Human herpes virus type 1 (HSV-1) is known to have a tightly-regulated cascade expression of its immediate early (IE), early (E), and late (L) genes. Previously, digitoxin, which was widely-used as cardiac drug, was shown to inhibit in vitro replication of HSV-1. In this study, we found that digitoxin can repress HSV-2 and acyclovir-resistant HSV-1, and several structural analogues of digitoxin such as digoxin, ouabain octahydrate and G-strophanthin also exhibited anti-HSV activity. The inhibitory effects of digitoxin are likely to be introduced at the early stage of HSV-1 replication. In HSV-infected Vero cells, the protein levels of IE gene ICP4 and ICP27 as well as the ratio of ICP4-positive cells decreased in the presence of digitoxin. The decrease of ICP4 protein level by digitoxin was most effective when digitoxin was added at 3-4 h post-infection, indicating that the inhibitory effect was less likely attributed to blocking of virus entry or post-entry events, such as uncoating and nuclear localization. Moreover, this reduction was not due to degradation of ICP4 and ICP27 protein, and the steady mRNA level suggests that the ICP4 and ICP27 protein translation was interrupted by digitoxin. At present, the involvement of HSV-encoded small RNA, miR-H6, and some eukaryotic translation initiation factors, including eIF3m, eIF4G and eIF4E in digitoxin-induced interruption of viral protein translation was excluded, and the specific interaction between digitoxin and Na+/K+-ATPase (NKA) pump was proved to be essential for such inhibition. Our results demonstrated that digitoxin is a specific inhibitor of HSV IE protein translation and could be a candidate of anti-HSV agents.