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具有新型SCN2A变体的人类皮质类器官表现出过度兴奋性以及对抗癫痫化合物的不同反应。

Human Cortical Organoids with a Novel SCN2A Variant Exhibit Hyperexcitability and Differential Responses to Anti-Seizure Compounds.

作者信息

Yang Yuling, Cai Yang, Wang Shuyang, Wu Xiaoling, Shao Zhicheng, Wang Xin, Ding Jing

机构信息

Department of Neurology, Zhongshan Hospital, Fudan University, Shanghai, 200032, China.

Department of Neurology, Zhongshan Hospital, Institute for Translational Brain Research, State Key Laboratory of Brain Function and Disorders, MOE Frontiers Center for Brain Science, Fudan University, Shanghai, 200032, China.

出版信息

Neurosci Bull. 2025 Jun 20. doi: 10.1007/s12264-025-01429-w.

Abstract

Mutations in ion channel genes have long been implicated in a spectrum of epilepsy syndromes. However, therapeutic decision-making is relatively complex for epilepsies associated with channelopathy. Therefore, in the present study, we used a patient-derived organoid model with a novel SCN2A mutation (p.E512K) to investigate the potential of utilizing such a model as a platform for preclinical testing of anti-seizure compounds. The electrophysiological properties of the variant Nav1.2 exhibited gain-of-function effects with increased current amplitude and premature activation. Immunofluorescence staining of patient-derived cortical organoids (COs) displayed normal neurodevelopment. Multielectrode array (MEA) recordings of patient-derived COs showed hyperexcitability with increased spiking and remarkable network bursts. Moreover, the application of patient-derived COs for preclinical drug testing using the MEA showed that they exhibit differential responses to various anti-seizure drugs and respond well to carbamazepine. Our results demonstrate that the individualized organoids have the potential to serve as a platform for preclinical pharmacological assessment.

摘要

长期以来,离子通道基因突变一直与一系列癫痫综合征有关。然而,对于与通道病相关的癫痫,治疗决策相对复杂。因此,在本研究中,我们使用了一种具有新型SCN2A突变(p.E512K)的患者来源类器官模型,以研究利用这种模型作为抗癫痫化合物临床前测试平台的潜力。变异型Nav1.2的电生理特性表现出功能增强效应,电流幅度增加且激活提前。患者来源的皮质类器官(COs)的免疫荧光染色显示神经发育正常。患者来源的COs的多电极阵列(MEA)记录显示兴奋性过高,尖峰增加且有明显的网络爆发。此外,使用MEA将患者来源的COs应用于临床前药物测试表明,它们对各种抗癫痫药物表现出不同的反应,且对卡马西平反应良好。我们的结果表明,个体化类器官有潜力作为临床前药理学评估的平台。

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