Department of Clinical Pharmacology, Hunan Key Laboratory of Pharmacogenetics, National Clinical Research Center for Geriatric Disorders, Xiangya Hospital, Central South University, Changsha, P.R. China.
Hunan Cancer Hospital, The Affiliated Cancer Hospital of Xiangya School of Medicine, Central South University, Changsha, P.R. China.
CNS Neurosci Ther. 2024 Aug;30(8):e14911. doi: 10.1111/cns.14911.
Epilepsy is a widespread central nervous system disorder with an estimated 50 million people affected globally. It is characterized by a bimodal incidence peak among infants and the elderly and is influenced by a variety of risk factors, including a significant genetic component. Despite the use of anti-epileptic drugs (AEDs), drug-refractory epilepsy develops in about one-third of patients, highlighting the need for alternative therapeutic approaches.
The primary aim of this study was to evaluate the neuroprotective effects of troglitazone (TGZ) in epilepsy and to explore the potential mechanisms underlying its action.
We employed both in vitro and in vivo models to assess TGZ's effects. The in vitro model involved glutamate-induced toxicity in HT22 mouse hippocampal neurons, while the in vivo model used kainic acid (KA) to induce epilepsy in mice. A range of methods, including Hoechst/PI staining, CCK-8 assay, flow cytometry, RT-PCR analysis, Nissl staining, scanning electron microscopy, and RNA sequencing, were utilized to assess various parameters such as cellular damage, viability, lipid-ROS levels, mitochondrial membrane potential, mRNA expression, seizure grade, and mitochondrial morphology.
Our results indicate that TGZ, at doses of 5 or 20 mg/kg/day, significantly reduces KA-induced seizures and neuronal damage in mice by inhibiting the process of ferroptosis. Furthermore, TGZ was found to prevent changes in mitochondrial morphology. In the glutamate-induced HT22 cell damage model, 2.5 μM TGZ effectively suppressed neuronal ferroptosis, as shown by a reduction in lipid-ROS accumulation, a decrease in mitochondrial membrane potential, and an increase in PTGS2 expression. The anti-ferroptotic effect of TGZ was confirmed in an erastin-induced HT22 cell damage model as well. Additionally, TGZ reversed the upregulation of Plaur expression in HT22 cells treated with glutamate or erastin. The downregulation of Plaur expression was found to alleviate seizures and reduce neuronal damage in the mouse hippocampus.
This study demonstrates that troglitazone has significant therapeutic potential in the treatment of epilepsy by reducing epileptic seizures and the associated brain damage through the inhibition of neuronal ferroptosis. The downregulation of Plaur expression plays a crucial role in TGZ's anti-ferroptotic effect, offering a promising avenue for the development of new epilepsy treatments.
癫痫是一种广泛存在的中枢神经系统疾病,全球估计有 5000 万人受其影响。它的发病高峰呈双峰分布,分别在婴儿和老年人中出现,受多种风险因素影响,其中包括重要的遗传因素。尽管使用了抗癫痫药物(AEDs),但仍有约三分之一的患者出现药物难治性癫痫,这突显了需要替代治疗方法的必要性。
本研究的主要目的是评估曲格列酮(TGZ)在癫痫中的神经保护作用,并探讨其作用的潜在机制。
我们采用了体内和体外模型来评估 TGZ 的作用。体外模型涉及谷氨酸诱导的 HT22 小鼠海马神经元毒性,而体内模型则使用海人酸(KA)诱导小鼠癫痫。我们使用了一系列方法,包括 Hoechst/PI 染色、CCK-8 测定、流式细胞术、RT-PCR 分析、尼氏染色、扫描电子显微镜和 RNA 测序,来评估细胞损伤、活力、脂质-ROS 水平、线粒体膜电位、mRNA 表达、癫痫发作程度和线粒体形态等各种参数。
我们的结果表明,TGZ 以 5 或 20mg/kg/天的剂量给药,可通过抑制铁死亡过程显著减轻 KA 诱导的癫痫发作和小鼠神经元损伤。此外,TGZ 被发现可防止线粒体形态的改变。在谷氨酸诱导的 HT22 细胞损伤模型中,2.5μM TGZ 有效抑制神经元铁死亡,表现为脂质-ROS 积累减少、线粒体膜电位降低和 PTGS2 表达增加。在 erastin 诱导的 HT22 细胞损伤模型中也证实了 TGZ 的抗铁死亡作用。此外,TGZ 逆转了谷氨酸或 erastin 处理的 HT22 细胞中 Plaur 表达的上调。下调 Plaur 表达可减轻小鼠海马中的癫痫发作并减少神经元损伤。
本研究表明,曲格列酮通过抑制神经元铁死亡,减少癫痫发作和相关的脑损伤,在治疗癫痫方面具有显著的治疗潜力。Plaur 表达的下调在 TGZ 的抗铁死亡作用中发挥关键作用,为开发新的癫痫治疗方法提供了有希望的途径。
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