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一种新型吲哚相关化合物对小鼠海人酸诱导的癫痫持续状态的抗惊厥作用:抗氧化和抗炎机制的作用

The Anticonvulsant Effect of a Novel Indole-Related Compound in the Kainate-Induced Status Epilepticus in Mice: The Role of the Antioxidant and Anti-inflammatory Mechanism.

作者信息

Tchekalarova Jana, Stoyanova Tsveta, Tzoneva Rumiana, Angelova Violina, Andreeva-Gateva Pavlina

机构信息

Institute of Neurobiology, Bulgarian Academy of Sciences, Acad. G. Bonchev Str., Bl. 23, 1113, Sofia, Bulgaria.

Institute of Biophysics and Biomedical Engineering, BAS, Sofia, Bulgaria.

出版信息

Neurochem Res. 2022 Feb;47(2):327-334. doi: 10.1007/s11064-021-03447-2. Epub 2021 Sep 12.

DOI:10.1007/s11064-021-03447-2
PMID:34510375
Abstract

We synthesized a series of novel indole compounds containing aroylhydrazone moieties and evaluated them in mice to check their anticonvulsant activity. In the present study the most potent C3-modified derivative 3e, containing 2-furyl fragment was evaluated in kainate (KA)-induced status epilepticus (SE) and the consequences on oxidative stress and inflammation in the hippocampus in mice were explored. Melatonin was used as positive control while the melatonin receptor antagonist Luzindol was studied alone or in combination with melatonin or 3e, respectively. After intraperitoneal (i.p.) pre-treatment with melatonin 3e, Luzindol + melatonin and Luzindol + 3e for 7 days (melatonin and 3e-30 mg kg or 60 mg kg, Luzindol 10 mg kg) the animals were i.p. injected with KA (30 mg kg, i.p.). The 3e decreased the SE-induced seizure intensity while melatonin suppressed seizures at the higher dose of 60 mg kg. Luzindol blocked the anticonvulsant effect of both Mel and 3e. The dose-dependent antioxidant effect of 3e measured by reduced glutathione (GSH) and total GSH in the hippocampus, was comparable to the effect of melatonin. Luzindol fully blocked the effect of melatonin but affected partially the antioxidant activity of 3e. The KA-induced increased amplifier of neuroinflammation high-mobility group box protein 1 (HMGB1) was neither alleviated by melatonin, nor by 3e. The activation by this DNA-binding protein receptor for advanced glycation end products (RAGE) was not affected by SE, melatonin and 3e pre-treatment. Our results suggest that the novel indole derivate 3e, containing 2-furyl fragment, might be clinically useful as an adjunct therapy against SE and concomitant oxidative stress.

摘要

我们合成了一系列含有芳酰腙部分的新型吲哚化合物,并在小鼠中对其进行评估以检查它们的抗惊厥活性。在本研究中,对含有2-呋喃基片段的最有效的C3修饰衍生物3e在海藻酸(KA)诱导的癫痫持续状态(SE)中进行了评估,并探讨了其对小鼠海马氧化应激和炎症的影响。褪黑素用作阳性对照,而褪黑素受体拮抗剂鲁辛朵单独使用或分别与褪黑素或3e联合使用进行研究。在腹腔内(i.p.)用褪黑素3e、鲁辛朵+褪黑素和鲁辛朵+3e预处理7天(褪黑素和3e - 30mg/kg或60mg/kg,鲁辛朵10mg/kg)后,动物腹腔内注射KA(30mg/kg,i.p.)。3e降低了SE诱导的癫痫发作强度,而褪黑素在60mg/kg的较高剂量下抑制了癫痫发作。鲁辛朵阻断了Mel和3e的抗惊厥作用。通过海马中还原型谷胱甘肽(GSH)和总GSH测量的3e的剂量依赖性抗氧化作用与褪黑素的作用相当。鲁辛朵完全阻断了褪黑素的作用,但部分影响了3e的抗氧化活性。KA诱导的神经炎症增强子高迁移率族蛋白1(HMGB1)的增加既未被褪黑素也未被3e缓解。这种晚期糖基化终产物(RAGE)的DNA结合蛋白受体的激活不受SE、褪黑素和3e预处理的影响。我们的结果表明,含有2-呋喃基片段的新型吲哚衍生物3e可能作为治疗SE及伴随氧化应激的辅助疗法具有临床应用价值。

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本文引用的文献

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Discovery of novel indole-based aroylhydrazones as anticonvulsants: Pharmacophore-based design.新型吲哚基芳酰腙类化合物的发现及其作为抗惊厥药物的研究:基于药效团的设计。
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褪黑素与多发性硬化症:从神经药理学作用机制的推测到实验和临床证据。
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Pharmacol Biochem Behav. 2013 Oct;111:44-50. doi: 10.1016/j.pbb.2013.08.006. Epub 2013 Aug 24.