Neuroprotective Activity of 5-ethoxy-2-ethylthiobenzimidazole (Etomerzol) and 2-ethylthiobenzimidazole (Bemitil) in a Model of Middle Cerebral Artery Occlusion

Q3 Pharmacology, Toxicology and Pharmaceutics Drug Development and Registration Pub Date : 2023-10-12 DOI:10.33380/2305-2066-2023-12-4-1584
E. Yu. Zavarina, E. K. Krasova, I. A. Titovich, A. N. Kimaev
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Abstract

Introduction. Cerebrovascular diseases (CVD) are one of the most pressing medical and social problems due to the high rate of mortality and disability. Stroke is the leading cause of CVD. About 15 million strokes are registered annually in the world according to the World Federation of Neurological Societies. It should be noted that CVD of ischemic origin has a tendency to rejuvenation and growth. Traditionally, in clinical practice, antihypoxic, antioxidant agents, as well as drugs with neuroprotective and neurorehabilitation effects are used to treat CVD. In connection with the increase in the incidence of CVD, there is an urgent need to search for promising neuroprotectors. Aim. To study the neuroprotective activity of 5-ethoxy-2-ethylthiobenzimidazole (etomerzol) and 2-ethylthiobenzimidazole (bemityl) in a model of middle cerebral artery occlusion. Materials and methods. Occlusion of the middle cerebral artery (ОMCA) was used as a model. The object of the study was inbred male rats of the Dark Agouti line, randomized into five groups: a group of intact animals and four groups with OSMA: a control group, a group with the introduction of 5-ethoxy-2-ethylthiobenzimidazole (etomerzole, 25 mg/kg), a group with the introduction 2-ethylthiobenzimidazole (bemityl, 25 mg/kg) and a group with the reference drug dimethyl fumarate (DMF, 100 mg/kg). On the 1st, 3rd, and 7th days after the operation, the "Limb Stimulation" (SC) test was performed. On the 7th day, the tests "Open field" (OP) and "Elevated plus maze" (EPM) were performed. Euthanasia was performed on the 7th day in an induction chamber (Bioscape GmbH, CO 2 box for euthanasia, Germany). Results and discussion. The study showed a pronounced pharmacological effect of etomerzole in a model of acute ischemic stroke. The introduction of bemitil, etomerzol and DMF significantly reduced the neurological deficit 24 hours after OSMA and improved the psycho-functional state on the 7th day. Thus, in the etomerzol group on the first day after surgery, the neurological deficit was reduced by 1.9 times ( p < 0.05), and by 3 and 2.0 times ( p < 0.05) compared with the control group. While bemityl and DMF reduced the index by 1.3 ( p < 0.05) and 1.4 times ( p < 0.05) on the 3rd day and by 1.5 times ( p < 0.05) on the 7th day. In the OP test in the etomerzol group, an increase in HDA by 2.7 times ( p < 0.05) was observed compared with the control. The rate of peering into minks in the etomersol and bemitil groups was higher than in the control group by 2.6 ( p < 0.05) and 3.4 times ( p < 0.05), respectively. Search and research activity was increased in the same groups by 2.0 ( p < 0.05) and 2.2 times ( p < 0.05) compared to control animals. In the PCL test, the etomerzol and DMF groups showed an increase in the number of uprights in the sleeves compared to the control group by 2.7 ( p < 0.05) and 3.8 times ( p < 0.05), respectively. In the etomerzol and bemityl groups, there was an increase in the number of overhangs by 3.4 ( p < 0.05) and 6.2 times ( p < 0.05). Conclusion. The data obtained during the study of the activity of benzimidazoles after ischemic stroke indicate a significant increase in the motor activity of animals in the OP tests, which may indicate a psychostimulating and potential nootropic effect of etomerzole and bemitil, and an increase in the number of racks and hangings in the PCL test can be regarded as manifestation of anxiolytic activity. In our study, the severity of the pharmacological effects of DMF was inferior to benzimidazoles. However, a significant decrease in neurological deficit in the SC test and an increase in the number of uprights in the sleeves in the PCL may indicate the presence of anxiolytic activity in the drug. The results obtained underline the importance of conducting additional studies to evaluate the effectiveness of DMF in OSMA.
