Abstract Both Dengue viruses (DV) and Japanese encephalitis virus (JEV) are mosquito-borne flaviviruses. They share the same genomic organization and both are positive-sense, single-stranded RNAs. However, the symptoms of their infection are very different. JEV causes severe, even lethal encephalitis in humans. Pathological studies of JEV have shown that developing neurons are the major target of JEV. The DV complex consists of four serotypes (DV1-DV4). They may cause dengue fever (DF), dengue hemorrhagic fever (DHF), or dengue shock syndrome (DSS). Interestingly, most flaviviruses but DV cause neurotropism. Possibilities are that DV has difficulty to enter or propagate in neurons. Hence, I employed imaging technique to determine if DV2 and JEV can infect neurons by investigating the accumulation kinetics of viral replication in mouse primary neurons and mosquito cells. Since dengue symptoms are limited to human, I also analyzed the viral infectivity of DV2 and JEV in human neuroblastoma IMR-32. The results showed that both human and mouse neurons could be infected not only by JEV but also by DV2. And, the accumulation kinetics for DV and JEV were similar in the mouse primary neurons and mosquito cells. Hence, DV rarely causing neurotropism is not due to inability of infectivity and/or replication in neuron cells.