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在哺乳动物听觉突触中,由γ-氨基丁酸(GABA)共释放所塑造的甘氨酸能传递。

Glycinergic transmission shaped by the corelease of GABA in a mammalian auditory synapse.

作者信息

Lu Tao, Rubio Maria E, Trussell Laurence O

机构信息

Oregon Hearing Research Center and Vollum Institute, Oregon Health & Science University, Portland, OR 97239, USA.

出版信息

Neuron. 2008 Feb 28;57(4):524-35. doi: 10.1016/j.neuron.2007.12.010.

Abstract

The firing pattern of neurons is shaped by the convergence of excitation and inhibition, each with finely tuned magnitude and duration. In an auditory brainstem nucleus, glycinergic inhibition features fast decay kinetics, the mechanism of which is unknown. By applying glycine to native or recombinant glycine receptors, we show that response decay times are accelerated by addition of GABA, a weak partial agonist of glycine receptors. Systematic variation in agonist exposure time revealed that fast synaptic time course may be achieved with submillisecond exposures to mixtures of glycine and GABA at physiological concentrations. Accordingly, presynaptic terminals generally contained both transmitters, and depleting terminals of GABA slowed glycinergic synaptic currents. Thus, coreleased GABA accelerates glycinergic transmission by acting directly on glycine receptors, narrowing the time window for effective inhibition. Packaging both weak and strong agonists in vesicles may be a general means by which presynaptic neurons regulate the duration of postsynaptic responses.

摘要

神经元的放电模式由兴奋和抑制的汇聚所塑造,二者的强度和持续时间都经过精细调节。在听觉脑干核中,甘氨酸能抑制具有快速衰减动力学,其机制尚不清楚。通过将甘氨酸应用于天然或重组甘氨酸受体,我们发现加入GABA(甘氨酸受体的一种弱部分激动剂)会加速反应衰减时间。激动剂暴露时间的系统变化表明,在生理浓度下,对甘氨酸和GABA混合物进行亚毫秒级暴露可能实现快速的突触时间进程。因此,突触前终末通常同时含有这两种递质,耗尽GABA会减慢甘氨酸能突触电流。因此,共同释放的GABA通过直接作用于甘氨酸受体来加速甘氨酸能传递,缩小有效抑制的时间窗口。将弱激动剂和强激动剂都包装在囊泡中可能是突触前神经元调节突触后反应持续时间的一种普遍方式。

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