In-silico Studies and Antioxidant and Neuroprotective Assessment of Microencapsulated Celecoxib against Scopolamine-induced Alzheimer's Disease.

IF 2.6 4区 医学 Q2 PHARMACOLOGY & PHARMACY Current pharmaceutical design Pub Date : 2024-08-28 DOI:10.2174/0113816128298289240723103828
Rajendra Herur Vishnumurthy, M Gnana Ruba Priya, Prashant Tiwari, Viswas Raja Solomon
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Abstract

Background and objective: Alzheimer's Disease (AD) is an enervating and chronic progressive neurodegenerative disorder. Celecoxib (CXB) possesses efficacious antioxidants and has neuroprotective, anti- inflammatory, and immunomodulatory properties. However, the poor bioavailability of CXB limits its therapeutic utility. Thus, this study aimed to evaluate the microencapsulated celecoxib MCXB) for neuroprotection.

Methodology: CXB was screened by molecular docking study using AutoDock (version 5.2), and the following proteins, such as 4EY7, 2HM1, 2Z5X, and 1PBQ were selected for predicting its neuroprotective effect. Scopolamine 20 mg/kg/day for approximately 7 days was administered to albino rats. Pure CXB 100 mg/kg/- day and 200 mg/kg/day, and MCXB 100 mg/kg/day and 200 mg/kg/day were administered, respectively. Further, to assess the oxidative stress, the nitric oxide (NO), superoxide dismutase (SOD), catalase, and lipid peroxidation (LPO) were evaluated using chemical methods. The neurochemical biomarkers like AChE, glutamate, and dopamine were evaluated using the ELISA method. Further, the histopathology of brain cells was carried out to assess the neuro-regeneration and neurodegeneration of the neurons.

Results: There was a significant binding interaction of CXB (score -6.3, -6.5, -5.1, -9.1) and donepezil (score- 5.5, -7.6, -7.0, and -8.6) with AchE (4EY7), β-secretase (2HM1, monoamine oxidase (2Z5X), and glutamate (1PBQ), respectively. MCXB-treated rats (100 mg/kg/day, 200 mg/kg/day) showed increased SOD levels (p < 0.001), whereas NO, catalase, and LPO levels were significantly (p < 0.001) decreased as compared to scopolamine-treated rats. Further, MCXB-treated rats showed a modulatory effect in the level of dopamine and AchE. However, the glutamate level was significantly (p < 0.001) decreased.

Conclusion: In addition to that, histopathological examination of the hippocampus part showed remarkable improvement in brain cells. So, the findings of the results revealed that MCXB, in a dose-dependent manner, showed a neuroprotective effect against scopolamine-induced AD. This effect may be attributed to the activation of cholinergic pathways.

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微胶囊塞来昔布针对东莨菪碱诱发的阿尔茨海默病的分子内研究及抗氧化和神经保护评估
背景和目的:阿尔茨海默氏症(AD)是一种慢性进行性神经退行性疾病。塞来昔布(CXB)是一种有效的抗氧化剂,具有神经保护、抗炎和免疫调节特性。然而,塞来昔布的生物利用度较低,限制了其治疗作用。因此,本研究旨在评估微囊塞来昔布(MCXB)的神经保护作用:使用 AutoDock(5.2 版)进行分子对接研究,筛选出 4EY7、2HM1、2Z5X 和 1PBQ 等蛋白质用于预测 CXB 的神经保护作用。给白化大鼠注射东莨菪碱 20 毫克/千克/天,持续约 7 天。分别给予纯 CXB 100 毫克/千克/天和 200 毫克/千克/天,以及 MCXB 100 毫克/千克/天和 200 毫克/千克/天。此外,为了评估氧化应激,还使用化学方法评估了一氧化氮(NO)、超氧化物歧化酶(SOD)、过氧化氢酶和脂质过氧化物(LPO)。使用 ELISA 方法评估了 AChE、谷氨酸和多巴胺等神经化学生物标志物。此外,还对脑细胞进行了组织病理学检查,以评估神经元的神经再生和神经退化情况:结果:CXB(得分-6.3、-6.5、-5.1、-9.1)和多奈哌齐(得分-5.5、-7.6、-7.0、-8.6)分别与 AchE(4EY7)、β-分泌酶(2HM1)、单胺氧化酶(2Z5X)和谷氨酸(1PBQ)有明显的结合相互作用。与东莨菪碱处理的大鼠相比,MCXB(100 毫克/千克/天、200 毫克/千克/天)处理的大鼠的 SOD 水平升高(p < 0.001),而 NO、过氧化氢酶和 LPO 水平则显著降低(p < 0.001)。此外,经 MCXB 处理的大鼠对多巴胺和 AchE 水平有调节作用。结论:MCXB 对大鼠的组织病理学研究结果表明,MCXB 对大鼠的多巴胺和 AchE 水平有调节作用,但谷氨酸水平明显下降(p < 0.001):此外,海马部分的组织病理学检查显示脑细胞有明显改善。因此,研究结果表明,MCXB 对东莨菪碱诱导的注意力缺失症具有神经保护作用。这种效应可能归因于胆碱能通路的激活。
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来源期刊
CiteScore
6.30
自引率
0.00%
发文量
302
审稿时长
2 months
期刊介绍: Current Pharmaceutical Design publishes timely in-depth reviews and research articles from leading pharmaceutical researchers in the field, covering all aspects of current research in rational drug design. Each issue is devoted to a single major therapeutic area guest edited by an acknowledged authority in the field. Each thematic issue of Current Pharmaceutical Design covers all subject areas of major importance to modern drug design including: medicinal chemistry, pharmacology, drug targets and disease mechanism.
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