Noé Francesco, Frasca Angelisa, Balducci Claudia, Carli Mirjana, Sperk Gunther, Ferraguti Francesco, Pitkänen Asla, Bland Ross, Fitzsimons Helen, During Matthew, Vezzani Annamaria
Department of Neuroscience, Mario Negri Institute for Pharmacological Research, Milano 20156, Italy.
Neurotherapeutics. 2009 Apr;6(2):300-6. doi: 10.1016/j.nurt.2009.01.012.
Gene therapy may represent a promising alternative treatment of epileptic patients who are resistant to conventional anti-epileptic drugs. Among the various approaches for the application of gene therapy in the treatment of CNS disorders, recombinant adeno-associated viral (AAV) vectors have been most widely used. Preclinical studies using a selection of "therapeutic" genes injected into the rodent brain to correct the compromised balance between inhibitory and excitatory transmission in epilepsy, showed significant reduction of seizures and inhibition of epileptogenesis. In particular, transduction of neuropeptide genes, such as galanin and neuropeptide Y (NPY) in specific brain areas in experimental models of seizures resulted in significant anticonvulsant effects. Recent findings showed a long-lasting NPY over-expression in the rat hippocampus by local application of recombinant AAV vectors associated with reduced generalization of seizures, delayed kindling epileptogenesis, and strong reduction of chronic spontaneous seizures. These results establish a proof-of-principle evidence of the efficacy of gene therapy as anticonvulsant treatment. Additional investigations are required to address safety concerns and possible side effects in more detail.
基因治疗可能是对传统抗癫痫药物耐药的癫痫患者一种有前景的替代治疗方法。在基因治疗应用于中枢神经系统疾病治疗的各种方法中,重组腺相关病毒(AAV)载体应用最为广泛。临床前研究通过向啮齿动物脑内注射一系列“治疗性”基因来纠正癫痫中抑制性和兴奋性传递之间受损的平衡,结果显示癫痫发作显著减少且癫痫发生受到抑制。特别是,在癫痫实验模型的特定脑区转导神经肽基因,如甘丙肽和神经肽Y(NPY),产生了显著的抗惊厥作用。最近的研究结果表明,通过局部应用重组AAV载体,大鼠海马中NPY长期过度表达,这与癫痫发作泛化减少、点燃性癫痫发生延迟以及慢性自发性癫痫发作强烈减少有关。这些结果为基因治疗作为抗惊厥治疗的有效性建立了原理验证证据。还需要进一步研究以更详细地解决安全性问题和可能的副作用。