White spot syndrome virus (WSSV) is a large DNA virus with highly infectious and high mortalities to Penaeid shrimp. Since the first outbreaks of WSSV in southeast China in early 1990s, it spreads all over the world and causes serious economic losses. However, there’s no treatment for WSSV. After infection of DNA virus, it remains la-tency and switches into lytic cycle with appropriate environmental stimulation, subse-quently expressing immediate-early genes, early genes and late genes. So far, twenty one WSSV immediate-early genes (IE genes) have been found. Among these IE genes, wssv108 contains transcriptional activity. Transient transfection experiments showed that WSSV108 activated the promoter of wssv304 about 6.5-fold in insect cells. Dele-tion analysis of the promoter suggested that nucleotides -93 to -36 in wssv304 promoter is important to the activation by WSSV108. Moreover, electrophoretic mobility shift assay verified that wssv108 binds to the nucleotide -65 to -46 in wssv304 promoter. Meanwhile, site-directed mutagenesis proved that -59 to -50 in wssv304 promoter is important to the activation by WSSV108. In addition, GST pull-down assay showed that wssv108 forms dimer and interacts with LvYY1 directly. Therefore, this study demonstrated that wssv108 enhances the transcription of wssv304, suggesting that WSSV108 acts as a transcription factor in the regulation of other viral genes.