Long-lasting hyperalgesia induced by fentanyl in rats: preventive effect of
ketamine
by
Celerier E, Rivat C, Jun Y, Laulin JP, Larcher A, Reynier P, Simonnet G
Institut National de la Sante et de la Recherche Medicale (INSERM) U 259,
Bordeaux, France.
Anesthesiology 2000 Feb; 92(2):465-72
ABSTRACT
BACKGROUND: It has been reported that mu-opioid receptor activation leads to
a sustained increase in glutamate synaptic effectiveness at the
N-methyl-D-aspartate (NMDA) receptor level, a system associated with central
hypersensitivity to pain. One hypothesis is that postoperative pain may result
partly from the activation of NMDA pain facilitatory processes induced by opiate
treatment per se. The authors tested here the effectiveness of the opiate
analgesic fentanyl for eliciting a delayed enhancement in pain sensitivity.
METHODS: The consequences of four bolus injections (every 15 min) of fentanyl
(20-100 microg/kg per injection, subcutaneously) on immediate (for several
hours) and long-term (for several days) sensitivity to nociceptive stimuli in
the rat (paw-pressure vocalization test) were evaluated. The effects of the
combination of the NMDA-receptor antagonist ketamine (10 mg/kg, subcutaneously)
with fentanyl also were assessed. RESULTS: Fentanyl administration exhibited a
biphasic time-dependent effect: first, an early response (for 2-5 h) associated
with a marked increase in nociceptive threshold (analgesia), and second, a later
response associated with sustained lowering of the nociceptive threshold (5 days
for the longest effect) below the basal value (30% of decrease for the maximal
effect) indicative of hyperalgesia. The higher the fentanyl dose used, the more
pronounced was the fentanyl-induced hyperalgesia. Ketamine pretreatment, which
had no analgesic effect on its own, enhanced the earlier response (analgesia)
and prevented the development of long-lasting hyperalgesia. CONCLUSIONS:
Fentanyl activates NMDA pain facilitatory processes, which oppose analgesia and
lead to long-lasting enhancement in pain sensitivity.
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