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5-乙氧基-2-乙基硫代苯并咪唑(Etomerzol)和2-乙基硫代苯并咪唑(Bemitil)对大脑中动脉闭塞模型的神经保护作用
介绍。脑血管病(CVD)因其高死亡率和致残率而成为最紧迫的医学和社会问题之一。中风是心血管疾病的主要原因。根据世界神经学会联合会的数据,全世界每年约有1500万例中风病例。值得注意的是,缺血性心血管疾病有恢复和生长的趋势。传统上,在临床实践中,抗缺氧、抗氧化剂以及具有神经保护和神经康复作用的药物被用于治疗心血管疾病。随着心血管疾病发病率的增加,迫切需要寻找有前途的神经保护剂。的目标。目的研究5-乙氧基-2-乙基硫代苯并咪唑(etomerzol)和2-乙基硫代苯并咪唑(bemityl)对大脑中动脉闭塞模型的神经保护作用。材料和方法。以大脑中动脉闭塞(ОMCA)为模型。研究对象为近交系黑鼠系雄性大鼠,随机分为5组:完整动物组和4组OSMA:对照组、5-乙氧基-2-乙基硫代苯并咪唑组(依托咪唑,25 mg/kg)、2-乙基硫代苯并咪唑组(乙咪唑,25 mg/kg)和对照药物富马酸二甲酯组(DMF, 100 mg/kg)。术后第1、3、7天进行“肢体刺激”(SC)试验。第7天进行“空地”(OP)和“高架+迷宫”(EPM)试验。第7天在诱导室(Bioscape GmbH, CO 2 box for安乐死,德国)中进行安乐死。结果和讨论。该研究表明,艾美唑对急性缺血性脑卒中模型有明显的药理作用。贝米特、乙omerzol和DMF的引入显著降低了OSMA后24小时的神经功能缺损,并在第7天改善了心理功能状态。因此,术后第一天使用依omerzol组,神经功能缺损减少了1.9倍(p <0.05),分别增加3倍和2.0倍(p <0.05),与对照组比较。而bemityl和DMF使该指数降低了1.3 (p <0.05)和1.4倍(p <0.05),第3天增加1.5倍(p <第7天0.05)。在OP试验中,艾美唑组HDA升高2.7倍(p <与对照组比较,差异有统计学意义(0.05)。乙omersol组和bemitil组的刺入水貂率比对照组高2.6 (p <0.05)和3.4倍(p <分别为0.05)。同一组的搜索和研究活动增加了2.0 (p <0.05)和2.2倍(p <0.05)。在PCL试验中,与对照组相比,乙omerzol组和DMF组在套筒中的直立数量增加了2.7 (p <0.05)和3.8倍(p <分别为0.05)。在乙omerzol和bemityl组中,悬垂数增加了3.4个(p <0.05)和6.2倍(p <0.05)。结论。在缺血性卒中后苯并咪唑活性研究中获得的数据表明,OP试验中动物的运动活动明显增加,这可能提示依咪唑和贝米特具有精神刺激和潜在的益智作用,PCL试验中挂架次数的增加可视为抗焦虑活性的表现。在我们的研究中,DMF药理作用的严重程度不如苯并咪唑。然而,SC试验中神经功能缺陷的显著减少和PCL中袖子中直立数量的增加可能表明药物中存在抗焦虑活性。所获得的结果强调了开展进一步研究以评估DMF在OSMA中的有效性的重要性。
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来源期刊
Drug Development and Registration
Drug Development and Registration Pharmacology, Toxicology and Pharmaceutics-Pharmaceutical Science
CiteScore
1.20
自引率
0.00%
发文量
61
审稿时长
8 weeks
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