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吗啡、[D-丙氨酸2,D-亮氨酸5]-脑啡肽和纳洛酮在大鼠杏仁核中的惊厥作用:脑电图、形态学和行为后遗症

Convulsant action of morphine, [D-Ala2, D-Leu5]-enkephalin and naloxone in the rat amygdala: electroencephalographic, morphological and behavioural sequelae.

作者信息

Ikonomidou-Turski C, Cavalheiro E A, Turski W A, Bortolotto Z A, Turski L

出版信息

Neuroscience. 1987 Feb;20(2):671-86. doi: 10.1016/0306-4522(87)90118-7.

Abstract

Morphine hydrochloride (25-200 nmol), [D-Ala2, D-Leu5]enkephalin (10-200 nmol) and naloxone hydrochloride (100-1000 nmol) were injected unilaterally into the rat amygdala and the following electrographic, behavioural and neuropathological responses were studied. Microinjections of low doses of morphine (25-50 nmol) resulted in behavioural alterations characterized by staring, gustatory automatisms and wet shakes, whereas higher doses additionally produced motor limbic seizures and status epilepticus. The first changes in the electroencephalogram appeared in the amygdala immediately after the administration of morphine and rapidly spread to hippocampal and cortical areas. Electrographic alterations consisted of high voltage fast activity, spiking, bursts of polyspiking, electrographic seizures and periods of postictal depression. Neuropathological analysis of frontal forebrain sections by means of light microscopy revealed widespread, seizure-related damage confined to amygdala, olfactory cortex, thalamus, hippocampal formation, neocortex and substantia nigra. Pretreatment of animals with naloxone, 2-20 mg/kg s.c., as well as simultaneous microinjection of the non-convulsant dose of naloxone, 100 nmol, with morphine, 100 nmol, into the amygdala failed to block the development of convulsant activity and seizure-related brain damage produced by the opiate. In contrast, diazepam, 10 mg/kg i.p., when administered prior to the microinjection of morphine into the amygdala, abolished the epileptogenic effects of the drug. [D-Ala2, D-Leu5]Enkephalin, 10-200 nmol, elicited electrographic and behavioural responses similar to those seen after low doses of morphine, when administered into the amygdala. High voltage fast activity, single spikes, bursts of polyspiking, electrographic seizures and periods of postictal depression were seen in the electroencephalogram, but no behavioural signs of motor limbic seizures could be detected. The only behavioural correlates of epileptiform electrographic activity were wet shakes, myoclonic head twiches and gustatory automatisms. The examination of frontal forebrain sections from rats receiving [D-Ala2, D-Leu5]enkephalin revealed no morphological changes. Pretreatment of rats with either naloxone, 2 mg/kg, or diazepam, 10 mg/kg, blocked the development of behavioural and electrographic sequelae of the peptide. Naloxone, 100-1000 nmol, when microinjected into the amygdala, produced electrographic, behavioural and morphological alterations resembling those seen after high doses of morphine.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

将盐酸吗啡(25 - 200纳摩尔)、[D - Ala2,D - Leu5]脑啡肽(10 - 200纳摩尔)和盐酸纳洛酮(100 - 1000纳摩尔)单侧注射到大鼠杏仁核中,并研究以下脑电图、行为和神经病理学反应。微量注射低剂量吗啡(25 - 50纳摩尔)会导致行为改变,表现为凝视、味觉自动症和湿抖,而高剂量时还会引发运动性边缘性癫痫发作和癫痫持续状态。吗啡给药后,脑电图的最初变化立即出现在杏仁核,并迅速扩散到海马和皮质区域。脑电图改变包括高电压快速活动、尖峰放电、多棘波爆发、脑电图癫痫发作和发作后抑郁期。通过光学显微镜对额叶前脑切片进行神经病理学分析,发现广泛的、与癫痫发作相关的损伤局限于杏仁核、嗅皮质、丘脑、海马结构、新皮质和黑质。用2 - 20毫克/千克皮下注射纳洛酮预处理动物,以及将100纳摩尔非惊厥剂量的纳洛酮与100纳摩尔吗啡同时微量注射到杏仁核中,均未能阻止阿片类药物引起的惊厥活性发展和与癫痫发作相关的脑损伤。相比之下,在向杏仁核微量注射吗啡之前腹腔注射10毫克/千克地西泮,可消除该药物的致癫痫作用。将10 - 200纳摩尔的[D - Ala2,D - Leu5]脑啡肽注射到杏仁核中时,会引发与低剂量吗啡注射后相似的脑电图和行为反应。脑电图中可见高电压快速活动、单个尖峰放电、多棘波爆发、脑电图癫痫发作和发作后抑郁期,但未检测到运动性边缘性癫痫发作的行为迹象。癫痫样脑电图活动的唯一行为相关表现是湿抖、肌阵挛性头部抽搐和味觉自动症。对接受[D - Ala2,D - Leu5]脑啡肽的大鼠额叶前脑切片检查未发现形态学变化。用2毫克/千克纳洛酮或10毫克/千克地西泮预处理大鼠,可阻止该肽引起的行为和脑电图后遗症的发展。当将100 - 1000纳摩尔纳洛酮微量注射到杏仁核中时,会产生与高剂量吗啡注射后相似的脑电图、行为和形态学改变。(摘要截断于400字)

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