Effects of acrous gramimeus and its main component alpha-asarone on the reactivity and convulsive threshold of immature rats to electric stimulation

BACKGROUND： The traditional Chinese medicine acrous gramimeus is the dry rhizome of Acrous gramimeus Soland, a kind of Araceae familial perennial herb, which has a sedation action, anticonvulsant and antiepileptic effect. Its effective component has not been known yet, and α-asarone, the major component of the volatile oil extracted from acrous gramineus, has been supposed to play a necessary role in it. OBJECTIVE： To explore the effects of acrous gramimeu and α-asarone on the reactivity and convulsive threshold to electric stimulation in immature rats, furthermore, attempt to definitize the anticonvulsant effect of α-asarone. DESIGN： A randomized controlled study.SETTINGS： Department of Pediatrics, First Hospital of Jilin University; Department of Histology and Embryology, School of Basic Medical Sciences of Jilin University; Department of Neurology, First Clinical Hospital affiliated to Harbin Medical University; Department of Internal Medicine, Children＇s Hospital of Changchun City. MATERIALS ： Seventy 3-week immature Wistar rats （either males or females） of 34-40 g were used. Acrous gramimeu （1 g/bag, the content of α-oasarone was 0.046 26%-0.070 16%） with the batch number of 0307113 was provided by Tianjiang Medicine Company Limited, Jiangyin City. α-asarone tablet （60 mg per tablet） with the batch number of 030219 was provided by Tianwei Pharmaceutical Factory, Shenyang City. α-asarone injectable preparation （2 mL per piece） with the batch number of 030105 was provided by Shuanghe Medicine Limited Company, Beijing City. METHODS ： The experiments were carried out in the Neurological Laboratory of the First Hospital of Jilin University between August and October in 2004.① The 70 rats were randomly divided into intragastric subset and intraperitoneal subset. The intragastric subset included four groups of control, phenobarbital sodium, acrous gramimeu and α-asarone; the intraperitoneal subset included three groups of control, phenobarbital sodium and α-asarone. There were 10 rats per group. ② In the intragastric subset, different group was treated with saline （1 mL for each time, phenobarbital sodium （18 mg/kg per day）, acrous gramineu （2 350 mg/kg per day） and α-asarone （29 mg/kg per day） respectively twice every day for 5 days. In the intraperitoneal subset, different group was treated with saline （0.5 mL）, phenobarbital sodium （29 mg/kg） and α-asarone （2.9 mg/kg） respectively. ③ Before and after administration for 5 days in the intragastric subset as well as before and after administration for about 1 hour in the intraperitoneal subset respectively, the rats were given electric stimulation with the NIHOM KOMDEM multifunctional electrophysiological recorder, and the reactivity and convulsive threshold to electric stimulation of the rats were recorded. MAIN OUTCOME MEASURES： The reactivity and convulsive threshold to electric stimulation in immature rats were compared. RESULTS： All the rats were involved in the analysis of results. ① Results for intragastric administration： Before intragastric administration, there were no obvious differences in the reactivity and convulsive threshold to electric stimulation among the groups （P 〉 0.05）. After intragastric administration for 5 days, the reactivity and convulsive threshold to the electric stimulation had no obvious changes in the control group, but those were significantly higher than before administration in the drug administration groups （t=-3.317-7.401, P 〈 0.01）, which were also obviously higher than those in the control group （t=3.027-8.941, P 〈 0.01）, and those in the acrous gramimeu group and α-asarone group were not markedly different from those in the phenobarbital sodium group. ② Results for intraperitoneal injection： Before intraperitoneal injection, the reactivity and convulsive threshold to the electric stimulation had no obvious differences among the groups. After the intraperitoneal injection for 1 hour, the reactivity and convulsive threshold to the electric stimulation had no obvious change in the control group, but those were significantly higher than before administration in the drug administration groups （P 〈 0.01）, which were also obviously higher than those in the control group （t=6.211-7.237, P 〈 0.01; t=4.085-5.633, P 〈 0.05）, and there was no marked difference between α-asarone group and phenobarbital sodium group （P 〉 0.05）.CONCLUSION ： ① As effective anticonvulsants, both acrous gramineu and α-asarone can enhance the reactivity and convulsive threshold of immature rats to electric stimulation. ② As one of the major effective components against convulsion of acrous gramineu, α-asarone is equivalent to phenobarbital sodium.

石菖蒲及其有效成分-细辛醚对癫痫幼鼠海马区神经元N-甲基-D-天冬氨酸受体表达的影响

目的探讨在戊四氮(PTZ)诱发的癫痫动物模型中,石菖蒲及其主要成分α-细辛醚对海马区神经元N-甲基-D-天冬氨酸受体1(NMDAR1) mRNA表达水平的影响。方法3周龄Wistar幼鼠ipPTZ60mg/kg建立癫痫模型。动物模型随机分为模型对照组、石菖蒲组、α-细辛醚组,另设正常对照组。各组均ig给药。正常对照组给予生理盐水1.0mL/d,其余各组分别给予石菖蒲2350mg/(kg·d),α-细辛醚29mg/(kg·d),连续7d。次日ipPTZ60mg/kg,观察动物行为变化,1d后处死动物,取左侧大脑固定用于原位杂交;取右侧海马组织用于半定量RT-PCR,检测海马CA1、CA3区神经元NMDRA1 mRNA的表达情况。结果原位杂交结果显示,阳性染色颗粒定位于海马神经元胞质内。石菖蒲和α-细辛醚治疗组海马区神经元阳性细胞数和平均吸光度均明显少于模型对照组(P<0.05)。半定量RT-PCR结果显示,石菖蒲和α-细辛醚治疗组海马组织中NMDAR1 mRNA的相对表达量均较显著低于模型对照组(P<0.05)。结论石菖蒲和α-细辛醚可能通过抑制海马区神经元谷氨酸NMDAR1表达而发挥抑制PTZ诱发的幼鼠癫痫发作。

石菖蒲及其成分对幼鼠电刺激反应性和电致惊厥阈的影响

目的 观察石菖蒲及其成分对幼鼠电刺激反应性和电致惊厥阈的影响 ,以阐明石菖蒲及其成分抗儿童癫痫的有效性。方法 将 70只 3周龄 Wister幼鼠随机分为灌胃组和腹腔注射组 ,灌胃组于用药前后 5 d,腹腔注射组于用药前后 1h分别给予电刺激 ,观测电刺激反应性和电致惊厥阈。结果 石菖蒲及其成分 α-细辛醚能提高电刺激反应性和电致惊厥阈 ,治疗前各组无显著差异 (P>0 .0 5 ) ,治疗后与对照组比较均有显著差异 (P<0 .0 5 )。石菖蒲与 α-细辛醚治疗前后各组比较无显著差异 (P>0 .0 5 )。结论 (1)石菖蒲及 α-细辛醚能提高幼鼠电刺激反应性和电致惊厥阈 ,有较好的抗癫痫作用。石菖蒲与 α-细辛醚的疗效一致。 (2 ) α-细辛醚是石菖蒲抗癫痫的主要有效成分之一 ,值得进一步研究。