KMID : 0811720060100050255
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Korean Journal of Physiology & Pharmacology 2006 Volume.10 No. 5 p.255 ~ p.262
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Calcium Ions are Involved in Modulation of Melittin-induced Nociception in Rat: I. Effect of Voltage-gated Calcium Channel Antagonist
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Shin Hong-Kee
Lee Kyung-Hee
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Abstract
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Melittin-induced nociceptive responses are mediated by selective activation of capsaicin-sensitive primary afferent fibers and are modulated by excitatory amino acid receptor, cyclooxygenase, protein kinase C and serotonin receptor. The present study was undertaken to investigate the peripheral and spinal actions of voltage-gated calcium channel antagonists on melittin-induced nociceptive responses. Changes in mechanical threshold and number of flinchings were measured after intraplantar (i.pl.) injection of melittin (30¥ìg/paw) into mid-plantar area of hindpaw. L-type calcium channel antagonists, verapamil [intrathecal (i.t.), 6 or 12¥ìg; i.pl.,100 & 200¥ìg; i.p., 10 or 30 mg], N-type calcium channel blocker, ¥ø-conotoxin GVIA (i.t., 0.1 or 0.5¥ìg; i.pl., 5¥ìg) and P-type calcium channel antagonist, ¥ø- agatoxin IVA (i.t., 0.5¥ìg; i.pl., 5¥ìg) were administered 20 min before or 60 min after i.pl. injection of melittin. Intraplantar pre-treatment and i.t. pre- or post-treatment of verapamil and ¥ø-conotoxin GVIA dose-dependently attenuated the reduction of mechanical threshold, and melittin-induced flinchings were inhibited by i.pl. or i.t. pre-treatment of both antagonists. P-type calcium channel blocker, ¥ø- agatoxin IVA, had significant inhibitory action on flinching behaviors, but had a limited effect on melittin-induced decrease in mechanical threshold. These experimental findings suggest that verapamil and ¥ø-conotoxin GVIA can inhibit the development and maintenance of melittin-induced nociceptive responses.
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KEYWORD
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Melittin, Hyperalgesia, Spontaneous pain, Voltage-gated calcium channel antagonist
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