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Vol. 288, Issue 2, 635-642, February 1999
Department of Pharmacology, Georgetown University Medical Center,
Washington, DC
Acute administration of morphine alters various neuroendocrine and
immune parameters via opioid receptors located within the central
nervous system. Similar effects have been reported after systemic
nicotine treatment. To examine the possible relationship between opioid
and nicotinic receptor activation on the immune system, we compared the
effects of morphine with both nicotine and the highly selective
nicotinic agonist, epibatidine. Male Sprague-Dawley rats were treated
with either morphine (10 mg/kg, s.c.), nicotine (2.85 mg/kg, s.c. = 1 mg/kg freebase), or epibatidine (5 µg/kg, s.c.) and sacrificed 2 hours later. Each drug increased plasma corticosterone levels and
decreased the magnitude of the peripheral blood lymphocyte
proliferation response to the T cell mitogen concanavalin A. None of
the treatments had a significant effect on splenic or thymic lymphocyte
responses. The effects of nicotine treatment were dose-dependent.
Pretreatment with the quaternary ganglionic antagonist chlorisondamine
(0.5 mg/kg, i.p.), completely blocked the effect of epibatidine on
blood lymphocytes without altering the elevation of corticosterone
levels. Although naltrexone (10 mg/kg, s.c.) blocked all effects of
morphine, the effects of epibatidine were not blocked by the opioid
receptor antagonist. Furthermore, in contrast to morphine (), central injection of neither nicotine (30 or 240 nmol) nor
epibatidine (5, 50, or 500 ng) altered blood lymphocyte responses. These results suggest that, like morphine, nicotinic agonists decrease
blood lymphocyte proliferation responses, apparently independent of
elevated corticosterone. However, unlike morphine, nicotinic agonists
appear to act predominantly at peripheral receptors, suggesting that
nicotinic receptors are downstream of opioid receptors in a centrally
mediated opioid-induced immunomodulatory pathway.
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