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首页> 外文期刊>The Journal of Physiology >The dynamics of single spike-evoked adenosine release in the cerebellum.
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The dynamics of single spike-evoked adenosine release in the cerebellum.

机译:小脑中单峰诱发腺苷释放的动力学。

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The purine adenosine is a potent neuromodulator in the brain, with roles in a number of diverse physiological and pathological processes. Modulators such as adenosine are difficult to study as once released they have a diffuse action (which can affect many neurones) and, unlike classical neurotransmitters, have no inotropic receptors. Thus rapid postsynaptic currents (PSCs) mediated by adenosine (equivalent to mPSCs) are not available for study. As a result the mechanisms and properties of adenosine release still remain relatively unclear. We have studied adenosine release evoked by stimulating the parallel fibres in the cerebellum. Using adenosine biosensors combined with deconvolution analysis and mathematical modelling, we have characterised the release dynamics and diffusion of adenosine in unprecedented detail. By partially blocking K+ channels, we were able to release adenosine in response to a single stimulus rather than a train of stimuli. This allowed reliable sub-second release of reproducible quantities of adenosine with stereotypic concentration waveforms that agreed well with predictions of a mathematical model of purine diffusion. We found no evidence for ATP release and thus suggest that adenosine is directly released in response to parallel fibre firing and does not arise from extracellular ATP metabolism. Adenosine release events showed novel short-term dynamics, including facilitated release with paired stimuli at millisecond stimulation intervals but depletion-recovery dynamics with paired stimuli delivered over minute time scales. These results demonstrate rich dynamics for adenosine release that are placed, for the first time, on a quantitative footing and show strong similarity with vesicular exocytosis.
机译:嘌呤腺苷是大脑中一种有效的神经调节剂,在许多不同的生理和病理过程中起作用。腺苷等调节剂很难研究,因为它们一旦释放便具有扩散作用(会影响许多神经元),并且与经典的神经递质不同,它没有正性肌力受体。因此,腺苷介导的快速突触后电流(PSC)(相当于mPSC)尚无法研究。结果,腺苷释放的机制和性质仍然相对不清楚。我们已经研究了通过刺激小脑中的平行纤维引起的腺苷释放。使用腺苷生物传感器结合去卷积分析和数学建模,我们以前所未有的细节描述了腺苷的释放动力学和扩散。通过部分阻断K +通道,我们能够响应单一刺激而非一系列刺激而释放腺苷。这样就可以可靠地亚秒释放具有定型浓度波形的可复制量的腺苷,这与嘌呤扩散数学模型的预测非常吻合。我们没有发现ATP释放的证据,因此表明腺苷是响应平行纤维燃烧而直接释放的,而不是由细胞外ATP代谢引起的。腺苷释放事件显示出新颖的短期动力学,包括在毫秒刺激间隔内与成对刺激物一起促进释放,但在分钟时间内传递成对刺激物的消耗-恢复动力学。这些结果证明了腺苷释放的丰富动力学,这是首次将其定量定位,并显示出与囊泡胞吐作用的强相似性。

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