SYNERGISM BETWEEN DISTINCT ENHANSON DOMAINS IN VIRAL INDUCTION OF THE HUMAN BETA-INTERFERON GENE

This study demonstrates distinct virus-inducible enhanson properties for three regions of the human beta interferon (IFN-β) promoter; maximum virus inducibility required syngerism among all three enhansons. Expression of the IRF-1 transcription factor differentially increased the expression of plasmids containing (AAGTGA)4 or PRDIII (-94 to -78) motifs but was inefficient in the induction of the intact IFN-β promoter. The human T-cell lymphotropic virus type I Tax protein was a strong positive activator of PRDII (-64 to -55)-containing plasmids but was also unable to stimulate the IFN-β promoter. Induction of the intact IFN-β promoter linked to a reporter plasmid was achieved in lymphoid and epithelioid cellular backgrounds by a triple transfection with IRF-1 and Tax expression plasmids or a combination of IRF-1 and phorbol ester, indicating that at least two trans-activating events and the association of two proteins on the promoter template are required for IFN-β activation.