: 29-36.

16.

Uchida

, Suzuki

, Okuda

, & Shikata

(1988) In vitro transmission of duck hepatitis B virus to primary duck hepatocyte cultures. Hepatology 8: 760-765.

17.

Watanabe

K.A.

, Reichman

, Hirota

, Lopez

, & Fox

J.J.

(1979) Synthesis and antiherpes virus activity of some 2′-fluoro-2′-deoxyarabinofuranosyl-pyrimidine nucleosides. Journal of Medicinal Chemistry 21: 21-24.

18.

T-T

, Coates

, Aldrich

, Summers

, & Mason

W.S.

(1995) In hepatocytes infected with duck hepatitis B virus, the template for viral RNA synthesis is amplified by an intracellular pathway. Virology 175: 255-261.

19.

Zuckerman

A.J.

(1987) Screening of antiviral drugs for hepadnavirus infection in peking ducks: a review. Journal Virology Methods 17: 119-126.

Comparison of Antiviral Effects of Mismatched Double-Stranded RNA and 1 -(2′-Deoxy-2′,-Fluoro-β-D-Arabinofuranosyl)-5-Methyluracil (D-FMAU) against Duck Hepatitis B virus in Vitro

Abstract

Keywords

References