Emoxypine succinate modulates behavioral and molecular responses in zebrafish model of iron Overload-Induced neuroinflammation via CDK5/GSK3- β and NLRP3 inflammasome pathway

IF 2.7 4区医学 Q3 NEUROSCIENCES

Brain Research Pub Date : 2024-09-12 DOI:10.1016/j.brainres.2024.149236

Siddhi Bagwe Parab , Ginpreet Kaur

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Abstract

Excessive iron accumulation in the brain plays a significant role in neurodegenerative processes, contributing to the pathogenesis of Alzheimer’s disease (AD). AD, a prominent neurological disorder affecting the central nervous system, is characterized by the accumulation of beta-amyloid (Aβ) and tau phosphorylation. This accumulation leads to the subsequent development of cognitive impairments, particularly in learning and memory functions. This study investigates the neuroprotective effects of emoxypine succinate in a zebrafish model of iron overload-induced neurodegeneration. Iron was administered to the zebrafish for 28 days to induce neurodegeneration. Following induction, Emoxypine succinate was employed as a treatment intervention for 14 days (concentrations of 4 mg/L, 8 mg/L, and 12 mg/L). Following the end of the treatment, behavioral tests (Y maze test, Novel tank test) were conducted on the zebrafish, and the biochemical (MDA, Catalase, SOD, GSH) and molecular parameters (AchE, Iron levels, IL-1β, TNF-α, CDK-5, GSK-3β, and NLRP3) of the zebrafish brain were also assessed. In the novel tank test, emoxypine succinate-treated groups exhibited significantly increased time in the upper zone (p < 0.001), higher distance travelled (p < 0.001), and shorter latency to the top (p < 0.001) compared to the negative control. Similarly, the Y-maze test revealed improved time in the novel arm (p < 0.001) and total distance travelled (p < 0.001) in treated groups versus the negative control. Assessment of oxidative stress parameters demonstrated significant reductions in oxidative stress in emoxypine succinate-treated groups. Furthermore, AChE activity decreased significantly (p < 0.001), and brain iron levels decreased substantially (p < 0.001) in treated groups, indicating positive therapeutic outcomes. Molecular analysis showed a significant reduction in pro-inflammatory markers like IL-1β, TNF-α, CDK-5, GSK-3β, and NLRP3 (p < 0.001). This comprehensive study highlights the potential efficacy of emoxypine succinate in mitigating neurodegeneration associated with iron dysregulation.

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琥珀酸恩莫西平通过 CDK5/GSK3- β 和 NLRP3 炎症小体通路调节铁超载诱导神经炎症斑马鱼模型的行为和分子反应

大脑中铁的过度积累在神经退行性过程中起着重要作用，是阿尔茨海默病（AD）的发病机理之一。阿尔茨海默病是一种影响中枢神经系统的常见神经系统疾病，其特征是β-淀粉样蛋白（Aβ）的积累和tau磷酸化。这种积累会导致认知障碍，尤其是学习和记忆功能障碍。本研究调查了琥珀酸依莫昔平在铁超载诱导的神经变性斑马鱼模型中的神经保护作用。给斑马鱼注射铁剂 28 天以诱导神经变性。诱导后，使用琥珀酸依莫司汀作为治疗干预，为期 14 天（浓度分别为 4 毫克/升、8 毫克/升和 12 毫克/升）。治疗结束后，对斑马鱼进行行为测试（Y迷宫测试、新型水箱测试），并评估斑马鱼大脑的生化指标（MDA、过氧化氢酶、SOD、GSH）和分子指标（AchE、铁水平、IL-1β、TNF-α、CDK-5、GSK-3β和NLRP3）。在新型坦克测试中，与阴性对照组相比，琥珀酸依莫司汀处理组在上区的时间显著增加（p < 0.001），行进距离显著增加（p < 0.001），到达顶部的潜伏期显著缩短（p < 0.001）。同样，Y-迷宫测试显示，与阴性对照组相比，治疗组在新手臂上的时间（p <0.001）和行进总距离（p <0.001）均有所改善。对氧化应激参数的评估表明，琥珀酸依莫司汀治疗组的氧化应激显著降低。此外，治疗组的 AChE 活性明显降低（p < 0.001），脑铁水平大幅下降（p < 0.001），表明治疗效果良好。分子分析表明，IL-1β、TNF-α、CDK-5、GSK-3β 和 NLRP3 等促炎标记物明显减少（p < 0.001）。这项综合研究强调了琥珀酸依莫昔平在缓解与铁失调相关的神经退行性变方面的潜在功效。

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来源期刊

Brain Research 医学-神经科学

CiteScore

5.90

自引率

3.40%

发文量

268

审稿时长

47 days

期刊介绍： An international multidisciplinary journal devoted to fundamental research in the brain sciences. Brain Research publishes papers reporting interdisciplinary investigations of nervous system structure and function that are of general interest to the international community of neuroscientists. As is evident from the journals name, its scope is broad, ranging from cellular and molecular studies through systems neuroscience, cognition and disease. Invited reviews are also published; suggestions for and inquiries about potential reviews are welcomed. With the appearance of the final issue of the 2011 subscription, Vol. 67/1-2 (24 June 2011), Brain Research Reviews has ceased publication as a distinct journal separate from Brain Research. Review articles accepted for Brain Research are now published in that journal.