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在Dravet综合征小鼠模型中,内侧隔区表达小白蛋白的抑制性神经元受损。

Medial septum parvalbumin-expressing inhibitory neurons are impaired in a mouse model of Dravet Syndrome.

作者信息

Zhu Limei, Demetriou Yiannos, Barden Joseph, Disla Juan, Mattis Joanna

出版信息

bioRxiv. 2024 Oct 31:2024.10.29.620933. doi: 10.1101/2024.10.29.620933.

Abstract

Dravet syndrome (DS) is a severe neurodevelopmental disorder caused by pathogenic variants in the gene, which encodes the voltage-gated sodium channel Na 1.1 α subunit. Experiments in animal models of DS - including the haploinsufficient mouse - have identified impaired excitability of interneurons in the hippocampus and neocortex; this is thought to underlie the treatment-resistant epilepsy that is a prominent feature of the DS phenotype. However, additional brain structures, such as the medial septum (MS), also express . The medial septum is known to play an important role in cognitive function and thus may contribute to the intellectual impairment that also characterizes DS. In this study, we employed whole cell patch clamp recordings in acute brain slices to characterize the electrophysiological properties of MS neurons in mice versus age-matched wild-type littermate controls. We found no discernible genotype-related differences in MS cholinergic (ChAT) neurons, but significant dysfunction within MS parvalbumin-expressing (PV) inhibitory neurons in mice. We further identified heterogeneity of firing patterns among MS PV neurons, and additional genotype differences in the proportion of subtype representation. These results confirm that the MS is an additional locus of pathology in DS, that may contribute to co- morbidities such as cognitive impairment.

摘要

德拉韦特综合征(DS)是一种严重的神经发育障碍,由编码电压门控钠通道Na 1.1α亚基的基因中的致病变异引起。在DS动物模型(包括单倍体不足的小鼠)中的实验已经确定海马体和新皮质中中间神经元的兴奋性受损;这被认为是DS表型的一个突出特征——难治性癫痫的基础。然而,其他脑结构,如内侧隔区(MS),也表达 。已知内侧隔区在认知功能中起重要作用,因此可能导致DS所特有的智力障碍。在本研究中,我们在急性脑片中采用全细胞膜片钳记录来表征 小鼠与年龄匹配的野生型同窝对照小鼠中内侧隔区神经元的电生理特性。我们发现内侧隔区胆碱能(ChAT)神经元中没有明显的基因型相关差异,但 小鼠内侧隔区表达小白蛋白(PV)的抑制性神经元存在明显功能障碍。我们进一步确定了内侧隔区PV神经元放电模式的异质性,以及亚型代表性比例的其他基因型差异。这些结果证实内侧隔区是DS中的另一个病理位点,可能导致认知障碍等合并症。

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