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喹吡罗对氯化锂-匹罗卡品诱导的大鼠癫痫发作的神经保护作用及其机制。

Neuroprotective effects of quinpirole on lithium chloride pilocarpine-induced epilepsy in rats and its underlying mechanisms.

机构信息

Department of Pediatrics, Qilu Hospital of Shandong University, Jinan, Shandong, China.

Department of Pediatrics, The Affiliated Taian City Central Hospital of Qingdao University, Taian, Shandong, China.

出版信息

Eur J Med Res. 2024 Feb 14;29(1):121. doi: 10.1186/s40001-024-01694-x.

Abstract

INTRODUCTION

Epilepsy is a common neurological disorder that presents with challenging mechanisms and treatment strategies. This study investigated the neuroprotective effects of quinpirole on lithium chloride pilocarpine-induced epileptic rats and explored its potential mechanisms.

METHODS

Lithium chloride pilocarpine was used to induce an epileptic model in rats, and the effects of quinpirole on seizure symptoms and cognitive function were evaluated. The Racine scoring method, electroencephalography, and Morris water maze test were used to assess seizure severity and learning and memory functions in rats in the epileptic group. Additionally, immunohistochemistry and Western blot techniques were used to analyze the protein expression levels and morphological changes in glutamate receptor 2 (GluR2; GRIA2), BAX, and BCL2 in the hippocampi of rats in the epileptic group.

RESULTS

First, it was confirmed that the symptoms in rats in the epileptic group were consistent with features of epilepsy. Furthermore, these rats demonstrated decreased learning and memory function in the Morris water maze test. Additionally, gene and protein levels of GluR2 in the hippocampi of rats in the epileptic group were significantly reduced. Quinpirole treatment significantly delayed seizure onset and decreased the mortality rate after the induction of a seizure. Furthermore, electroencephalography showed a significant decrease in the frequency of the spike waves. In the Morris water maze test, rats from the quinpirole treatment group demonstrated a shorter latency period to reach the platform and an increased number of crossings through the target quadrant. Network pharmacology analysis revealed a close association between quinpirole and GluR2 as well as its involvement in the cAMP signaling pathway, cocaine addiction, and dopaminergic synapses. Furthermore, immunohistochemistry and Western blot analysis showed that quinpirole treatment resulted in a denser arrangement and a more regular morphology of the granule cells in the hippocampi of rats in the epileptic group. Additionally, quinpirole treatment decreased the protein expression of BAX and increased the protein expression of BCL2.

CONCLUSION

The current study demonstrated that quinpirole exerted neuroprotective effects in the epileptic rat model induced by lithium chloride pilocarpine. Additionally, it was found that the treatment not only alleviated the rats' seizure symptoms, but also improved their learning and memory abilities. This improvement was linked to the modulation of protein expression levels of GLUR2, BAX, and BCL2. These findings provided clues that would be important for further investigation of the therapeutic potential of quinpirole and its underlying mechanisms for epilepsy treatment.

摘要

简介

癫痫是一种常见的神经系统疾病,其发病机制和治疗策略极具挑战性。本研究旨在探讨喹吡罗对氯化锂-匹罗卡品诱导的癫痫大鼠的神经保护作用及其潜在机制。

方法

采用氯化锂-匹罗卡品诱导癫痫大鼠模型,评价喹吡罗对癫痫大鼠癫痫发作症状和认知功能的影响。采用 Racine 评分法、脑电图和 Morris 水迷宫试验评估癫痫大鼠的癫痫发作严重程度和学习记忆功能。此外,采用免疫组织化学和 Western blot 技术分析癫痫大鼠海马谷氨酸受体 2(GluR2;GRIA2)、BAX 和 BCL2 的蛋白表达水平和形态变化。

结果

首先,证实了癫痫大鼠的症状与癫痫特征一致,并且 Morris 水迷宫试验中大鼠的学习记忆功能下降。此外,癫痫大鼠海马 GluR2 的基因和蛋白水平显著降低。喹吡罗治疗可显著延迟癫痫发作的发生时间,并降低癫痫发作后的死亡率。此外,脑电图显示尖波频率显著降低。在 Morris 水迷宫试验中,喹吡罗治疗组大鼠到达平台的潜伏期缩短,穿越目标象限的次数增加。网络药理学分析表明,喹吡罗与 GluR2 密切相关,涉及 cAMP 信号通路、可卡因成瘾和多巴胺能突触。此外,免疫组织化学和 Western blot 分析表明,喹吡罗治疗可使癫痫大鼠海马颗粒细胞排列更加紧密,形态更加规则。此外,喹吡罗治疗可降低 BAX 蛋白表达,增加 BCL2 蛋白表达。

结论

本研究表明,喹吡罗对氯化锂-匹罗卡品诱导的癫痫大鼠模型具有神经保护作用,不仅能减轻大鼠的癫痫发作症状,还能改善其学习记忆能力,这与调节 GLUR2、BAX 和 BCL2 的蛋白表达水平有关。这些发现为进一步研究喹吡罗的治疗潜力及其对癫痫治疗的潜在机制提供了线索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b470/10865707/a9824bebdfd8/40001_2024_1694_Fig1_HTML.jpg

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