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NMDA和非NMDA受体拮抗剂对未成熟大鼠同型半胱氨酸诱发癫痫发作的抗惊厥作用。

Anticonvulsant action of both NMDA and non-NMDA receptor antagonists against seizures induced by homocysteine in immature rats.

作者信息

Folbergrová J

机构信息

Institute of Physiology, Academy of Sciences of the Czech Republic, Vídeñská, Prague.

出版信息

Exp Neurol. 1997 Jun;145(2 Pt 1):442-50. doi: 10.1006/exnr.1997.6464.

DOI:10.1006/exnr.1997.6464
PMID:9217080
Abstract

Seizures were induced in immature 18-day-old rats by i.p. administration of homocysteine (11 mmol/kg) and the effects of selected antagonists of NMDA receptors [MK-801 (0.5 mg/kg), AP7 (0.33 mmol/kg), CGP 40116 (10 mg/kg)] and non-NMDA receptors [GDEE (4 mmol/kg), NBQX (two doses, 30 mg/kg each)] were studied. The effect of MgSO4 (two doses, 2 mmol/kg each) was also tested. The anticonvulsant effect was evaluated not only from the behavioral manifestations of seizures, but also in terms of some indicators of brain energy metabolism. Rat pups were sacrificed during generalized clonic-tonic seizures, corresponding to 16-45 min after homocysteine administration. Comparable time intervals were used for sacrificing the pups which had received the protective drugs. In contrast to neonatal rats, in which only NMDA antagonists could prevent homocysteine-induced seizures, both NMDA and non-NMDA receptor antagonists exerted an anticonvulsant effect in 18-day-old rats. In addition, the pronounced anticonvulsant effect could be achieved by the combined treatment with low subthreshold doses of NMDA (MK-801) and non-NMDA (NBQX) receptor antagonists. The protection was evident not only in suppressing behavioral symptoms of seizures, but also in preventing most of the metabolic changes accompanying seizures, mainly glycogen degradation. More than a sevenfold accumulation of lactate occurring during seizures was markedly reduced by all the tested drugs, but was not completely eliminated. All antagonists, when given alone in the same doses as those used for seizure protection, remained without any effect on lactate levels. Comparison of the present data with previous findings concerning neonatal rats suggests that there may be a developmental change in anticonvulsant efficacy of non-NMDA receptor antagonists against homocysteine-induced seizures in rats.

摘要

通过腹腔注射同型半胱氨酸(11 mmol/kg)诱导18日龄未成熟大鼠癫痫发作,并研究了NMDA受体的选定拮抗剂[MK-801(0.5 mg/kg)、AP7(0.33 mmol/kg)、CGP 40116(10 mg/kg)]和非NMDA受体的选定拮抗剂[GDEE(4 mmol/kg)、NBQX(两剂,各30 mg/kg)]的作用。还测试了硫酸镁(两剂,各2 mmol/kg)的作用。不仅从癫痫发作的行为表现评估抗惊厥作用,还根据脑能量代谢的一些指标进行评估。在全身阵挛性强直发作期间(相当于同型半胱氨酸给药后16 - 45分钟)处死幼鼠。对于接受了保护药物的幼鼠,采用相同的时间间隔进行处死。与新生大鼠不同,新生大鼠只有NMDA拮抗剂能预防同型半胱氨酸诱导的癫痫发作,而在18日龄大鼠中,NMDA和非NMDA受体拮抗剂均发挥抗惊厥作用。此外,联合使用低亚阈值剂量的NMDA(MK-801)和非NMDA(NBQX)受体拮抗剂可产生显著的抗惊厥作用。这种保护作用不仅体现在抑制癫痫发作的行为症状上,还体现在预防癫痫发作伴随的大多数代谢变化上,主要是糖原降解。所有受试药物均显著降低了癫痫发作期间出现的乳酸七倍以上的积累,但并未完全消除。所有拮抗剂单独以与癫痫保护相同的剂量给药时,对乳酸水平均无任何影响。将本研究数据与先前关于新生大鼠的研究结果进行比较表明,大鼠中针对同型半胱氨酸诱导的癫痫发作,非NMDA受体拮抗剂的抗惊厥疗效可能存在发育变化。

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