Ottolini Matteo, Barker Bryan S, Gaykema Ronald P, Meisler Miriam H, Patel Manoj K
Department of Anesthesiology and.
Neuroscience Graduate Program, University of Virginia Health System, Charlottesville, Virginia 22908, and.
J Neurosci. 2017 Aug 9;37(32):7643-7655. doi: 10.1523/JNEUROSCI.2709-16.2017. Epub 2017 Jul 4.
encephalopathy, or early infantile epileptic encephalopathy 13 (EIEE13), is caused predominantly by gain-of-function mutations in the voltage-gated Na channel Na1.6. Affected individuals suffer from refractory seizures, developmental delay, cognitive disability, and elevated risk of sudden unexpected death in epilepsy (SUDEP). A knock-in mouse model carrying the patient mutation p.Asn1768Asp (N1768D) reproduces many features of the disorder, including spontaneous seizures and SUDEP. We used the mouse model to examine the effects of the mutation on layer II stellate neurons of the medial entorhinal cortex (mEC), which transmit excitatory input to the hippocampus. Heterozygous (), homozygous (), and WT () littermates were compared at 3 weeks of age, the time of seizure onset for homozygous mice. Heterozygotes remain seizure free for another month. mEC layer II neurons of heterozygous and homozygous mice were hyperexcitable and generated long-lasting depolarizing potentials with bursts of action potentials after synaptic stimulation. Recording of Na currents revealed proexcitatory increases in persistent and resurgent currents and rightward shifts in inactivation parameters, leading to significant increases in the magnitude of window currents. The proexcitatory changes were more pronounced in homozygous mice than in heterozygotes, consistent with the earlier age of seizure onset in homozygotes. These studies demonstrate that the N1768D mutation increases the excitability of mEC layer II neurons by increasing persistent and resurgent Na currents and disrupting channel inactivation. The aberrant activities of mEC layer II neurons would provide excessive excitatory input to the hippocampus and contribute to hyperexcitability of hippocampal neurons in this model of encephalopathy. encephalopathy is a devastating neurological disorder that results from mutations in the Na channel Na1.6. In addition to seizures, patients suffer from cognitive and developmental delays and are at high risk for sudden unexpected death in epilepsy (SUDEP). A mouse knock-in model expressing the patient mutation N1768D reproduces several pathological phenotypes, including spontaneous seizures and sudden death. We demonstrate that medial entorhinal cortex (mEC) neurons from the mouse model exhibit proexcitatory alterations in Na channel activity, some of which were not seen in hippocampal or cortical neurons, and resulting in neuronal hyperexcitability. Because mEC neurons regulate the activity of the hippocampus, which plays an important role in seizure onset, we propose that these profound changes in mEC neuron excitability associated with the gain-of-function mutation of Na1.6 may increase excitatory drive into the hippocampus, culminating in seizure activity and SUDEP.
脑病,即早发性婴儿癫痫性脑病13型(EIEE13),主要由电压门控钠通道Na1.6的功能获得性突变引起。受影响个体患有难治性癫痫发作、发育迟缓、认知障碍以及癫痫猝死(SUDEP)风险升高。携带患者突变p.Asn1768Asp(N1768D)的基因敲入小鼠模型重现了该疾病的许多特征,包括自发性癫痫发作和SUDEP。我们使用该小鼠模型研究该突变对内侧内嗅皮质(mEC)II层星状神经元的影响,这些神经元向海马体传递兴奋性输入。在3周龄时比较杂合子()、纯合子()和野生型()同窝小鼠,此时是纯合子小鼠癫痫发作开始的时间。杂合子在接下来的一个月内仍无癫痫发作。杂合子和纯合子小鼠的mEC II层神经元兴奋性过高,在突触刺激后产生带有动作电位爆发的持久去极化电位。钠电流记录显示持续性和复苏性电流出现促兴奋性增加,失活参数向右偏移,导致窗电流幅度显著增加。纯合子小鼠中的促兴奋性变化比杂合子更明显,这与纯合子癫痫发作开始的年龄更早一致。这些研究表明,N1768D突变通过增加持续性和复苏性钠电流以及破坏通道失活来增加mEC II层神经元的兴奋性。mEC II层神经元的异常活动会向海马体提供过多的兴奋性输入,并导致该脑病模型中海马体神经元的兴奋性过高。脑病是一种由钠通道Na1.6突变引起的毁灭性神经系统疾病。除癫痫发作外,患者还患有认知和发育迟缓,并且癫痫猝死(SUDEP)风险很高。表达患者突变N1768D的小鼠基因敲入模型重现了几种病理表型,包括自发性癫痫发作和猝死。我们证明,来自该小鼠模型的内侧内嗅皮质(mEC)神经元在钠通道活性方面表现出促兴奋性改变,其中一些在海马体或皮质神经元中未观察到,从而导致神经元兴奋性过高。由于mEC神经元调节海马体的活动,而海马体在癫痫发作起始中起重要作用,我们提出,与Na1.6功能获得性突变相关的mEC神经元兴奋性的这些深刻变化可能会增加进入海马体的兴奋性驱动,最终导致癫痫发作活动和SUDEP。
