Inhibition of Borna disease virus replication by ribavirin
The guanosine analogue ribavirin was tested for antiviral activity in two neural cell lines,
human oligodendrocytes and rat glia, against Borna disease virus (BDV) strains V and
He/80. Ribavirin treatment resulted in lower levels of virus and viral transcripts within 12 h.
Addition of guanosine but not adenosine resulted in a profound reduction of the ribavirin
effect. Ribavirin appears to be an effective antiviral agent for treatment of BDV infection in
vitro. A likely mechanism for its activity is reduction of the intracellular GTP pool, resulting in …
human oligodendrocytes and rat glia, against Borna disease virus (BDV) strains V and
He/80. Ribavirin treatment resulted in lower levels of virus and viral transcripts within 12 h.
Addition of guanosine but not adenosine resulted in a profound reduction of the ribavirin
effect. Ribavirin appears to be an effective antiviral agent for treatment of BDV infection in
vitro. A likely mechanism for its activity is reduction of the intracellular GTP pool, resulting in …
Abstract
The guanosine analogue ribavirin was tested for antiviral activity in two neural cell lines, human oligodendrocytes and rat glia, against Borna disease virus (BDV) strains V and He/80. Ribavirin treatment resulted in lower levels of virus and viral transcripts within 12 h. Addition of guanosine but not adenosine resulted in a profound reduction of the ribavirin effect. Ribavirin appears to be an effective antiviral agent for treatment of BDV infection in vitro. A likely mechanism for its activity is reduction of the intracellular GTP pool, resulting in inhibition of transcription and capping of BDV mRNAs.
American Society for Microbiology