Fluoxetine accelerates epileptogenesis and magnifies disease severity in a rat model of acquired epilepsy

IF 6.6 1区医学 Q1 CLINICAL NEUROLOGY Epilepsia Pub Date : 2024-08-05 DOI:10.1111/epi.18080

Gabi Dezsi, Ezgi Ozturk, Davy Wong, Matthew R. Hudson, Gabriella Martello, Flavia M. M. Gomes, Michael R. Salzberg, Margaret J. Morris, Terence J. O'Brien, Nigel C. Jones

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Abstract

Objective

Many people with epilepsy experience comorbid anxiety and depression, and antidepressants remain a primary treatment for this. Emerging evidence suggests that these agents may modulate epileptogenesis to influence disease severity. Here, we assessed how treatment with the selective serotonin reuptake inhibitor (SSRI) antidepressant fluoxetine impacts epileptogenic, behavioral, and pathological sequelae following status epilepticus.

Methods

Male Wistar rats received kainic acid to induce status epilepticus (SE) or vehicle (sham). Animals then received either fluoxetine (10 mg/kg/day) or vehicle for 8 weeks via subcutaneous osmotic pump. Video-electroencephalography was recorded continuously until behavioral testing at day 56, including assessments of anxiety- and depression-like behavior and spatial cognition. Postmortem immunocytochemistry studies examined mossy fiber sprouting.

Results

Fluoxetine treatment significantly accelerated epileptogenesis following SE, reducing the average period to the first spontaneous seizure (from 32 days [vehicle] to 6 days [fluoxetine], p < .01). Also, fluoxetine exposure magnified the severity of the resultant epilepsy, increasing seizure frequency compared to vehicle (p < .01). Exposure to fluoxetine was associated with improved anxiety- and depression-like behaviors but significantly worsened cognition. Mossy fiber sprouting was more pronounced in fluoxetine-treated rats compared to vehicle (p < .0001).

Significance

Our studies demonstrate that, using a model exhibiting spontaneous seizures, epileptogenesis is accelerated and magnified by fluoxetine, an effect that may be related to more severe pathological neuroplasticity. The differential influence of fluoxetine on behavior indicates that different circuitry and mechanisms are responsible for these comorbidities. These findings suggest that caution should be exercised when prescribing SSRI antidepressants to people at risk of developing epilepsy.

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在获得性癫痫大鼠模型中，氟西汀会加速癫痫发生并加重疾病的严重程度。

目的：许多癫痫患者会合并焦虑和抑郁，而抗抑郁药仍然是治疗这种症状的主要药物。新的证据表明，这些药物可能会调节癫痫的发生，从而影响疾病的严重程度。在此，我们评估了选择性5-羟色胺再摄取抑制剂（SSRI）抗抑郁剂氟西汀的治疗如何影响癫痫状态后的致痫、行为和病理后遗症：雄性 Wistar 大鼠接受凯尼酸诱导癫痫状态（SE）或服用药物（假）。然后，动物通过皮下渗透泵接受氟西汀（10 毫克/千克/天）或药物治疗 8 周。连续记录视频脑电图，直到第 56 天进行行为测试，包括焦虑和抑郁样行为以及空间认知的评估。死后免疫细胞化学研究检测了苔藓纤维的发芽情况：结果：氟西汀治疗明显加速了SE后的癫痫发生，缩短了首次自发癫痫发作的平均时间（从32天[车辆]到6天[氟西汀]，p 意义重大：我们的研究表明，利用自发性癫痫发作模型，氟西汀会加速和放大癫痫的发生，这种效应可能与更严重的病理性神经可塑性有关。氟西汀对行为的不同影响表明，这些合并症是由不同的回路和机制造成的。这些研究结果表明，在给有患癫痫风险的人处方 SSRI 抗抑郁药时应谨慎行事。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Epilepsia 医学-临床神经学

CiteScore

10.90

自引率

10.70%

发文量

319

审稿时长

2-4 weeks

期刊介绍： Epilepsia is the leading, authoritative source for innovative clinical and basic science research for all aspects of epilepsy and seizures. In addition, Epilepsia publishes critical reviews, opinion pieces, and guidelines that foster understanding and aim to improve the diagnosis and treatment of people with seizures and epilepsy.