The present study was conducted to

The present study was conducted to determine the 96 h-LC50 of benomyl to the Nile tilapia, Oreochromis
niloticus and to investigate the biochemical or hematological indices of blood and the alterations in the
antioxidant enzymes of this fish in response to sublethal concentrations of benomyl. Fish weighing
71.61 ± 12.05 g were used in this study; they were subjected to fasting for 4 weeks before treatment.
An aqueous solution of benomyl (0, 0.5, 1, 2, 4, 8, and 16 mg L1
) was administered for 96 h to determine
the LC50. The 96 h-LC50 value of benomyl was 4.39 (3.23–5.60) mg L1
in the present study. For 5 weeks,
the aqueous solution of benomyl (0, 100, 200, and 400 lg L1
) was administered to investigate its effect
on the hematological parameters and antioxidant enzymes. The predominant hematological findings in
fish exposed to benomyl were as follows: no significant change in the Hb (g dL1
) level, MCV (lm3
),
MCH (pg) and MCHC (%) as compared to the control. Benomyl exposure led to greater increases in the
GPT, GOT (Karmen-unit), LDH (Wroblewski unit), total cholesterol, Fe, and Ca (mg dL1
) values, whereas
the levels of ALP (KA unit), total protein, triglyceride, albumin, and Mg (mg dL1
) did not increase. Benomyl increased the in vivo HSI (%), GST (nmol min1
mg protein1
), and SOD (U mg protein1
) values in
the fish livers in the test group, unlike those in the control group for 5 weeks. At concentrations higher
than 100 lg L1
, benomyl affected the GST and SOD levels of Nile tilapia in a dose- and time-dependent
manner. The present findings suggest that the in vivo hepatotoxicity associated with benomyl may, in
part, result from the hematological index, and antioxidants may provide limited protection against benomyl toxicity.