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Vol. 300, Issue 1, 149-156, January 2002
Department of Anatomy and Neurosciences, University of Texas
Medical Branch, Galveston, Texas (L.Z., Y.L., K.N.W.); and Eli Lilly & Co. Ltd., Windlesham, Surrey, United Kingdom (Y.C.)
Activation of ionotropic glutamate receptors has been shown previously
to be essential for the development of secondary thermal hyperalgesia.
The present study assessed involvement of group I metabotropic
glutamate receptors (mGlu) in both the induction and maintenance phases
of secondary thermal hyperalgesia initiated by knee joint inflammation
in rats. The dose dependence of each drug in antagonism of thermal
hypersensitivity was demonstrated in pre- and post-treatment paradigms.
Knee joint inflammation was induced by injection of kaolin and
carrageenan. Four hours later the paw withdrawal latencies were
significantly shorter than baseline values. Rats were pretreated by
spinal microdialysis infusion of group I mGlu receptor antagonists,
LY393053 [(±)-2-amino-2-(3-cis and
trans-carboxycyclobutyl-3-(9-thioxanthyl)propionic acid], LY367385 [(S)-(+)-
-amino-4-carboxy-2-methylbenzeneacetic
acid], or AIDA
[(R,S)-1-aminoindan-1,5-dicarboxylic acid/UPF
523] before knee joint injection.The paw withdrawal latencies
measured 4 h after the injection were significantly longer in the
presence of group I mGlu receptor antagonists than those of the
artificial cerebrospinal fluid-treated arthritic control group.
Post-treatment with the group I mGlu receptor antagonists LY367385 and
AIDA allowed significant recovery of the paw withdrawal latencies after
the onset of the knee joint inflammation. The knee joint inflammation itself was not affected by either treatment. The results of the present
study indicate that secondary thermal hyperalgesia can be effectively
attenuated during both the development and maintenance phases of acute
knee joint inflammation by spinal application of specific group I mGlu
receptor antagonists.
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