Novel mouse model of alternating hemiplegia of childhood exhibits prominent motor and seizure phenotypes.

IF 5.1 2区 医学 Q1 NEUROSCIENCES Neurobiology of Disease Pub Date : 2024-11-25 DOI:10.1016/j.nbd.2024.106751
Nicole A Hawkins, Jean-Marc DeKeyser, Jennifer A Kearney, Alfred L George
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Abstract

Pathogenic variants in ATP1A3 encoding the neuronal Na/K-ATPase cause a spectrum of neurodevelopmental disorders including alternating hemiplegia of childhood (AHC). Three recurrent ATP1A3 variants are associated with approximately half of known AHC cases and mouse models of two of these variants (p.D801N, p.E815K) replicated key features of the human disorder, which include paroxysmal hemiplegia, dystonia and seizures. Epilepsy occurs in 40-50 % of individuals affected with AHC, but detailed investigations of seizure phenotypes were limited in the previously reported mouse models. Using gene editing, we generated a novel AHC mouse expressing the third most recurrent ATP1A3 variant (p.G947R) to model neurological phenotypes of the disorder. Heterozygous Atp1a3-G947R (Atp1a3G947R) mice on a pure C57BL/6 J background were born at a significantly lower frequency than wildtype (WT) littermates, but in vitro fertilization or outcrossing to a different strain (C3HeB/FeJ) generated offspring at near-Mendelian genotype ratios, suggesting a defect in reproductive fitness rather than embryonic lethality. Heterozygous mutant mice were noticeably smaller and exhibited premature lethality, hyperactivity, anxiety-like behaviors, severe motor dysfunction including low grip strength, impaired coordination with abnormal gait and balance, reduced REM sleep, and cooling-induced hemiplegia and dystonia. We also observed a prominent seizure phenotype with lower thresholds to chemically (flurothyl, kainic acid) and electrically induced seizures, post-handling seizures, sudden death following seizures, and abnormal EEG activity. Together, our findings support face validity of a novel AHC mouse model with quantifiable traits including co-morbid epilepsy that will be useful as an in vivo platform for investigating pathophysiology and testing new therapeutic strategies for this rare neurodevelopmental disorder.

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儿童交替性偏瘫的新型小鼠模型表现出突出的运动和癫痫表型。
编码神经元 Na/K-ATP 酶的 ATP1A3 的致病变体可导致一系列神经发育障碍,包括儿童交替性偏瘫(AHC)。在已知的儿童交替性偏瘫病例中,约有一半与三个复发性 ATP1A3 变异有关,其中两个变体(p.D801N 和 p.E815K)的小鼠模型复制了人类疾病的主要特征,包括阵发性偏瘫、肌张力障碍和癫痫发作。40%-50%的 AHC 患者会出现癫痫,但在以前报道的小鼠模型中,对癫痫发作表型的详细研究非常有限。我们利用基因编辑技术生成了一种新型 AHC 小鼠,该小鼠表达了第三种最常见的 ATP1A3 变体(p.G947R),可模拟该疾病的神经表型。纯合C57BL/6 J背景的杂合子Atp1a3-G947R(Atp1a3G947R)小鼠的出生率明显低于野生型(WT)同胎仔鼠,但体外受精或与不同品系(C3HeB/FeJ)杂交产生的后代的基因型比例接近孟德尔基因型比例,这表明小鼠的生殖能力存在缺陷,而不是胚胎致死。杂合子突变体小鼠的体型明显较小,并表现出过早致死、多动、焦虑样行为、严重的运动功能障碍(包括低握力)、步态和平衡异常的协调性受损、快速眼动睡眠减少以及冷却诱发的偏瘫和肌张力障碍。我们还观察到一种突出的癫痫表型,对化学(氟乙酰、凯因酸)和电诱导癫痫发作、处理后癫痫发作、癫痫发作后猝死和异常脑电图活动的阈值较低。总之,我们的研究结果证明了新型 AHC 小鼠模型的有效性,该模型具有可量化的特征,包括合并癫痫,可作为研究这种罕见神经发育障碍的病理生理学和测试新治疗策略的体内平台。
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来源期刊
Neurobiology of Disease
Neurobiology of Disease 医学-神经科学
CiteScore
11.20
自引率
3.30%
发文量
270
审稿时长
76 days
期刊介绍: Neurobiology of Disease is a major international journal at the interface between basic and clinical neuroscience. The journal provides a forum for the publication of top quality research papers on: molecular and cellular definitions of disease mechanisms, the neural systems and underpinning behavioral disorders, the genetics of inherited neurological and psychiatric diseases, nervous system aging, and findings relevant to the development of new therapies.
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