Effects of narcotics, including morphine, on visual evoked potential in rats.

The side effects of narcotics, including morphine, on the visual system are still unclear; therefore, the present study was undertaken to examine the effects of narcotics on the visual system at each antinociceptive dose by using the evoked potential (VEP) in rats. Morphine (2 or 5 mg/kg) caused a significant increase in the amplitude of early and late VEP components (P(1)-N(1), N(1)-P(2), P(3)-N(3) and N(3)-P(4)). Fentanyl (0.02 mg/kg) also showed a significant increase in the amplitude of late VEP components (P(3)-N(3), N(3)-P(4)). The effects of morphine and fentanyl on VEP components were antagonized by naloxone (1 mg/kg). On the other hand, (+/-)-pentazocine (20 mg/kg) reduced the amplitude of the late VEP component (N(3)-P(4)), and this effect was not antagonized by naloxone. Butorphanol showed no significant changes in early and late VEP components. In conclusion, morphine stimulated the retino-geniculate-cortex pathway and the thalamus-cortical circuit through the opioid receptors, and fentanyl stimulated the thalamus-cortical circuit through the opioid receptors. It can therefore be assumed that VEP is a useful tool for examining the side effects of drugs, including narcotics, on the visual system.