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颞叶癫痫中海马下托细胞类型特异性中间神经元的环路重组

Circuit Reorganization of Subicular Cell-Type-Specific Interneurons in Temporal Lobe Epilepsy.

作者信息

Fei Fan, Wang Xia, Fan Xukun, Gong Yiwei, Yang Lin, Wang Yu, Xu Cenglin, Wang Shuang, Chen Zhong, Wang Yi

机构信息

Key Laboratory of Neuropharmacology and Translational Medicine of Zhejiang Province, School of Pharmaceutical Sciences, Zhejiang Chinese Medical University, Hangzhou 310053, China.

Institute of Pharmacology and Toxicology, College of Pharmaceutical Sciences, Zhejiang University, Hangzhou 310058, China.

出版信息

J Neurosci. 2025 Jan 29;45(5):e0760242024. doi: 10.1523/JNEUROSCI.0760-24.2024.

Abstract

The subiculum represents a crucial brain pivot in regulating seizure generalization in temporal lobe epilepsy (TLE), primarily through a synergy of local GABAergic and long-projecting glutamatergic signaling. However, little is known about how subicular GABAergic interneurons are involved in a cell-type-specific way. Here, employing Ca fiber photometry, retrograde monosynaptic viral tracing, and chemogenetics in epilepsy models of both male and female mice, we elucidate circuit reorganization patterns mediated by subicular cell-type-specific interneurons and delineate their functional disparities in seizure modulation in TLE. We reveal distinct functional dynamics of subicular parvalbumin+ and somatostatin+ interneurons during secondary generalized seizure. These interneuron subtypes have their biased circuit organizations in terms of both input and output patterns, which undergo distinct reorganization in chronic epileptic condition. Notably, somatostatin+ interneurons exert more effective feedforward inhibition onto pyramidal neurons compared with parvalbumin+ interneurons, which engenders consistent antiseizure effects in TLE. These findings provide an improved understanding of different subtypes of subicular interneurons in circuit reorganization in TLE and supplement compelling proofs for precise treatment of epilepsy by targeting subicular somatostatin+ interneurons.

摘要

海马下脚是调节颞叶癫痫(TLE)发作泛化的关键脑枢纽,主要通过局部γ-氨基丁酸能(GABAergic)信号和长投射谷氨酸能信号的协同作用来实现。然而,关于海马下脚GABA能中间神经元如何以细胞类型特异性方式参与其中,我们却知之甚少。在此,我们利用钙纤维光度法、逆行单突触病毒示踪法以及化学遗传学方法,对雄性和雌性小鼠的癫痫模型进行研究,以阐明由海马下脚细胞类型特异性中间神经元介导的回路重组模式,并描绘它们在TLE发作调节中的功能差异。我们揭示了继发性全身性癫痫发作期间海马下脚小白蛋白阳性(parvalbumin+)和生长抑素阳性(somatostatin+)中间神经元的不同功能动态。这些中间神经元亚型在输入和输出模式方面具有偏向性的回路组织,在慢性癫痫状态下会经历不同的重组。值得注意的是,与小白蛋白阳性中间神经元相比,生长抑素阳性中间神经元对锥体神经元施加更有效的前馈抑制,这在TLE中产生了一致的抗癫痫作用。这些发现有助于更好地理解海马下脚中间神经元不同亚型在TLE回路重组中的作用,并为通过靶向海马下脚生长抑素阳性中间神经元精准治疗癫痫提供了有力证据。

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