Effects of centrally acting analgesics on spinal segmental reflexes and wind-up
European Journal of Pain
Abstract
Background
The
spinal cord is a prime site of action for analgesia. Here we
characterize the effects of established analgesics on segmental spinal
reflexes. The aim of the study was to look for the pattern of action or
signature of analgesic effects on these reflexes.
Methods
We used a spinal cord in vitro
preparation of neonate mice to record ventral root responses to dorsal
root stimulation. Pregabalin, clonidine, morphine and duloxetine and an
experimental sigma-1 receptor antagonist (S1RA) were applied to the
preparation in a cumulative concentration protocol. Drug effects on the
wind-up produced by repetitive stimulation of C-fibres and on responses
to single A- and C-fibre intensity stimuli were analysed.
Results
All
compounds produced a concentration-dependent inhibition of total spikes
elicited by repetitive stimulation. Concentrations producing ∼50%
reduction in this parameter were (in μM) clonidine (0.01), morphine
(0.1), pregabalin (1), duloxetine (10) and S1RA (30). At these
concentrations clonidine, pregabalin and S1RA had significant effects on
the wind-up index and little depressant effects on responses to single
stimuli. Morphine and duloxetine did not depress wind-up index and
showed large effects on responses to single stimuli. None of the
compounds had strong effects on the amplitude of the non-nociceptive
monosynaptic reflex.
Conclusions
morphine
and duloxetine had general depressant effects on spinal reflexes,
whereas the effects of clonidine, pregabalin and S1RA appeared to be
restricted to signals originated by strong repetitive activation of
C-fibres.
Results are discussed in the context of reported behavioural effects of the compounds studied.
Results are discussed in the context of reported behavioural effects of the compounds studied.
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