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来自巴氏真涡蛛毒液的新型非选择性 GABA 摄取抑制剂 Parawixin2 可抑制戊四氮诱导的大鼠化学点燃。

Parawixin2, a novel non-selective GABA uptake inhibitor from Parawixia bistriata spider venom, inhibits pentylenetetrazole-induced chemical kindling in rats.

机构信息

Neurobiology and Venoms Laboratory, Department of Biology, College of Philosophy, Sciences and Literature of Ribeirão Preto, University of São Paulo, Ribeirão Preto, SP, Brazil.

出版信息

Neurosci Lett. 2013 May 24;543:12-6. doi: 10.1016/j.neulet.2013.02.074. Epub 2013 Apr 3.

DOI:10.1016/j.neulet.2013.02.074
PMID:23562887
Abstract

The aims of the present work were to investigate the effects of the repeated administration of Parawixin2 (2-amino-5-ureidopentanamide; formerly FrPbAII), a novel GABA and glycine uptake inhibitor, in rats submitted to PTZ-induced kindling. Wistar rats were randomly divided in groups (n=6-8) for different treatments. Systemic injections of PTZ were administered every 48 h in the dose of 33 mg/kg; i.p., that is sufficient to induce fully kindled seizures in saline i.c.v. treated rats in a short period of time (28 days). Treatments in two types of positive controls (diazepam - DZP and nipecotic acid - NA groups) consisted in daily systemic injections of DZP (2mg/kg; i.p.) or i.c.v. injections of NA (12 μg/μL), while in experimental groups in daily i.c.v. injections of different doses of Parawixin2 (0.15; 0.075; 0.015 μg/μL). Seizures were analyzed using the Lamberty & Klitgaard score and kindling was considered as established after at least three consecutive seizures of score 4 or 5. Cumulative seizure scores for each group were analyzed using repeated measures of ANOVA followed by Tukey test. PTZ induced 4 and 5-score seizures after 12 injections in saline treated rats, whereas daily injection of Parawixin2 inhibited the onset of seizures in a dose dependent manner. Also, the challenging administration of PTZ did not raise seizure score in animals treated with the highest dose of Parawixin2 or those treated with DZP or NA. These findings together with previous data from our laboratory show that Parawixin2 could be a useful probe to design new antiepileptic drugs.

摘要

本研究旨在探讨新型 GABA 和甘氨酸摄取抑制剂 Parawixin2(2-氨基-5-脲戊酰胺;前 FrPbAII)重复给药对匹鲁卡品诱导点燃大鼠的影响。Wistar 大鼠随机分为几组(n=6-8),进行不同的处理。PTZ 以 33mg/kg 的剂量腹腔内注射,每 48 小时 1 次,足以在短时间内(28 天)诱导盐水脑室注射的大鼠完全点燃发作。两种阳性对照(地西泮-DZP 和烟碱酸-NA 组)的治疗包括每日腹腔注射地西泮(2mg/kg;i.p.)或脑室注射烟碱酸(12μg/μL),而实验组则每日脑室注射不同剂量的 Parawixin2(0.15、0.075 和 0.015μg/μL)。采用 Lamberty 和 Klitgaard 评分分析发作,至少连续 3 次评分 4 或 5 分则认为点燃成功。采用重复测量方差分析和 Tukey 检验分析每组的累积发作评分。在盐水处理的大鼠中,PTZ 诱导 4 和 5 分评分发作 12 次后,Parawixin2 以剂量依赖的方式抑制发作的发生。此外,在给予最高剂量 Parawixin2 或 DZP 或 NA 处理的动物中,挑战性给予 PTZ 并未提高发作评分。这些发现与我们实验室之前的数据一起表明,Parawixin2 可能是设计新型抗癫痫药物的有用探针。

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