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Optogenetic control of epileptiform activity

机译:癫痫样活动的光遗传学控制

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摘要

The optogenetic approach to gain control over neuronal excitability both in vitro and in vivo has emerged as a fascinating scientific tool to explore neuronal networks, but it also opens possibilities for developing novel treatment strategies for neurologic conditions. We have explored whether such an optogenetic approach using the light-driven halorhodopsin chloride pump from Natronomonas pharaonis (NpHR), modified for mammalian CNS expression to hy-perpolarize central neurons, may inhibit excessive hyperexcitability and epileptiform activity. We show that a lentiviral vector containing the NpHR gene under the calcium/calmodulin-dependent protein kinase llα promoter transduces principal cells of the hippocampus and cortex and hyperpolarizes these cells, preventing generation of action potentials and epileptiform activity during optical stimulation. This study proves a principle, that selective hyperpolarization of principal cortical neurons by NpHR is sufficient to curtail paroxysmal activity in transduced neurons and can inhibit stimulation train-induced bursting in hippocampal organotypic slice cultures, which represents a model tissue of pharmacoresistant epilepsy. This study demonstrates that the optogenetic approach may prove useful for controlling epileptiform activity and opens a future perspective to develop it into a strategy to treat epilepsy.
机译:在体外和体内获得对神经元兴奋性的控制的光遗传学方法已经成为探索神经元网络的一种有趣的科学工具,但是它也为开发新的神经系统疾病治疗策略提供了可能性。我们已经研究了使用来自Natronomonas pharaonis(NpHR)的光驱动卤代视紫红质泵(针对哺乳动物CNS表达修饰为超极化中枢神经元)的这种光遗传学方法是否可能抑制过度的过度兴奋性和癫痫样活动。我们显示慢病毒载体包含钙/钙调蛋白依赖性蛋白激酶llα启动子下的NpHR基因转导海马和皮层的主要细胞,并使这些细胞超极化,从而防止了光刺激过程中动作电位和癫痫样活动的产生。这项研究证明了一个原理,即通过NpHR对主要皮层神经元进行选择性超极化足以抑制转导的神经元的阵发性活动,并可以抑制刺激火车诱导的海马器官型切片培养物中的爆发,这代表了药物耐药性癫痫的模型组织。这项研究表明,光遗传学方法可能被证明可用于控制癫痫样活动,并为将其发展为治疗癫痫的策略打开了未来的前景。

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