Pre-synaptic and post-synaptic A-type K+ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations

Guan Hsun Wang; Ai Yu Chuang; Yi Chen Lai; Hsin I. Chen; Shu Wei Hsueh; Ya Chin Yang

doi:10.1111/bph.15818

Pre-synaptic and post-synaptic A-type K⁺ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations

Guan Hsun Wang, Ai Yu Chuang, Yi Chen Lai, Hsin I. Chen, Shu Wei Hsueh, Ya Chin Yang^*

^*此作品的通信作者

生物醫學系(含學士班、臨床試驗與評估碩士班)

研究成果: 期刊稿件 › 文章 › 同行評審

3 引文斯高帕斯（Scopus）

摘要

Background and Purpose: Anticonvulsants targeting K⁺ channels have not been clinically available, although neuronal hyperexcitability in seizures could be suppressed by activation of K⁺ channels. Voltage-gated A-type K⁺ channel (A-channel) inhibitors may be prescribed for diseases of neuromuscular junction but could cause seizures. Consistently, genetic loss of function of A-channels may also cause seizures. It is unclear why inhibition of A-channels, compared with other types of K⁺ channels, is particularly prone to seizure induction. This hinders the development of relevant therapeutic interventions. Experimental Approach: Mechanisms underlying epileptogenesis with A-channel inhibition and antiepileptic actions of A-channel activation were investigated with electrophysiological, pharmacological, optogenetic, and behavioral approaches. Key Results: Pre-synaptic K_V1.4 and post-synaptic K_V4.3 A-channels act synergistically to gate glutamatergic transmission and control rhythmogenesis in the amygdala. The interconnected neurons set into the oscillatory mode by A-channel inhibition would reverberate with regular paces and the same top frequency, demonstrating a spatio-temporally well-orchestrated system with built-in oscillatory rhythms normally curbed by A-channels. Accordingly, selective over-excitation of glutamatergic neurons or inhibition of A-channels can induce behavioural seizures, which may be ameliorated by A-channel activators (e.g. NS-5806) or AMPA receptor antagonists (e.g. perampanel). Conclusion and Implications: Trans-synaptic voltage-dependent A-channels serve as a biophysical-biochemical transducer responsible for a novel form of synaptic plasticity. Such a network-level switch into and out of the oscillatory mode may underlie a wide scope of telencephalic information processing or, at its extreme, epileptic seizures. A-channels thus constitute a potential target of antiepileptic therapy.

原文	英語
頁（從 - 到）	3754-3777
頁數	24
期刊	British Journal of Pharmacology
卷	179
發行號	14
DOIs	https://doi.org/10.1111/bph.15818
出版狀態	已出版 - 07 2022

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Publisher Copyright:
© 2022 The British Pharmacological Society.

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10.1111/bph.15818

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@article{f51225fefd944e42a83a5fe69d9e3388,

title = "Pre-synaptic and post-synaptic A-type K+ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations",

abstract = "Background and Purpose: Anticonvulsants targeting K+ channels have not been clinically available, although neuronal hyperexcitability in seizures could be suppressed by activation of K+ channels. Voltage-gated A-type K+ channel (A-channel) inhibitors may be prescribed for diseases of neuromuscular junction but could cause seizures. Consistently, genetic loss of function of A-channels may also cause seizures. It is unclear why inhibition of A-channels, compared with other types of K+ channels, is particularly prone to seizure induction. This hinders the development of relevant therapeutic interventions. Experimental Approach: Mechanisms underlying epileptogenesis with A-channel inhibition and antiepileptic actions of A-channel activation were investigated with electrophysiological, pharmacological, optogenetic, and behavioral approaches. Key Results: Pre-synaptic KV1.4 and post-synaptic KV4.3 A-channels act synergistically to gate glutamatergic transmission and control rhythmogenesis in the amygdala. The interconnected neurons set into the oscillatory mode by A-channel inhibition would reverberate with regular paces and the same top frequency, demonstrating a spatio-temporally well-orchestrated system with built-in oscillatory rhythms normally curbed by A-channels. Accordingly, selective over-excitation of glutamatergic neurons or inhibition of A-channels can induce behavioural seizures, which may be ameliorated by A-channel activators (e.g. NS-5806) or AMPA receptor antagonists (e.g. perampanel). Conclusion and Implications: Trans-synaptic voltage-dependent A-channels serve as a biophysical-biochemical transducer responsible for a novel form of synaptic plasticity. Such a network-level switch into and out of the oscillatory mode may underlie a wide scope of telencephalic information processing or, at its extreme, epileptic seizures. A-channels thus constitute a potential target of antiepileptic therapy.",

keywords = "K1.4 channels, K4.3 channels, NS-5806, antiepileptic drug, brain rhythm regulation, epileptogenesis, glutamatergic transmission, neural network oscillations, voltage-gated A-type K channels",

author = "Wang, {Guan Hsun} and Chuang, {Ai Yu} and Lai, {Yi Chen} and Chen, {Hsin I.} and Hsueh, {Shu Wei} and Yang, {Ya Chin}",

note = "Publisher Copyright: {\textcopyright} 2022 The British Pharmacological Society.",

year = "2022",

month = jul,

doi = "10.1111/bph.15818",

language = "英语",

volume = "179",

pages = "3754--3777",

journal = "British Journal of Pharmacology",

issn = "0007-1188",

publisher = "John Wiley and Sons Inc",

number = "14",

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TY - JOUR

T1 - Pre-synaptic and post-synaptic A-type K+ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations

AU - Wang, Guan Hsun

AU - Chuang, Ai Yu

AU - Lai, Yi Chen

AU - Chen, Hsin I.

