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Vol. 292, Issue 2, 743-751, February 2000
Department of Anesthesia and Critical Care, University of Chicago,
Chicago, Illinois.
In the present study, we investigated the effects of intrathecal
gabapentin on nociceptive behaviors and the numbers of spinal Fos-like
immunoreactive (Fos-LI) neurons evoked by injection of 0.25 to 2.5%
formalin in the hindpaw of the rat. Pretreatment with gabapentin dose
dependently decreased flinches and weighted pain scores in phase 2, but
not phase 1, at each concentration of formalin. The highest dose of
gabapentin (100 µg) shifted the EC50 values of formalin
for both flinches and weighted pain scores to the right by 2.5-fold,
suggesting that formalin was perceived to be significantly less
noxious. Gabapentin also decreased phase 2 behaviors when administered
after formalin but was only one third as potent. Unlike its inhibition
of formalin-evoked nociceptive behaviors, the effect of gabapentin on
the expression of Fos-like immunoreactivity in the spinal cord was
highly dependent on the concentration of formalin. Intrathecal
pretreatment with 100 µg of gabapentin did not decrease the numbers
of Fos-LI neurons evoked by 0.5% formalin, yet this dose decreased the
numbers of Fos-LI neurons in laminae I-II and VII-X of rats that
received 1.25% formalin and uniformly decreased by 50% the numbers of
Fos-LI neurons in all laminae of rats that received 2.5% formalin.
These latter findings suggest that gabapentin neither nonselectively decreases the excitability of spinal cord neurons nor uniformly inhibits the release of all neurotransmitters from primary afferent terminals. Rather, its effects may be preferential for those
neurotransmitters released by higher, more noxious concentrations of
formalin and for conditions in which there is a greater induction of
central sensitization.
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