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Anticonvulsant and Antiepileptogenic Effects Mediated by Adeno-Associated Virus Vector Neuropeptide Y Expression in the Rat Hippocampus

机译:腺相关病毒载体神经肽Y在大鼠海马中介导的抗惊厥和抗癫痫作用

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摘要

Neuropeptide Y (NPY) inhibits seizures in experimental models and reduces excitability in human epileptic tissue. We studied the effect of long-lasting NPY overexpression in the rat hippocampus with local application of recombinant adeno-associated viral (AAV) vectors on acute kainate seizures and kindling epileptogenesis.Transgene expression was significantly increased by 7 d, reached maximal expression by 2 weeks, and persisted for at least 3 months. Serotype 2 AAV vector increased NPY expression in hilar interneurons, whereas the chimeric serotype 1/2 vector caused far more widespread expression, also including mossy fibers, pyramidal cells, and the subiculum. EEG seizures induced by intrahippocampal kainate were reduced by 50–75%, depending on the vector serotype, and seizure onset was markedly delayed.In rats injected with the chimeric serotype 1/2 vector, status epilepticus was abolished, and kindling acquisition was significantly delayed. Thus, targeted NPY gene transfer provides a potential therapeutic principle for the treatment of drug-resistant partial epilepsies.
机译:神经肽Y(NPY)在实验模型中抑制癫痫发作,并降低人类癫痫组织的兴奋性。我们研究了局部应用重组腺相关病毒(AAV)载体对大鼠海马长效NPY过度表达对急性海藻酸盐发作和点燃癫痫发生的影响。转基因表达在7 d时显着增加,在2周时达到最大表达,并持续至少3个月。血清型2 AAV载体增加了肺门中神经元中NPY的表达,而嵌合的血清型1/2载体引起了更广泛的表达,还包括苔藓纤维,锥体细胞和下丘脑。根据载体的血清型,海马内海藻酸盐诱发的脑电图发作减少了50-75%,癫痫发作明显延迟。在注射嵌合型1/2血清型载体的大鼠中,癫痫持续状态被取消,点燃获得明显延迟。因此,靶向NPY基因转移为耐药性部分癫痫的治疗提供了潜在的治疗原理。

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