柯奈新通过减轻神经炎症和氧化应激缓解 PTZ 诱发的大鼠癫痫模型

IF 5.3 2区 化学 Q2 CHEMISTRY, MULTIDISCIPLINARY Arabian Journal of Chemistry Pub Date : 2024-10-05 DOI:10.1016/j.arabjc.2024.106009
Fang Chen, Tingting Peng, Mengjiao Gou
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引用次数: 0

摘要

癫痫是一种复杂的神经系统疾病,不仅影响个人的生活质量,而且由于需要长期服药,还阻碍了个人和国家的经济状况。癫痫的病因多种多样,神经炎症被认为是疾病进展的主要诱因和刺激因素。因此,建议使用抗炎药物来治疗癫痫发作和预防癫痫。目前可用的抗癫痫药物会产生不良反应,阻碍了这些药物的使用,而且这些药物的成本效益也不高。植物化学物质是这些药物的有效替代品,也是传统医学的处方药。科尼辛是一种甾体生物碱,存在于 Holarrhena sps 树皮提取物中,具有抗生素、止泻、抗疟和消炎特性。我们分别用 10 毫克/千克和 20 毫克/千克的海茴香碱对 PTZ 挑战动物模型进行了抗癫痫药效评估。我们观察了大鼠癫痫发作的诱导、严重程度和行为变化。通过量化脑组织中的神经递质和 ATP 酶水平,评估了鹅肌肽对 PTZ 挑战大鼠神经化学信号传导的影响。通过测量抗氧化剂和 MDA 水平,评估了鹅肌肽在癫痫诱导大鼠体内的抗氧化能力。对脑部的刺激因子和炎症细胞因子水平进行量化,以分析柯尼辛在 PTZ 挑战大鼠中的抗神经炎症功效。在实验动物的脑组织中定量检测了 AKT/mTOR 信号蛋白在癫痫发生和发展过程中的作用。对神经退行性诱导剂细胞色素 c、NF-κB、COX-2 和 Caspase 3 进行了定量分析,以评估柯尼辛对 PTZ 诱导的神经元损伤的改善作用。通过对 PTZ 挑战大鼠脑组织进行组织病理学评分,证实了科尼辛的神经保护和抗癫痫作用。科尼辛能有效抑制癫痫大鼠的癫痫发作,调节神经化学信号传导。它还能减轻 PTZ 治疗诱导的神经炎症和氧化应激。一氧化氮合酶和 AKT/mTOR 信号转导蛋白被柯尼辛有效抑制,最终防止了神经退行性变的诱导。海茴香碱能明显提高 Caspase 3 的水平。组织病理学分析证实了科尼辛的神经保护、抗炎和抗癫痫作用。科尼辛治疗也不会对大鼠造成任何行为改变,因此它是现有抗癫痫药物的安全而有效的替代品。
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Conessine alleviates PTZ-induced epilepsy in rat model via attenuating neuroinflammation and oxidative stress
Epilepsy is a complex neurological disorder which affects the quality life of individual and also hinders the economic status of both the individuals and the country since it requires prolonged medications. The etiology of epilepsy is varied and the neuroinflammation has been considered to be the prime initiator and the stimulator of the disease progression. Therefore anti-inflammatory drugs are suggested to treat seizure and also to prevent epilepsy. The currently available antiepileptic drugs cause’s adverse effects which obstructs the usage of these drugs and also these drugs are not cost effective. Phytochemicals are effective alternative to these drugs and it is prescribed in the traditional medicine. Conessine, a steroidal alkaloid present in bark extracts of Holarrhena sps possess antibiotic, anti-diarrheal, antimalarial and anti-inflammatory properties. We evaluated the antiepileptic potency of conessine in PTZ challenged animal model treated with 10 and 20 mg/kg of conessine respectively. The seizure induction, severity and the behavioral changes were observed in the rats. The impact of conessine on neurochemical signaling in PTZ challenged rats were assessed via quantifying the neurotransmitter and ATPase levels in the brain tissue. Antioxidants and MDA levels were measured to evaluate the antioxidant potency of conessine in epilepsy induced rats. iNOS and nNOS which are inducers of NO during epileptic conditions were analyzed in the test rats. The stimulators and inflammatory cytokines levels were quantified in the brain to analyze the anti-neuroinflammatory efficacy of the conessine in PTZ challenged rats. AKT/mTOR prime signaling proteins in initiation and progression of epilepsy was quantified in the brain tissue of experimental animals. Neurodegeneration inducers cytochrome c, NF-κB, COX-2 and Caspase 3 were quantified to evaluate the ameliorative potency of conessine against PTZ induced neuronal damage. The neuroprotective and antiepileptic potency of conessine was confirmed with the histopathological scoring of brain tissue in PTZ challenged rats. Conessine treatment effectively inhibited the seizure induction and regulated the neurochemical signaling in epileptic induced rats. It also attenuated the neuroinflammation and oxidative stress induction induced by PTZ treatment. The prime signaling proteins nitric oxide synthatase and AKT/mTOR signaling proteins were effectively inhibited by the conessine treatment which eventually prevented the neurodegeneration inducers. Conessine treatment significantly enhanced the levels of Caspase 3. The histopathological analysis confirms the neuroprotective, anti-inflammatory and antiepileptic potency of conessine. Conessine treatment also doesn’t caused any behavioral alterations in the rats hence it is safe and potent alternative for currently available antiepileptic drugs.
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来源期刊
Arabian Journal of Chemistry
Arabian Journal of Chemistry CHEMISTRY, MULTIDISCIPLINARY-
CiteScore
10.80
自引率
3.30%
发文量
763
审稿时长
63 days
期刊介绍: The Arabian Journal of Chemistry is an English language, peer-reviewed scholarly publication in the area of chemistry. The Arabian Journal of Chemistry publishes original papers, reviews and short reports on, but not limited to: inorganic, physical, organic, analytical and biochemistry. The Arabian Journal of Chemistry is issued by the Arab Union of Chemists and is published by King Saud University together with the Saudi Chemical Society in collaboration with Elsevier and is edited by an international group of eminent researchers.
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