ABSTRACT: Type I interferon (IFN-?/?) plays a critical role in suppressing viral replication by driving the transcription of hundreds of interferon-sensitive genes (ISGs). While many ISGs are transcriptionally activated by the ISGF3 complex, the significance of other signaling intermediates in IFN-?/?-mediated gene regulation remains elusive, particularly in rare cases of gene silencing. In human Th2 cells, IFN-?/? signaling suppressed IL5 and IL13 mRNA expression during recall responses to T-cell receptor (TCR) activation. This suppression occurred through a rapid reduction in the rate of nascent transcription, independent of de novo expression of ISGs. Further, IFN-?/?-mediated STAT4 activation was required for repressing the human IL5 gene, and disrupting STAT4 dimerization reversed this effect. This is the first demonstration of STAT4 acting as a transcriptional repressor in response to IFN-?/? signaling and highlights the unique activity of this cytokine to acutely block the expression of an inflammatory cytokine in human T cells.