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Effects of Analgesics on Delayed Postherpetic Pain in Mice

疱疹后神经痛 医学 双氯芬酸 加巴喷丁 吗啡 麻醉 神经痛 单纯疱疹病毒 止痛药 美西律 木瓦 病毒 药理学 神经病理性疼痛 病理 免疫学 替代医学
作者
Ichiro Takasaki,Atsushi Sasaki,Tsugunobu Andoh,Hiroshi Nojima,Kimíyasu Shiraki,Yasushi Kuraishi
出处
期刊:Anesthesiology [Lippincott Williams & Wilkins]
卷期号:96 (5): 1168-1174 被引量:43
标识
DOI:10.1097/00000542-200205000-00021
摘要

Background Postherpetic neuralgia is pain that persists long after the disappearance of the cutaneous lesions of herpes zoster. However, the mechanisms of this delayed pain are unclear. Herpes simplex virus infection induces cutaneous lesions and pain-related responses in mice. The authors examined whether such responses would persist after the disappearance of the cutaneous lesions and whether some analgesics would be effective against them. Methods Female BALB/c mice were inoculated with herpes simplex virus type 1 on the unilateral hind paw. Pain-related responses of hind paw were determined using von Frey filaments. Beginning 5 days after inoculation, mice were given perorally the antiherpes agent acyclovir five times a day for 7 days. Effects of morphine (3-5 mg/kg subcutaneously), gabapentin (30-100 mg/kg perorally), mexiletine (10-30 mg/kg intraperitoneally), and diclofenac (30 mg/kg intraperitoneally) on pain-related responses were examined on days 25-35 after inoculation. Results Viral inoculation induced cutaneous lesions and pain-related responses beginning on day 5 after inoculation. Acyclovir treatment healed all skin lesions by day 15 after inoculation. Approximately half of the mice given acyclovir showed pain-related responses at least until day 40 after inoculation. Morphine, gabapentin, and mexiletine dose-dependently inhibited pain-related responses, but diclofenac had no effects. Conclusions The authors show a mouse model of delayed postherpetic pain. This may be useful for manifesting the mechanisms of postherpetic neuralgia and the factors contributing to the transition from acute herpetic pain to delayed postherpetic pain. This may also be useful for the development of new analgesics against postherpetic neuralgia.

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