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大鼠脊髓中自发突触传递的发育

Development of spontaneous synaptic transmission in the rat spinal cord.

作者信息

Gao B X, Cheng G, Ziskind-Conhaim L

机构信息

Department of Physiology and Center for Neuroscience, University of Wisconsin Medical School, Madison, Wisconsin 53706, USA.

出版信息

J Neurophysiol. 1998 May;79(5):2277-87. doi: 10.1152/jn.1998.79.5.2277.

Abstract

Dorsal root afferents form synaptic connections on motoneurons a few days after motoneuron clustering in the rat lumbar spinal cord, but frequent spontaneous synaptic potentials are detected only after birth. To increase our understanding of the mechanisms underlying the differentiation of synaptic transmission, we examined the developmental changes in properties of spontaneous synaptic transmission at early stages of synapse formation. Spontaneous postsynaptic currents (PSCs) and tetrodotoxin (TTX)-resistant miniature PSCs (mPSCs) were measured in spinal motoneurons of embryonic and postnatal rats using whole cell patch-clamp recordings. Spontaneous PSC frequencies were higher than mPSC frequencies in both embryonic and postnatal motoneurons, suggesting that even at embryonic stages, when action-potential firing rate was low, presynaptic action potentials played an important role in triggering spontaneous PSCs. After birth, the twofold increase in spontaneous PSC frequency was attributed to an increase in action-potential-independent quantal release rather than to a higher rate of action-potential firing. In embryonic motoneurons, the fluctuations in peak amplitude of spontaneous PSCs were normally distributed around single peaks with modal values similar to those of mPSCs. These data indicated that early in synapse differentiation spontaneous PSCs were primarily composed of currents generated by quantal release. After birth, mean mPSC amplitude increased by 50% but mean quantal current amplitude did not change. Synchronous, multiquantal release was apparent in postnatal motoneurons only in high-K+ extracellular solution. Comparison of the properties of miniature excitatory and inhibitory postsynaptic currents (mEPSCs and mIPSCs) demonstrated that mean mEPSC frequency was higher than mIPSC frequency, suggesting that either excitatory synapses outnumbered inhibitory synapses or that the probability of excitatory transmitter release was higher than the release of inhibitory neurotransmitters. The finding that mIPSC duration was several-fold longer than mEPSC duration implied that despite their lower frequency, inhibitory currents could modulate motoneuron synaptic integration by shunting incoming excitatory inputs for prolonged time intervals.

摘要

在大鼠腰脊髓运动神经元集群形成几天后,背根传入纤维在运动神经元上形成突触连接,但只有在出生后才检测到频繁的自发突触电位。为了增进我们对突触传递分化潜在机制的理解,我们研究了突触形成早期自发突触传递特性的发育变化。使用全细胞膜片钳记录技术,在胚胎期和新生大鼠的脊髓运动神经元中测量自发突触后电流(PSC)和河豚毒素(TTX)抗性微小PSC(mPSC)。在胚胎期和新生运动神经元中,自发PSC频率均高于mPSC频率,这表明即使在胚胎期,当动作电位发放频率较低时,突触前动作电位在触发自发PSC中也发挥着重要作用。出生后,自发PSC频率增加两倍归因于与动作电位无关的量子释放增加,而非动作电位发放频率提高。在胚胎运动神经元中,自发PSC峰值幅度的波动围绕单峰呈正态分布,其模态值与mPSC相似。这些数据表明,在突触分化早期,自发PSC主要由量子释放产生的电流组成。出生后,平均mPSC幅度增加了50%,但平均量子电流幅度没有变化。仅在高钾细胞外溶液中,新生运动神经元中才出现同步的多量子释放。对微小兴奋性和抑制性突触后电流(mEPSC和mIPSC)特性的比较表明,平均mEPSC频率高于mIPSC频率,这表明要么兴奋性突触数量多于抑制性突触,要么兴奋性递质释放概率高于抑制性神经递质的释放概率。mIPSC持续时间比mEPSC持续时间长几倍这一发现表明,尽管抑制性电流频率较低,但它们可以通过长时间分流传入的兴奋性输入来调节运动神经元的突触整合。

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