Epstein-Barr virus (EBV) is a human herpesvirus that contains two distinct life cycles, latency and lytic cycle. During the lytic cycle, EBV encodes a series of proteins that are necessary for viral lytic DNA replication, capsid assembly and viral maturation to produce infectious viral particles. The production and assembly of capsid proteins are important to the maturation of EBV virion, but the mechanism is unclear. The capsids of herpesviruses have a common icosahedral structure. In EBV, the capsid contains a major capsid protein, VCA and two minor capsid proteins, BORF1 and BDLF1. Tripartite-motif 5 alpha (TRIM5α) that possesses the ubiquitin E3 ligase activity is a restriction factor of retroviruses. Previous study showed that TRIM5α binds the retroviral capsids and disrupts viral structure to accelerate uncoating of capsids, which influences the replication of retroviruses. This study demonstrates that TRIM5α binds to EBV capsid proteins, BORF1 and VCA, through the C-terminal B30.2 domain. Moreover, TRIM5α promotes the ubiquitination of BORF1 in vitro and in vivo and the SUMO-interaction motifs in TRIM5α are important to the ubiquitination of BORF1. Furthermore, over-expressing of TRIM5α reduces the amount of BORF1, while knocking down of TRIM5α enhances the level of BORF1. Finally, inhibition the expression of TRIM5α enhances EBV lytic progression and promotes virion production. Taken together, this study demonstrates that TRIM5α targets to EBV capsid proteins to inhibit the lytic progression.