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在鉴定的大鼠 CA1 中间神经元突触上,通过紧张型大麻素受体激活实现 GABA 的异步释放。

Asynchronous release of GABA via tonic cannabinoid receptor activation at identified interneuron synapses in rat CA1.

机构信息

Department of Pharmacology, School of Pharmacy, University of London, 29/39 Brunswick Square, London WC1N 1AX, UK.

出版信息

Eur J Neurosci. 2010 Apr;31(7):1196-207. doi: 10.1111/j.1460-9568.2010.07165.x. Epub 2010 Mar 19.

Abstract

The influence of local circuit interneurons is thought to play an important role in adjusting synaptic strength via endogenous cannabinoid type 1 (CB1) receptors. Using paired whole-cell recordings, combined with double immunofluorescence and biocytin labelling in acute slices of rat CA1 at postnatal day 18-23, we investigated the properties of Cholecystokinin (CCK)-positive stratum radiatum local circuit interneuron connections that utilised CB1 receptors. Three types of synaptic connections were studied, lacunosum-moleculare-radiatum perforant path-associated (LM-R PPA) to Shaffer collateral-associated (SCA) interneurons, SCA-SCA interneurons and SCA-pyramidal cells. These three synapses were differentially under tonic reduction of inhibition that was blocked by the CB1 receptor inverse agonist AM-251 (10 microM), which enhanced IPSPs. The strength of tonic reduction of inhibition was correlated with asynchronous release which was apparent at connections among interneurons. AM-251 increased the ratio of synchronous to asynchronous release (synchronicity ratio), while the CB receptor agonist anandamide (14 microM) decreased the synchronicity ratio. Fast and slow calcium chelators (BAPTA-AM and EGTA-AM) also increased the synchronicity ratio, accelerated inhibitory time courses and reduced IPSP amplitudes. These data suggest that CB1 receptors at connections among interneuron synapses play a role in tonic suppression of inhibition and govern the asynchronous release of GABA, modulating the time windows of inhibition. Effects of calcium chelators suggest that asynchronous release is a result of a long-lasting presynaptic calcium transients and/or a large distance between calcium source and sensor of exocytosis. These properties of specialised inhibitory neurons may have important modulatory roles in controlling spike timing among local circuit interneurons.

摘要

局部回路中间神经元的影响被认为通过内源性大麻素 1 型 (CB1) 受体在调节突触强度方面发挥重要作用。使用在生后第 18-23 天的大鼠 CA1 急性切片中进行的配对全细胞记录,结合双免疫荧光和生物胞素标记,我们研究了利用 CB1 受体的胆囊收缩素 (CCK) 阳性放射状层局部回路中间神经元连接的特性。研究了三种类型的突触连接,即腔隙-分子层放射状通路相关 (LM-R PPA) 到沙费尔侧支相关 (SCA) 中间神经元、SCA-SCA 中间神经元和 SCA-锥体神经元。这三个突触受到抑制的紧张性降低的不同影响,这种抑制的紧张性降低被 CB1 受体反向激动剂 AM-251(10 μM)阻断,从而增强 IPSP。抑制紧张性降低的强度与异步释放相关,这种异步释放在中间神经元之间的连接中很明显。AM-251 增加了同步释放与异步释放的比值(同步性比值),而 CB 受体激动剂大麻素(14 μM)降低了同步性比值。快速和慢速钙螯合剂(BAPTA-AM 和 EGTA-AM)也增加了同步性比值,加速了抑制时间进程并降低了 IPSP 幅度。这些数据表明,中间神经元突触之间的 CB1 受体在抑制的紧张性抑制中起作用,并控制 GABA 的异步释放,调节抑制的时间窗口。钙螯合剂的作用表明,异步释放是由于长时间的突触前钙瞬变和/或钙源和出胞传感器之间的大距离造成的。这些特殊抑制性神经元的特性可能在控制局部回路中间神经元的尖峰定时方面具有重要的调节作用。

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