Relative roles of HCN4 and synaptic excitation in pyramidal neuron firing rates in a hyperactive Rheb-mTOR condition.

IF 6.6 1区医学 Q1 CLINICAL NEUROLOGY

Epilepsia Pub Date : 2025-06-13 DOI:10.1111/epi.18456

Alexandra Pierri Chatzikalymniou, Stephanie A Getz, Youfen Xu, Dhruv R Patel, Ivan Soltesz, Angélique Bordey

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引用次数: 0

Abstract

Objective: De novo somatic mutations in mTOR pathway genes during fetal development lead to focal malformation of cortical development (FMCD) and epilepsy. This FMCD is characterized by misplacement of enlarged pyramidal neurons displaying increased mTOR activity. Whether these neurons display enhanced excitability has remained an open question. Several lines of evidence in experimental murine FMCD suggest that FMCD neurons display a complex set of alterations, including dendrite hypertrophy associated with decreased rheobase but opposing changes in excitability due to the abnormal expression of hyperpolarization-activated cyclic nucleotide-gated isoform 4 (HCN4) channels. However, there is very little information on synaptic excitatory activity and how these different alterations are integrated to shape their firing rate, particularly at the onset of seizures at approximately postnatal day 21 (P21) and after the establishment of recurrent seizures (at P28).

Methods: To address these questions, we generated FMCD by using in utero electroporation to express a constitutively active Rheb (Rheb^S16H), an mTOR canonical activator, in layer 2/3 cortical pyramidal neurons, and assessed its effects on pyramidal cell excitability at P21 and P28 using acute brain slices in vitro.

Results: At both time points, Rheb^S16H neurons exhibited cytomegaly along with increased dendritic complexity and abnormal HCN current expression. However, they displayed distinct changes in the properties of spines and excitatory postsynaptic currents (EPSCs). Specifically, there was an increase in EPSC amplitude at both ages, but whereas no change in frequency was observed at P21, a decrease in frequency was seen at P28. Experimental data-driven multicompartment single-cell computational models investigating dysmorphic neuronal excitability at P28 predicted that HCN4 channels, rather than excitatory synaptic inputs, predominantly contribute to the firing of Rheb^S16H neurons.

Significance: Overall, these experimental and computational findings advance our understanding of the mechanisms of excitability of Rheb^S16H neurons, with implications for FMCD-related seizure activity due to mTOR hyperactivity.

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HCN4和突触兴奋在过度活跃Rheb-mTOR条件下锥体神经元放电率中的相对作用。

目的：胎儿发育过程中mTOR通路基因的新生体细胞突变可导致局灶性皮质发育畸形（FMCD）和癫痫。这种FMCD的特征是锥体神经元的错位，显示mTOR活性增加。这些神经元是否表现出增强的兴奋性仍然是一个悬而未决的问题。实验小鼠FMCD的几条证据表明，FMCD神经元表现出一系列复杂的改变，包括与流变酶降低相关的树突肥大，但由于超极化激活的环核苷酸门控异构体4 （HCN4）通道异常表达而导致的兴奋性相反的变化。然而，关于突触兴奋性活动以及这些不同的改变如何整合以形成其放电速率的信息很少，特别是在大约出生后第21天（P21）癫痫发作和复发性癫痫发作后（P28）。方法：为了解决这些问题，我们利用子宫内电穿孔法在2/3层皮质锥体神经元中表达mTOR典型激活物Rheb （RhebS16H）生成FMCD，并在体外急性脑切片中评估其对P21和P28锥体细胞兴奋性的影响。结果：在两个时间点，RhebS16H神经元呈现巨细胞增生，树突复杂性增加，HCN电流表达异常。然而，它们在脊髓和兴奋性突触后电流（EPSCs）的特性上表现出明显的变化。具体来说，两个年龄的EPSC振幅都有所增加，但P21的频率没有变化，而P28的频率有所下降。实验数据驱动的多室单细胞计算模型研究了P28畸形神经元的兴奋性，预测HCN4通道，而不是兴奋性突触输入，主要促进了RhebS16H神经元的放电。意义：总的来说，这些实验和计算结果促进了我们对RhebS16H神经元兴奋性机制的理解，并对fmcd相关的癫痫发作活动产生影响。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Epilepsia 医学-临床神经学

CiteScore

10.90

自引率

10.70%

发文量

319

审稿时长

2-4 weeks

期刊介绍： Epilepsia is the leading, authoritative source for innovative clinical and basic science research for all aspects of epilepsy and seizures. In addition, Epilepsia publishes critical reviews, opinion pieces, and guidelines that foster understanding and aim to improve the diagnosis and treatment of people with seizures and epilepsy.