Immune and virus-induced interferons may activate cells by different derepressional mechanisms

Abstract

Virus-induced interferon (VIF), and immune interferon (IIF) produced by lymphocytes following activation by various mitogens (phytohaemagglutinin, concanavalin A, staphylococcal enterotoxin A) or by specific antigenic stimulation (tuberculin, bacterial toxoids, and viral antigens) show important functional differences. These include different antitumour¹ and immunoregulatory activities² and differential inhibition of activity by mercaptoethanol³. Another important difference has recently been shown: cells treated with IIF acquire the antiviral state much more slowly than those treated with VIF⁴. This may be due to (1) difference in cellular receptors, (2) presence of an inhibitor of antiviral activity in the IIF preparations, or (3) a different mechanism of activation of the antiviral state by the two types of interferon. The first two hypotheses seem unlikely, since (1) no difference between cell association by the two types of interferon has been detected⁴, and (2) the presence of the slow acting IIF preparation did not inhibit the rapid activation by VIF⁴. The present study shows that the different kinetics of induction of the antiviral state result from a major difference in the mechanism by which IIF and VIF activate cells.