Epstein-Barr Virus (EBV) belongs to the gammaherpesvirus family, and is known to be associated with several neoplastic diseases. EBV usually remains latent after infection. Upon stimulated by environmental factors, EBV would enter into the lytic cycle and then produce infective viral particles. During the lytic cycle, capsid proteins need to be translocated into the nucleus for capsid assembly. Among them, only BORF1, BVRF2, and BdRF1 contain the nuclear localization signal (NLS), while the translocation pathways of other capsid proteins are unclear. In herpes simplex virus 1 (HSV-1), scaffold protein is responsible for the translocation of major capsid protein. However, the immunofluorescence results indicated that translocation of VCA is not dependent on BdRF1, unless BFRF3 is also present. Therefore, this study aims to clarify the involvement of BFRF3 in the translocation of VCA. This study found that BFRF3 binds to VCA. Sucrose gradient analysis subsequently revealed that BFRF3 is required for the reduction of VCA oligomerization. Deletion analysis indicates that amino acid residues 1-65 of BFRF3 is required for VCA de-oligomerization. Finally, this study confirms that VCA, BFRF3, and BdRF1 aggregate at promyelocytic leukemia nuclear bodies (PML- NBs). The study provides insight into the mechanism how capsid proteins were translocated into the nucleus for capsid assembly.