Depression represents one of the most common comorbidities in patients with epilepsy. However, the mechanisms of depression in epilepsy patients are poorly understood. Establishment of animal models of this comorbidity is critical for both understanding the mechanisms of the condition, and for preclinical development of effective therapies. The current study examined whether a commonly used animal model of temporal lobe epilepsy (TLE) is characterized by behavioural and biochemical alterations involved in depression. Male Wistar rats were subjected to LiCl and pilocarpine status epilepticus (SE). The development of chronic epileptic state was confirmed by the presence of spontaneous seizures and by enhanced brain excitability. Post-SE animals exhibited increase in immobility time under conditions of forced swim test (FST) which was indicative of despair-like state, and loss of taste preference in saccharin solution consumption test which pointed to the symptomatic equivalence of anhedonia. Biochemical studies revealed compromised serotonergic transmission in the raphe-hippocampal serotonergic pathway: decrease of serotonin (5-HT) concentration and turnover in the hippocampus, measured by high performance liquid chromatography, and decrease of 5-HT release from the hippocampus in response to raphe stimulation, measured by fast cyclic voltammetry. Administration of fluoxetine (FLX, 20 mg/kg/day for 10 days) to naive animals significantly shortened immobility time under conditions of FST, and inhibited 5-HT turnover in the hippocampus. In post-SE rats FLX treatment led to a further decrease of hippocampal 5-HT turnover; however, performance in FST was not improved. At the same time, FLX reversed SE-induced increase in brain excitability. In summary, our studies provide initial evidence that post-SE model of TLE might serve as a model of the comorbidity of epilepsy and depression. The finding that behavioural equivalents of depression were resistant to an antidepressant medication suggested that depression in epilepsy might have distinct underlying mechanisms beyond alterations in serotonergic pathways.
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机译:抑郁症是癫痫患者最常见的合并症之一。然而,对癫痫患者抑郁的机制了解甚少。建立这种合并症的动物模型对于理解病情的机制和有效疗法的临床前开发都至关重要。本研究检查了颞叶癫痫(TLE)的常用动物模型是否具有与抑郁有关的行为和生化改变的特征。对雄性Wistar大鼠进行LiCl和毛果芸香碱癫痫持续状态(SE)。慢性癫痫状态的发展被自然发作和脑兴奋性增强所证实。 SE后的动物在强迫游泳试验(FST)的条件下表现出不动时间的增加,这表明处于绝望状态,在糖精溶液消耗试验中味觉偏好的丧失表明了快感缺乏症的对等症状。生化研究表明,在裂谷-海马血清素能途径中的血清素能传递受到损害:通过高效液相色谱法测定,海马中5-羟色胺(5-HT)浓度和周转率的降低,以及对裂殖剂响应后海马中5-HT释放的降低刺激,通过快速循环伏安法测量。给幼稚动物服用氟西汀(FLX,20 mg / kg /天,持续10天)可显着缩短FST条件下的固定时间,并抑制海马体中的5-HT转换。在SE后大鼠中,FLX治疗导致海马5-HT周转率进一步降低。但是,FST的性能没有提高。同时,FLX逆转了SE诱导的大脑兴奋性增加。总而言之,我们的研究提供了初步的证据,证明TLE的SE后模型可作为癫痫和抑郁症合并症的模型。抑郁的行为等效对抗抑郁药有抗性的发现表明,癫痫病的抑郁可能具有除血清素能途径改变之外的独特潜在机制。
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