Benzidine, a manufactured chemical that does not occur naturally, is used as manufacture dyes, especially azo dyes in the leather, textile, and paper industries. Previous studies have demonstrated that persistent exposure to benzidine increased the accidence of bladder cancer, however, the environmental toxicity of benzidine still remained to be elucidated. Here, we used zebrafish as a model to investigate the toxicity and teratogenicity of benzidine. Exposed to benzidine induced mortality in a dose- and time-dependent manner. Furthermore, treated with benzidine resulted in massive apoptosis, particularly in the brain and dorsal axis region. Malformation of the brain region and disruption of forebrain/midbrain and midbrain/hindbrain boundary was also found in benzidine-treated embryos. RT-PCR analysis revealed that Benzidine activates p53-dependent pathway and increase bax and noxa activites. In addition, benzidine attenuated Otx2 gene expression as evidenced by whole mount in situ hybridization. More strikingly, exposed to high dose of benzidine (100 μM and 200 μM) exhibited abnormal blood vasculogensis in transgenic fli1:EGFP zebrafish. Taken together, our data suggest benzidine-induced neurotoxicity and abnormal vasculogensis which resulted in markedly abnormal development and eventually caused death of zebrafish。