刺梨皮酒精提取物的抗惊厥作用。

Dhirender Kaushik, Ajay Kumar, Pawan Kaushik, Avatar C Rana
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引用次数: 17

摘要

目的:研究刺梨皮醇提物的抗惊厥活性。(AEPR)在印度传统医学系统中用于治疗惊厥。方法:采用最大电击法(MES)和戊四唑(PTZ)诱导的大鼠抗惊厥作用。在MES模型中,通过耳电极给予150ma 0.2 s电流诱导大鼠惊厥。以后肢强直性伸展的持续时间为终点,即预防或减少后肢伸展的持续时间作为保护作用。在PTZ模型中,AEPR的抗惊厥特性是通过其延迟PTZ腹腔注射引起的肌阵挛性痉挛和阵挛性惊厥发作的能力来评估的。结果:AEPR剂量为300和500 mg/kg体重可显著减少mes诱导的惊厥各期发作(p)。结论:AEPR对全身性强直-阵挛性和部分性惊厥均有效。因此,AEPR对MES和ptz诱导的Wistar大鼠癫痫发作具有抗惊厥作用。然而,进一步的研究正在进行中,以分离出负责其活性的化合物。
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Anticonvulsant activity of alcoholic extract of bark of Pinus roxburghii Sarg.

Objective: To study the anticonvulsant activity of alcoholic extract of bark of Pinus roxburghii Sarg. (AEPR) used in Indian traditional medicine system in treating convulsion.

Methods: Anticonvulsant activity was evaluated by maximal electroshock (MES) and pentylenetetrazole (PTZ)-induced seizures in Wistar albino rats. In the MES model, 150 mA current for 0.2 s was given through ear electrodes to induce convulsions in rats. The duration of tonic extension of hind limb was used as the end point, namely, prevention or decrease in the duration of hind limb extension was considered as a protective action. In the PTZ model, the anticonvulsant property of AEPR was assessed by its ability to delay the onset of myoclonic spasm and clonic convulsions produced by intraperitoneal administration of PTZ.

Results: In the MES-induced seizure model, AEPR in doses of 300 and 500 mg/kg body weight reduced all the phases of convulsion significantly (P<0.01). Standard drug phenytoin at a dose of 25 mg/kg significantly reduced flexion phase (P<0.01) and abolished all phases of convulsion. In the PTZ-induced seizure model, the administration of the extract at doses of 300 and 500 mg/kg 30 min prior to injection of PTZ significantly delayed the onset of clonic seizure (P<0.01). AEPR at the dose of 100 mg/kg body weight could not exert any significant protective effect on PTZ-induced convulsions. Standard drug diazepam at a dose of 4 mg/kg showed much delayed onset of clonic seizure.

Conclusion: The study suggests that AEPR would be effective against generalized tonic-clonic and partial seizures. Thus AEPR possesses anticonvulsant property against MES- and PTZ-induced seizures in Wistar rats. However, further research is in progress to isolate the compound responsible for its activity.

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