Inhibition of retrovirus DNA supercoiling in interferon-treated cells.

AUTOR(ES)

Huleihel, M

RESUMO

The effect of interferon (IFN) on the cytoplasmic synthesis of murine sarcoma virus DNA, its transport to the host nucleus, and its integration into the cellular genome were investigated. For this purpose, at various intervals after infection. DNA was extracted from the cytoplasmic fraction, nuclear Hirt supernatant, and chromosomal DNA pellet. The relative amount of viral DNA was estimated by C0t kinetics analysis of hybridization to murine sarcoma virus-specific [3H]cDNA. IFN was found to delay viral DNA synthesis by about 2.5 h, but the amount of viral DNA eventually formed in IFN-treated cells was comparable to that of the control. The transport of this DNA to the nucleus was delayed by IFN for 6 to 18 h, but once again, all the cytoplasmic viral DNA formed in IFN-treated cells was eventually transferred to their nucleus. However, although the main part of the viral DNA formed in control cells was finally integrated into the host genome, no significant integration was observed in IFN-treated cells. Alkaline sucrose gradient analysis revealed that IFN inhibited the accumulation of supercoiled viral DNA in the nucleus. Since supercoiled viral DNA is considered a precursor to integrated provirus, this observation may suggest that IFN inhibits viral DNA integration by blocking its supercoiling.

Documentos Relacionados

• Fate of interferon-treated cells.
• Translational elongation rate changes in encephalomyocarditis virus-infected and interferon-treated cells.
• Double-stranded RNA inhibits a phosphoprotein phosphatase present in interferon-treated cells.
• Formation and characteristics of reovirus subviral particles in interferon-treated mouse L cells.
• Control of HLA-A,B,C synthesis and expression in interferon-treated cells.