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海马mu型阿片肽受体介导大鼠癫痫发作敏感性形成
作者姓名:Liu H  Gao HM  Zhang WQ  Tang YY  Song HS
作者单位:1. 解放军210医院神经内科,大连,116021;大连理工大学神经信息研究所,大连,116024
2. 大连医科大学生理学教研室,大连,116027
3. 大连理工大学神经信息研究所,大连,116024
摘    要:为探讨海马mu型阿片肽受体介导癫痫发作敏感性形成的作用,实验采用微渗透泵技术,观察大鼠腹侧海马注射mu型阿片肽受体激动剂PL017(2.09、2.59、3.29μg/μ1)、拮抗剂β-funaltrexamine hydrochloride(β-FNA、0.88、1.10、1.35μg/μl)对红藻氨酸(kainic acid,KA)诱导癫痫发作的干预作用.PL017能够明显缩短癫痫发作潜伏期、增加癫痫发作级别(P<0.05),β-FNA则可显著延长癫痫发作潜伏期、降低发作级别(P<0.01);PL017和β-FNA的干预作用均表现出剂量依赖效应.结果表明,海马mu型阿片肽受体具有促进KA诱导的癫痫发作敏感性形成作用.

关 键 词:mu型阿片肽受体  癫痫发作敏感性  海马  癫痫  红藻氨酸  大鼠

Effects of chronic administration of PL017 and beta-funaltrexamine hydrochloride on susceptibility of kainic acid-induced seizures in rats
Liu H,Gao HM,Zhang WQ,Tang YY,Song HS.Effects of chronic administration of PL017 and beta-funaltrexamine hydrochloride on susceptibility of kainic acid-induced seizures in rats[J].Acta Physiologica Sinica,2004,56(1):101-106.
Authors:Liu Hui  Gao Hui-Ming  Zhang Wan-Qin  Tang Yi-Yuan  Song He-Shan
Institution:Department of Neurology, PLA 210 Hospital, Dalian 116021, China. liuh2002@hotmail.com
Abstract:There is evidence that 5-7 d after acute seizure episodes induced by kainic acid (KA) the rats develop a long-lasting increase in the susceptibility to seizures followed by spontaneous recurrent seizures (SRS). The present study was focused on the role of hippocampal mu opioid receptors (MORs) in the susceptibility of rats to seizures with the KA model of epilepsy. The rats received a convulsant dose of KA (10 mg/kg, i.p.) were continuously infused with a selective MOR agonist PL017 (2.09, 2.59, 3.29 microg/microl), or a selective MOR antagonist beta-funaltrexamine hydrochloride (beta-FNA, 0.88, 1.10, and 1.35 microg/microl) into ventral hippocampus by means of mini-osmotic pumps. Seven days later, the susceptibility of rats to seizures was checked by a subconvulsant dose of KA (5 mg/kg, i.p.). PL017 infusion shortened the latency and increased the stage of seizures induced by subconvulsant dose of KA in a dose-dependent manner. In contrast, infusion of beta-FNA exhibited a dose-dependent effect against seizures challenged by subconvulsant dose of KA. These results indicate that hippocampal MOR may exert a promoting effect on the susceptibility of rats to KA-induced seizures.
Keywords:mu opioid receptor  susceptibility to seizures  hippocampus  epilepsy  kainic acid  rat
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