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顶树突和基树突之间的巧合检测驱动小脑高尔基细胞中的突触可塑性。

Coincidence detection between apical and basal dendrites drives STDP in cerebellar Golgi cells.

作者信息

Pali Eleonora, Masoli Stefano, Di Domenico Danila, Sorbo Teresa, Prestori Francesca, D'Angelo Egidio

机构信息

Department of Brain and Behavioural Sciences, University of Pavia, Pavia, Italy.

Digital Neuroscience Centre, IRCCS Mondino Foundation, Pavia, Italy.

出版信息

Commun Biol. 2025 May 12;8(1):731. doi: 10.1038/s42003-025-08153-1.

Abstract

Cerebellar Golgi cells (GoCs), segregate parallel fiber (pf), and mossy fiber (mf) inputs on apical and basal dendrites. Computational modeling predicted that this anatomical arrangement, coupled with a specific ionic channel localization, could be instrumental to drive STDP at mf-GoC synapses. Here, we test this hypothesis with GoC patch-clamp recordings in acute mouse cerebellar slices. Repeated mf-pf pairing on the theta-band within a ± 50 ms time window induces anti-symmetric Hebbian-STDP, with spike-timing long-term potentiation or depression (st-LTP or st-LTD) occurring when action potentials (APs) elicited by pf stimulation follow or precede the activation of mf synapses, respectively. Mf-GoC STDP induction requires AP backpropagation from apical to basal dendrites, NMDA receptor activation at mf-GoC synapses, and intracellular calcium changes. Importantly, STDP is inverted by inhibitory control. Thus, experimental evidence confirms and extends model predictions suggesting that GoC STDP can bind molecular layer to granular layer activity, regulating cerebellar computation and learning.

摘要

小脑高尔基细胞(GoC)在顶树突和基底树突上分离平行纤维(pf)和苔藓纤维(mf)输入。计算模型预测,这种解剖结构与特定的离子通道定位相结合,可能有助于在mf-GoC突触处驱动突触可塑性。在这里,我们在急性小鼠小脑切片中通过GoC膜片钳记录来检验这一假设。在±50毫秒的时间窗口内,在θ波段重复进行mf-pf配对可诱导反对称的赫布型突触可塑性,当pf刺激引发的动作电位(AP)分别跟随或先于mf突触的激活时,会出现尖峰时间长时程增强或抑制(st-LTP或st-LTD)。Mf-GoC突触可塑性的诱导需要AP从顶树突向基底树突的反向传播、mf-GoC突触处的NMDA受体激活以及细胞内钙变化。重要的是,突触可塑性可通过抑制性控制而反转。因此,实验证据证实并扩展了模型预测,表明GoC突触可塑性可以将分子层活动与颗粒层活动联系起来,调节小脑的计算和学习。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8dbd/12066733/eb0bc8143a67/42003_2025_8153_Fig1_HTML.jpg

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