vigabatrin 但不是丙戊酸钠可预防 N-甲基-D-天冬氨酸 (NMDA) 在未成年大鼠中诱导的年龄特异性屈肌发作。
Vigabatrin but not valproate prevents development of age-specific flexion seizures induced by N-methyl-D-aspartate (NMDA) in immature rats.
机构信息
Institute of Physiology, Academy of Sciences of the Czech Republic, Prague, Czech Republic.
出版信息
Epilepsia. 2010 Mar;51(3):469-72. doi: 10.1111/j.1528-1167.2009.02305.x. Epub 2009 Sep 22.
In immature rats, N-methyl-D-aspartate (NMDA) induces several seizure types: flexion seizures (FS; in rats younger than 3 weeks), clonic seizures (in animals older than 3 weeks), and clonic-tonic seizures (CTS; in rats of all ages). FS represent a model of human infantile spasms. Effects of vigabatrin and valproate against all types of NMDA-induced seizures were studied in rats at postnatal days 12 (P12) and 25 (P25). NMDA (60 or 300 mg/kg) was injected to animals pretreated with vigabatrin (300-1,200 mg/kg; 24 h before NMDA) or valproate (100-400 mg/kg; 15 min before NMDA). Vigabatrin suppressed FS in P12 rats, but was ineffective against CTS in both age groups. Valproate suppressed CTS in P12, but not in P25 rats. Clonic seizures were rare in NMDA-treated P25 rats, but valproate pretreatment increased their incidence significantly. Neither drug decreased NMDA-induced mortality, which occurred within approximately 15 min after NMDA administration and reached almost 100% in all groups.
在未成熟的大鼠中,N-甲基-D-天冬氨酸(NMDA)会引起多种癫痫发作类型:屈肌发作(FS;在 3 周龄以下的大鼠中)、阵挛性发作(在 3 周龄以上的动物中)和阵挛-强直发作(CTS;在所有年龄段的大鼠中)。FS 代表了人类婴儿痉挛的一种模型。在出生后第 12 天(P12)和第 25 天(P25)的大鼠中研究了氨己烯酸和丙戊酸对所有类型 NMDA 诱导的癫痫发作的作用。NMDA(60 或 300 mg/kg)注射到预先用氨己烯酸(300-1200 mg/kg;NMDA 前 24 小时)或丙戊酸(100-400 mg/kg;NMDA 前 15 分钟)预处理的动物中。氨己烯酸抑制 P12 大鼠的 FS,但对两个年龄组的 CTS 均无效。丙戊酸抑制 P12 大鼠的 CTS,但对 P25 大鼠无效。NMDA 处理的 P25 大鼠中很少发生阵挛性发作,但丙戊酸预处理显著增加了其发生率。两种药物都不能降低 NMDA 诱导的死亡率,这种死亡率在 NMDA 给药后约 15 分钟内发生,在所有组中几乎达到 100%。
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