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吡拉西坦可预防戊四氮点燃诱导的神经元丢失和学习缺陷。

Piracetam prevents pentylenetetrazol kindling-induced neuronal loss and learning deficits.

作者信息

Pohle W, Becker A, Grecksch G, Juhre A, Willenberg A

机构信息

Department of Pharmacology and Toxicology, Faculty of Medicine, Otto-von-Guericke-University-Magdeburg, Germany.

出版信息

Seizure. 1997 Dec;6(6):467-74. doi: 10.1016/s1059-1311(97)80022-2.

Abstract

The effect of the nootropic drug piracetam (100 mg/kg) on kindled seizures, kindling-induced learning deficits, and histological alterations due to changes in central excitability was investigated in Wistar rats. The animals were kindled by repeated i.p. injections of an initially subconvulsive dose of pentylenetetrazol (PTZ). As a control, piracetam or physiological saline was given 60 minutes before PTZ. Twenty-four hours after completion of kindling the rats were tested in a shuttle-box paradigm. Seven days after the final kindling injection, the animals received a challenge dose of PTZ. Finally, the brains of the rats were processed for histological investigation. Pentylenetetrazol-kindled animals showed increasing seizure scores, and a learning deficit in the shuttle-box. Piracetam had no effect either on kindling development or on the reaction to a challenge dose of PTZ, but it protected the animals against the kindling-induced reduction of learning performance. The substance had no effect on learning performance in control animals. In distinct hippocampal structures, a neuronal cell loss was found in kindled rats. Interestingly, piracetam counteracted this damage efficaciously. The effects of piracetam are discussed in terms of its cytoprotective action. It is suggested that a coadministration of piracetam with clinically used antiepileptic drugs might be useful in antiepileptic therapy.

摘要

在Wistar大鼠中研究了促智药吡拉西坦(100毫克/千克)对点燃性癫痫发作、点燃诱导的学习缺陷以及由于中枢兴奋性变化引起的组织学改变的影响。通过反复腹腔注射初始亚惊厥剂量的戊四氮(PTZ)使动物产生点燃效应。作为对照,在注射PTZ前60分钟给予吡拉西坦或生理盐水。点燃完成24小时后,在穿梭箱范式中对大鼠进行测试。在最后一次点燃注射7天后,给动物注射一次激发剂量的PTZ。最后,对大鼠的大脑进行处理以进行组织学研究。戊四氮点燃的动物癫痫发作评分增加,并且在穿梭箱中存在学习缺陷。吡拉西坦对点燃发展或对激发剂量PTZ的反应均无影响,但它保护动物免受点燃诱导的学习能力下降的影响。该物质对对照动物的学习能力没有影响。在点燃的大鼠的不同海马结构中,发现了神经元细胞丢失。有趣的是,吡拉西坦有效地抵消了这种损伤。从其细胞保护作用方面讨论了吡拉西坦的作用。有人提出,吡拉西坦与临床使用的抗癫痫药物联合给药可能在抗癫痫治疗中有用。

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