Sex differences in seizure presentation in a Dravet syndrome mouse model.

IF 1.6 4区医学 Q4 NEUROSCIENCES

Neuroreport Pub Date : 2025-05-14 Epub Date: 2025-04-01 DOI:10.1097/WNR.0000000000002159

Sheryl Anne D Vermudez, Rui Lin, Gabrielle E McGinty, Yongho Choe, Amanda Liebhardt, Benjamin Hui, Ella Lubbers, Sameer C Dhamne, Mustafa Q Hameed, Alexander Rotenberg

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引用次数: 0

Abstract

Objectives: Dravet syndrome is an epileptic encephalopathy mostly because of haploinsufficiency of the SCN1A voltage-gated sodium channel subunit. Disease presentation (i.e. severe seizures and early life mortality) is faithfully modeled in mice haploinsufficient in Scn1a ( Scn1a+/ - ). However, the characterization of sex differences in mortality and seizure morbidity is limited. Given the reliance of mouse models for studying disease pathophysiology and for the development of novel treatments, we tested whether disease presentation differed in juvenile and adult female and male Scn1a+/ - mice.

Methods: Mortality and seizure morbidity were quantified in juvenile and adult female and male Scn1a+/ - animals on an F1 hybrid C57 × 129S6 background.

Results: Mortality was significantly higher in female Scn1a+/ - mice compared with males regardless of age, and juvenile female Scn1a+/ - mice had a significantly lower febrile seizure threshold than age-matched Scn1a+/ - males. Conversely, long-term video EEG recordings revealed that adult male Scn1a+/ - mice had significantly more frequent and longer spontaneous seizures than adult females. Adult female Scn1a+/- mice, however, were significantly more hyperactive, which may indicate sleep impairment.

Conclusion: The phenotypic presentation of Scn1a+/ - mice is sex-dependent which may have translational implications for understanding basic pathophysiological mechanisms as well as therapeutic drug discovery in Dravet syndrome.

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Dravet综合征小鼠模型中癫痫表现的性别差异。

目的：Dravet综合征是一种癫痫性脑病，主要原因是SCN1A电压门控钠通道亚基单倍性不足。疾病表现（即严重癫痫发作和早期生命死亡）忠实地模拟了Scn1a （Scn1a+/-）单倍不足的小鼠。然而，死亡率和癫痫发病率的性别差异的特征是有限的。考虑到研究疾病病理生理和开发新治疗方法的小鼠模型的依赖性，我们测试了幼年和成年雌性和雄性Scn1a+/-小鼠的疾病表现是否不同。方法：以F1杂交C57 × 129S6为背景，对Scn1a+/-雌、雄幼鼠和成年鼠的死亡率和癫痫发病率进行量化分析。结果：无论年龄大小，雌性Scn1a+/-小鼠的死亡率都明显高于雄性，幼年雌性Scn1a+/-小鼠的热发作阈值明显低于与年龄匹配的雄性Scn1a+/-小鼠。相反，长期视频脑电图记录显示，成年雄性Scn1a+/-小鼠比成年雌性自发性癫痫发作的频率和时间明显更长。然而，成年雌性Scn1a+/-小鼠明显更加活跃，这可能表明睡眠障碍。结论：Scn1a+/-小鼠的表型表现是性别依赖的，这可能对理解Dravet综合征的基本病理生理机制和治疗药物的发现具有翻译意义。

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

Neuroreport 医学-神经科学

CiteScore

3.20

自引率

0.00%

发文量

150

审稿时长

1 months

期刊介绍： NeuroReport is a channel for rapid communication of new findings in neuroscience. It is a forum for the publication of short but complete reports of important studies that require very fast publication. Papers are accepted on the basis of the novelty of their finding, on their significance for neuroscience and on a clear need for rapid publication. Preliminary communications are not suitable for the Journal. Submitted articles undergo a preliminary review by the editor. Some articles may be returned to authors without further consideration. Those being considered for publication will undergo further assessment and peer-review by the editors and those invited to do so from a reviewer pool. The core interest of the Journal is on studies that cast light on how the brain (and the whole of the nervous system) works. We aim to give authors a decision on their submission within 2-5 weeks, and all accepted articles appear in the next issue to press.