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通过内源性三磷酸腺苷实现成熟听觉神经元的音频拓扑动作电位调谐。

Tonotopic action potential tuning of maturing auditory neurons through endogenous ATP.

作者信息

Jovanovic Saša, Radulovic Tamara, Coddou Claudio, Dietz Beatrice, Nerlich Jana, Stojilkovic Stanko S, Rübsamen Rudolf, Milenkovic Ivan

机构信息

Institute of Biology, Faculty of Biosciences, Pharmacy and Psychology, University of Leipzig, Leipzig, Germany.

Carl Ludwig Institute for Physiology, Faculty of Medicine, University of Leipzig, Leipzig, Germany.

出版信息

J Physiol. 2017 Feb 15;595(4):1315-1337. doi: 10.1113/JP273272. Epub 2016 Dec 28.

Abstract

KEY POINTS

Following the genetically controlled formation of neuronal circuits, early firing activity guides the development of sensory maps in the auditory, visual and somatosensory system. However, it is not clear whether the activity of central auditory neurons is specifically regulated depending on the position within the sensory map. In the ventral cochlear nucleus, the first central station along the auditory pathway, we describe a mechanism through which paracrine ATP signalling enhances firing in a cell-specific and tonotopically-determined manner. Developmental down-regulation of P2X2/3R currents along the tonotopic axis occurs simultaneously with an increase in AMPA receptor currents, suggesting a high-to-low frequency maturation pattern. Facilitated action potential (AP) generation, measured as higher firing rate, shorter EPSP-AP delay in vivo and shorter AP latency in slice experiments, is consistent with increased synaptic efficacy caused by ATP. The long lasting change in intrinsic neuronal excitability is mediated by the heteromeric P2X2/3 receptors.

ABSTRACT

Synaptic refinement and strengthening are activity-dependent processes that establish orderly arranged cochleotopic maps throughout the central auditory system. The maturation of auditory brainstem circuits is guided by action potentials (APs) arising from the inner hair cells in the developing cochlea. The AP firing of developing central auditory neurons can be modulated by paracrine ATP signalling, as shown for the cochlear nucleus bushy cells and principal neurons in the medial nucleus of the trapezoid body. However, it is not clear whether neuronal activity may be specifically regulated with respect to the nuclear tonotopic position (i.e. sound frequency selectivity). Using slice recordings before hearing onset and in vivo recordings with iontophoretic drug applications after hearing onset, we show that cell-specific purinergic modulation follows a precise tonotopic pattern in the ventral cochlear nucleus of developing gerbils. In high-frequency regions, ATP responsiveness diminished before hearing onset. In low-to-mid frequency regions, ATP modulation persisted after hearing onset in a subset of low-frequency bushy cells (characteristic frequency< 10 kHz). Down-regulation of P2X2/3R currents along the tonotopic axis occurs simultaneously with an increase in AMPA receptor currents, thus suggesting a high-to-low frequency maturation pattern. Facilitated AP generation, measured as higher firing frequency, shorter EPSP-AP delay in vivo, and shorter AP latency in slice experiments, is consistent with increased synaptic efficacy caused by ATP. Finally, by combining recordings and pharmacology in vivo, in slices, and in human embryonic kidney 293 cells, it was shown that the long lasting change in intrinsic neuronal excitability is mediated by the P2X2/3R.

摘要

关键点

在神经元回路的基因控制形成之后,早期放电活动引导听觉、视觉和体感系统中感觉图谱的发育。然而,尚不清楚中枢听觉神经元的活动是否根据感觉图谱内的位置受到特异性调节。在听觉通路的第一个中枢站——蜗腹侧核中,我们描述了一种旁分泌ATP信号以细胞特异性和音频拓扑决定的方式增强放电的机制。沿音频拓扑轴P2X2/3R电流的发育性下调与AMPA受体电流的增加同时发生,这表明存在从高频到低频的成熟模式。以更高的放电率、体内更短的兴奋性突触后电位-动作电位延迟以及脑片实验中更短的动作电位潜伏期来衡量的动作电位(AP)产生的促进,与ATP引起的突触效能增加一致。内在神经元兴奋性的持久变化由异聚体P2X2/3受体介导。

摘要

突触的细化和强化是依赖活动的过程,在整个中枢听觉系统中建立有序排列的耳蜗拓扑图谱。听觉脑干回路的成熟由发育中的耳蜗内毛细胞产生的动作电位(AP)引导。发育中的中枢听觉神经元的AP放电可由旁分泌ATP信号调节,如耳蜗核浓密细胞和梯形体内侧核的主神经元所示。然而,尚不清楚神经元活动是否可能根据核音频拓扑位置(即声音频率选择性)受到特异性调节。通过在听力开始前进行脑片记录以及在听力开始后通过离子电泳药物应用进行体内记录,我们表明在发育中的沙鼠蜗腹侧核中,细胞特异性嘌呤能调制遵循精确的音频拓扑模式。在高频区域,ATP反应性在听力开始前降低。在低频到中频区域,ATP调制在听力开始后在一部分低频浓密细胞(特征频率<10kHz)中持续存在。沿音频拓扑轴P2X2/3R电流的下调与AMPA受体电流的增加同时发生,因此表明存在从高频到低频的成熟模式。以更高的放电频率、体内更短的兴奋性突触后电位-动作电位延迟以及脑片实验中更短的动作电位潜伏期来衡量的AP产生的促进,与ATP引起的突触效能增加一致。最后,通过在体内、脑片和人胚肾293细胞中结合记录和药理学研究,表明内在神经元兴奋性的持久变化由P2X2/3R介导。

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