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二氢吡啶类钙离子拮抗剂对电休克惊厥的抗惊厥作用。

Anticonvulsant effects of dihydropyridine Ca2+ antagonists in electrocortical shock seizures.

作者信息

Meyer F B, Anderson R E, Sundt T M

机构信息

Cerebrovascular Research Department of Neurosurgery, Mayo Clinic, Rochester, Minnesota 55905.

出版信息

Epilepsia. 1990 Jan-Feb;31(1):68-74. doi: 10.1111/j.1528-1157.1990.tb05362.x.

Abstract

The dihydropyridine calcium antagonists nimodipine (NMD), PN200-110, and nicardipine were compared with phenytoin (PHT) as potential anticonvulsants in electrocortical shock (ECS)-induced seizures in the white New Zealand rabbit. Before treatment, seizure duration ranged from 43.8 +/- 5.1 to 49.6 +/- 5.2 s with an ECS stimulus of 10-V, 100-Hz, 0.1-ms pulses for 5 s. Each drug was administered into the right internal intracarotid artery 2 min before the ECS. A cumulative nimodipine dose of 440 micrograms/kg decreased seizure discharge to 6.6 +/- 5.0 s (p less than 0.001), whereas a total dose of 1.0 mg/kg PN200-110 was required to achieve a similar effect. Nicardipine was ineffective. A cumulative dose of 7 mg/kg phenytoin was required to suppress seizure discharge. These results indicate that Ca2+ channels modulated by dihydropyridines play a facilitating role in ECS-induced seizures. We propose that the anticonvulsant effects of nimodipine and PN200-110 are due to inhibition of neuronal calcium L-channels. Dihydropyridine Ca2+ antagonists that penetrate the blood-brain barrier (BBB) and bind to neuronal tissue may emerge as a novel class of anticonvulsants.

摘要

在白色新西兰兔的电皮质休克(ECS)诱发癫痫实验中,将二氢吡啶类钙拮抗剂尼莫地平(NMD)、PN200 - 110和尼卡地平与苯妥英(PHT)作为潜在的抗惊厥药进行了比较。治疗前,在10伏、100赫兹、0.1毫秒脉冲刺激5秒的ECS作用下,癫痫发作持续时间为43.8±5.1至49.6±5.2秒。每种药物均在ECS前2分钟经右侧颈内动脉给药。尼莫地平累积剂量440微克/千克可使癫痫放电减少至6.6±5.0秒(p<0.001),而PN200 - 110达到类似效果则需要总剂量1.0毫克/千克。尼卡地平无效。抑制癫痫放电需要苯妥英累积剂量7毫克/千克。这些结果表明,二氢吡啶调节的Ca2 +通道在ECS诱发的癫痫中起促进作用。我们认为尼莫地平和PN200 - 110的抗惊厥作用是由于抑制了神经元钙L通道。能够穿透血脑屏障(BBB)并与神经元组织结合的二氢吡啶类Ca2 +拮抗剂可能会成为一类新型抗惊厥药。

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