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Vol. 296, Issue 2, 378-387, February 2001
Anesthesiology Research Unit, Institut Municipal
d'Investigació Mèdica, Department of Anesthesiology,
Hospital Universitario del Mar, Barcelona, Spain
The inhibitory effects of central and peripherally acting opioid
agonists on intestinal permeability (PER) were evaluated during acute
and chronic intestinal inflammation in mice. Inflammation was induced
by the intragastric (p.o.) administration of one (acute) or two
(chronic) doses of croton oil (CO), whereas controls received saline
(SS). Intestinal PER was assessed by the blood-to-lumen transfer of
51Cr-ethylenediaminetetraacetate
(51Cr-EDTA). CO significantly increased PER during acute
(2.5 times) and chronic (3.2 times) inflammation. The potency of s.c.
morphine-inhibiting PER was enhanced 3.8 and 8.7 times in acute and
chronic CO, whereas that of s.c. fentanyl was increased 2.0 and 4.3 times, respectively, compared with SS. Similarly, s.c.
[D-Pen2,5]-enkephalin was 4.7 and 11.1 times
more potent during acute and chronic CO, and the
Emax values of the dose-response curves
increased 35% during inflammation. The potency of s.c. U50,488H was
5.6 (acute) and 6.7 times (chronic) greater compared with SS. All effects were reversed by specific antagonists. The i.p. administration of 
-funaltrexamine differentially blocked morphine effects during acute and chronic CO, suggesting that the effects are mediated by
different populations of functional µ-opioid receptors (OR). The
increase in potencies of s.c. PL017 and ICI-204,448 during CO were
comparable to those observed with fentanyl and U50,488H and their
effects were antagonized by s.c. naloxone methiodide. Moreover, the
potency of the agonists during inflammation was unaltered when
administered i.c.v. The results show that intestinal inflammation
enhances the effects of 
- > µ- > 
-opioid agonists on PER by
activation of peripheral OR.
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