National Epilepsy Center, Shizuoka Institute of Epilepsy and Neurological Disorders, Shizuoka, Japan.
Epilepsia. 2012 Jul;53(7):1140-5. doi: 10.1111/j.1528-1167.2012.03497.x. Epub 2012 May 11.
We previously reported a mutant mouse carrying a severe myoclonic epilepsy in infancy (SMEI) mutation in Scn1a. In this study, we examined the susceptibility to hyperthermia-induced seizures of heterozygous Scn1a mutant mice (Scn1a(RX/+)) and wild-type (Scn1a(+/+) ) mice. Then we assessed the efficacy of stiripentol (STP) monotherapy versus STP and clobazam (CLB) combination therapy to prevent hyperthermia-induced seizures in Scn1a(RX/+) mice.
The seizure-inducing body temperatures in Scn1a(RX/+) mice and age-matched Scn1a(+/+) mice were compared in three age groups (1 month, 3-5 months, > 6 months). Then STP, CLB, or STP + CLB was administered intraperitoneally to Scn1a(RX/+) mice of two age groups (p1M, aged 1 month; p5M, aged 5-10 months). The efficacy of medications was assessed by comparing the seizure-inducing body temperature and the duration of seizures.
The seizure-inducing body temperature was significantly lower in Scn1a(RX/+) than in Scn1a(+/+) mice for all age groups (p < 0.01). The seizure-inducing body temperature was significantly elevated after administration of STP in p1M (p < 0.05) but not in p5M (p > 0.05), and it was significantly elevated after administration of CLB in both age groups (p < 0.05). The seizure-inducing body temperature was significantly higher after administration of STP + CLB than after administration of CLB in p5M (p < 0.05).
Scn1a (RX/+) mice have increased susceptibility to hyperthermia-induced seizure in all age groups. STP monotherapy is effective in preventing hyperthermia-induced seizures in Scn1a(RX/+) mice aged 1 month, but not in those aged 5 months and older. When used in combination therapy with CLB, STP inhibits the metabolism of CLB and probably synergistically enhances the anticonvulsant effect in mice aged 1 month.
我们之前报道了一种携带 Scn1a 严重婴儿肌阵挛性癫痫(SMEI)突变的突变型小鼠。在这项研究中,我们检测了杂合型 Scn1a 突变小鼠(Scn1a(RX/+))和野生型(Scn1a(+/+))小鼠对高热诱导性癫痫发作的易感性。然后,我们评估了 stiripentol(STP)单药治疗与 STP 和 clobazam(CLB)联合治疗预防 Scn1a(RX/+)小鼠高热诱导性癫痫发作的疗效。
在三个年龄组(1 个月、3-5 个月、>6 个月)中比较 Scn1a(RX/+)小鼠和年龄匹配的 Scn1a(+/+)小鼠的致痫体温。然后,将 STP、CLB 或 STP+CLB 腹腔内给药给两个年龄组的 Scn1a(RX/+)小鼠(p1M,年龄 1 个月;p5M,年龄 5-10 个月)。通过比较致痫体温和癫痫发作持续时间来评估药物的疗效。
所有年龄组的 Scn1a(RX/+)小鼠的致痫体温均明显低于 Scn1a(+/+)小鼠(p<0.01)。STP 给药后,p1M 组(p<0.05)但 p5M 组(p>0.05)的致痫体温显著升高,CLB 给药后两个年龄组的致痫体温均显著升高(p<0.05)。p5M 组 STP+CLB 给药后的致痫体温明显高于 CLB 给药后(p<0.05)。
Scn1a(RX/+)小鼠在所有年龄组均对高热诱导性癫痫发作的易感性增加。STP 单药治疗可有效预防 1 月龄 Scn1a(RX/+)小鼠高热诱导性癫痫发作,但对 5 月龄及以上小鼠无效。当与 CLB 联合应用时,STP 抑制 CLB 的代谢,可能在 1 月龄小鼠中协同增强抗惊厥作用。
