Abstract

The effects of intravenous morphine, (-)-naloxone and (+)-naloxone have been studied on three ipsilateral cutaneo-muscular reflexes in spinal rabbits. Morphine, 3 mg/kg caused a slow-onset depression of all three reflexes. This effect was naloxone reversible. The ipsilateral extensor reflexes, sural to gastrocnemius medialis and saphenous to vastus lateralis were both enhanced to more than double control size following a 5 micrograms/kg dose of naloxone given in the absence of morphine. For the sural-gastrocnemius reflex, naloxone potentiated the reflex drive from all groups of myelinated afferent fibres. The ipsilateral flexion reflex, sural to semitendinosus, was only weakly enhanced by naloxone, the 5 micrograms dose leading to an increase in the size of the reflex to 130% of control. All observed actions of naloxone were stereospecific as the enantiomer (+)-naloxone failed to affect any of the reflexes even in a dose of 50 micrograms/kg. We conclude from these findings that opioid peptides are tonically released in rabbit spinal cord, and that they have differential effects in control of flexion and extension reflexes. It is suggested that the ipsilateral extension reflexes are held under a more powerful opioid-mediated depression than that operating upon the flexion reflexes, and that this difference may be related to the greater inhibitory inflow to extensor motoneurones from ipsilateral skin areas.

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