AU - Hsueh, Shu Wei

AU - Yang, Ya Chin

PY - 2022/7

Y1 - 2022/7

N2 - Background and Purpose: Anticonvulsants targeting K+ channels have not been clinically available, although neuronal hyperexcitability in seizures could be suppressed by activation of K+ channels. Voltage-gated A-type K+ channel (A-channel) inhibitors may be prescribed for diseases of neuromuscular junction but could cause seizures. Consistently, genetic loss of function of A-channels may also cause seizures. It is unclear why inhibition of A-channels, compared with other types of K+ channels, is particularly prone to seizure induction. This hinders the development of relevant therapeutic interventions. Experimental Approach: Mechanisms underlying epileptogenesis with A-channel inhibition and antiepileptic actions of A-channel activation were investigated with electrophysiological, pharmacological, optogenetic, and behavioral approaches. Key Results: Pre-synaptic KV1.4 and post-synaptic KV4.3 A-channels act synergistically to gate glutamatergic transmission and control rhythmogenesis in the amygdala. The interconnected neurons set into the oscillatory mode by A-channel inhibition would reverberate with regular paces and the same top frequency, demonstrating a spatio-temporally well-orchestrated system with built-in oscillatory rhythms normally curbed by A-channels. Accordingly, selective over-excitation of glutamatergic neurons or inhibition of A-channels can induce behavioural seizures, which may be ameliorated by A-channel activators (e.g. NS-5806) or AMPA receptor antagonists (e.g. perampanel). Conclusion and Implications: Trans-synaptic voltage-dependent A-channels serve as a biophysical-biochemical transducer responsible for a novel form of synaptic plasticity. Such a network-level switch into and out of the oscillatory mode may underlie a wide scope of telencephalic information processing or, at its extreme, epileptic seizures. A-channels thus constitute a potential target of antiepileptic therapy.

AB - Background and Purpose: Anticonvulsants targeting K+ channels have not been clinically available, although neuronal hyperexcitability in seizures could be suppressed by activation of K+ channels. Voltage-gated A-type K+ channel (A-channel) inhibitors may be prescribed for diseases of neuromuscular junction but could cause seizures. Consistently, genetic loss of function of A-channels may also cause seizures. It is unclear why inhibition of A-channels, compared with other types of K+ channels, is particularly prone to seizure induction. This hinders the development of relevant therapeutic interventions. Experimental Approach: Mechanisms underlying epileptogenesis with A-channel inhibition and antiepileptic actions of A-channel activation were investigated with electrophysiological, pharmacological, optogenetic, and behavioral approaches. Key Results: Pre-synaptic KV1.4 and post-synaptic KV4.3 A-channels act synergistically to gate glutamatergic transmission and control rhythmogenesis in the amygdala. The interconnected neurons set into the oscillatory mode by A-channel inhibition would reverberate with regular paces and the same top frequency, demonstrating a spatio-temporally well-orchestrated system with built-in oscillatory rhythms normally curbed by A-channels. Accordingly, selective over-excitation of glutamatergic neurons or inhibition of A-channels can induce behavioural seizures, which may be ameliorated by A-channel activators (e.g. NS-5806) or AMPA receptor antagonists (e.g. perampanel). Conclusion and Implications: Trans-synaptic voltage-dependent A-channels serve as a biophysical-biochemical transducer responsible for a novel form of synaptic plasticity. Such a network-level switch into and out of the oscillatory mode may underlie a wide scope of telencephalic information processing or, at its extreme, epileptic seizures. A-channels thus constitute a potential target of antiepileptic therapy.

KW - K1.4 channels

KW - K4.3 channels

KW - NS-5806

KW - antiepileptic drug

KW - brain rhythm regulation

KW - epileptogenesis

KW - glutamatergic transmission

KW - neural network oscillations

KW - voltage-gated A-type K channels

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U2 - 10.1111/bph.15818

DO - 10.1111/bph.15818

M3 - 文章

C2 - 35170022

AN - SCOPUS:85126206907

SN - 0007-1188

VL - 179

SP - 3754

EP - 3777

JO - British Journal of Pharmacology

JF - British Journal of Pharmacology

IS - 14

ER -

Pre-synaptic and post-synaptic A-type K+ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations

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Pre-synaptic and post-synaptic A-type K⁺ channels regulate glutamatergic transmission and switching of the network into epileptiform oscillations