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Vol. 302, Issue 3, 1031-1036, September 2002
Department of Pharmacology and Therapeutics, Louisiana State
University Health Sciences Center, Shreveport, Louisiana
Interleukin-1 (IL-1) induces hypophagia, which can be reduced by
cyclooxygenase (COX) inhibitors. Earlier studies with COX knockout
(COXko) mice suggested that COX2 was more important for hypophagia than
COX1. However, behavioral responses occur long before COX2 is induced.
Hypophagia was assessed in mice by measuring the intake of
sweetened milk in a brief period. The intake was reduced within 30 min
after intraperitoneal injection of IL-1
and was depressed for about
2 h. When milk intake was measured 30 to 40 min after IL-1
,
COX1ko mice showed an attenuated response, whereas COX2ko mice
responded more like wild-type animals. By contrast, 90 to 120 min after
IL-1
COX1ko mice responded normally, whereas COX2ko mice showed only
small responses. The COX2-selective inhibitor, celecoxib, failed to
alter the response to IL-1
30 min after administration, but low
doses antagonized the effects of IL-1
at 90 to 120 min. The
COX1-selective inhibitor, SC560, attenuated both the early and
late responses, but a larger effect at 30 min than at 90 min suggested
a role for COX1 at the earlier time. These results suggest that shortly
after IL-1
administration, COX1 is the major enzyme involved in the
reduction of milk intake, whereas at later times COX2 is more
important, paralleling its induction. Celecoxib also attenuated the
milk intake response observed 2 h after lipopolysaccharide (LPS),
and the reductions of food pellet intake and body weight induced by
IL-1
and LPS in the subsequent 24 h, suggesting that the role
of COX2 may be more significant biologically than that of COX1.
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