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The effect of intrathecal mu, delta, kappa, and alpha-2 agonists on thermal hyperalgesia induced by mild burn on hind paw in rats

Authors
Kim, Hyun JungSeol, Tae KyungLee, Hee JongYaksh, Tony L.Jun, Jong Hun
Issue Date
Dec-2011
Publisher
SPRINGER JAPAN KK
Keywords
Mu agonist; Delta agonist; Kappa agonist; Alpha-2 agonist; Thermal hyperalgesia; Intrathecal injection
Citation
JOURNAL OF ANESTHESIA, v.25, no.6, pp.884 - 891
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF ANESTHESIA
Volume
25
Number
6
Start Page
884
End Page
891
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/166967
DOI
10.1007/s00540-011-1240-2
ISSN
0913-8668
Abstract
Mild cutaneous thermal injury, leading to a first-degree burn, induces a sensation of burning pain and enhances the pain sensitivity of the skin. Opioid and alpha(2) receptor agonists are commonly used to reduce such hyperalgesia. We investigated conditions that induced adequate thermal hyperalgesia in rats and compared the effects of mu, delta, kappa, and alpha(2) receptors at the level of the spinal cord in this model. A total of 149 male Sprague-Dawley rats were submitted to this study. A first-degree burn injury was induced in the hind paw by contact with a hot plate. The nociceptive threshold was determined by measuring the time from the application of a light beam to the hind paw to the withdrawal response (paw withdrawal latency, PWL). Various hot-plate exposure times and light beam intensities were tested to determine the conditions that induced adequate hyperalgesia. We also tested the effects of intrathecal morphine (mu agonist), DPDPE ([D-Pen2, D-Pen5] enkephalin, a delta agonist), U50488H (trans(+)-3,4-dichloro-N-methyl-N-[2-(1-pyrrolidinyl) cyclohexyl]-benzacetamide methane sulfonate salt, a kappa agonist), and ST-91 (2-[2,6-diethyl-phenylamino]-2-imidazoline, an alpha(2) agonist) on PWL. A first-degree burn was induced by contact with the hot plate for 45 s. Using current of 5.0 A, PWL was reduced by 40% from baseline. Intrathecally administered morphine, DPDPE, and ST-91, but not U50488H, showed dose-dependent antinociceptive effects in both injured and normal paws. Based on these findings, we could find adequate conditions for thermal hyperalgesia model. In this experimental model, mu, delta, and alpha(2) receptor agonists produced antinociceptive effects at the level of the spinal cord, but the kappa receptor agonist did not.
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COLLEGE OF MEDICINE (DEPARTMENT OF ANESTHESIA AND MEDICINE)
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