The involvement of the opioidergic system in the antinociceptive mechanism
of action of antidepressant compounds
by
Gray AM, Spencer PS, Sewell RD
Division of Pharmacology,
The Welsh School of Pharmacy, UWC, Cardiff, Wales.
Br J Pharmacol 1998 Jun; 124(4):669-74
ABSTRACT
1. Debate exists as to the nature of antidepressant-induced antinociception.
It is unclear whether antidepressants are inherently antinociceptive, are able
to potentiate opioid antinociception or both. We have used the acetic acid
induced abdominal constriction assay in mice to investigate
antidepressant-induced antinociception. 2. All the antidepressants tested (s.c.)
produced dose-dependent protection against acetic acid-induced abdominal
constriction. Similarly, morphine and aspirin were also effective
antinociceptive agents in this nociceptive assay. 3. Opioid antagonists,
naloxone (0.5 mg kg(-1), s.c.) and naltrindole (1 mg kg(-1), s.c.), shifted the
dose-response relationships to the right for each of the antidepressant agents
(dothiepin, amitriptyline, sibutramine, (+)-oxaprotiline and paroxetine). In
this context the naloxone dose-ratios were 1.95, 3.90, 2.32, 4.50 and 2.65, with
naltrindole dose-ratios of 4.36, 17.00, 4.28, 11.48 and 2.65 were obtained,
respectively. Naloxone also shifted the morphine dose-response relationship to
the right, by a factor of 2.62, whilst naltrindole had no effect upon morphine
antinociception. Aspirin antinociception remained unaffected by both opioid
antagonists. 4. The enkephalin catabolism inhibitor acetorphan, by itself,
produced no activity in this test at a dose of 10 mg kg(-1) (s.c.). However, at
higher doses, acetorphan produced a linear dose-response relationship against
acetic acid-induced abdominal constriction. 5. When acetorphan was administered
before either the antidepressants or morphine, there was a clear potentiation of
the antidepressant- or morphine-induced antinociception. However, acetorphan had
no effect on aspirin antinociception. 6. Since neither of the opioid antagonists
were able to attenuate, nor was acetorphan able to potentiate, aspirin
antinociception, we concluded that the mechanism of antidepressant-induced
antinociception is different from that of the non-steroidal anti-inflammatory
drugs. 7. These data are consistent with the view that antidepressants may
induce endogenous opioid peptide release, as shown by the acetorphan study. In
this context, the ability of naltrindole to displace the antidepressant
dose-response relationship to the right without affecting morphine
antinociception, implicates the delta-opioid receptor and endogenous opioid
peptides in antidepressant-induced antinociception.
Prozac and the opioid pathways
Is morphine an antidepressant?
Depression, opioids and the HPA
Buprenorphine as an antidepressant
Morphine for endogenous depressives
The opioid connection: venlafaxine and mirtazapine

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