Aix Marseille Univ, Inserm, MMG, Marseille, France.
Aix Marseille Univ, CNRS, INT, Marseille, France.
Epilepsia. 2022 Nov;63(11):2813-2826. doi: 10.1111/epi.17405. Epub 2022 Sep 27.
Variants in the Kv7.2 channel subunit encoded by the KCNQ2 gene cause epileptic disorders ranging from a benign form with self-limited epileptic seizures and normal development to severe forms with intractable epileptic seizures and encephalopathy. The biological mechanisms involved in these neurological diseases are still unclear. The disease remains intractable in patients affected by the severe form. Over the past 20 years, KCNQ2 models have been developed to elucidate pathological mechanisms and to identify new therapeutic targets. The diversity of Kcnq2 mouse models has proven invaluable to access neuronal networks and evaluate the associated cognitive deficits. This review summarizes the available models and their contribution to our current understanding of KCNQ2 epileptic disorders.
Kv7.2 通道亚基的变异由 KCNQ2 基因编码,可引起癫痫疾病,范围从具有自限性癫痫发作和正常发育的良性形式到具有难治性癫痫发作和脑病的严重形式。这些神经疾病涉及的生物学机制尚不清楚。严重形式的患者的疾病仍然难以治疗。在过去的 20 年中,已经开发了 KCNQ2 模型来阐明病理机制并确定新的治疗靶点。Kcnq2 小鼠模型的多样性已被证明对于访问神经元网络和评估相关认知缺陷非常有价值。本综述总结了现有的模型及其对我们目前对 KCNQ2 癫痫疾病的理解的贡献。
