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突触后超极化增强了苔藓纤维与CA3锥体细胞之间大型突触处AMPA介导的突触传递强度。

Postsynaptic hyperpolarization increases the strength of AMPA-mediated synaptic transmission at large synapses between mossy fibers and CA3 pyramidal cells.

作者信息

Berretta N, Rossokhin A V, Kasyanov A M, Sokolov M V, Cherubini E, Voronin L L

机构信息

Neuroscience Program and INFM Unit, International School for Advanced Studies, Via Beirut 2-4, 34014, Trieste, Italy.

出版信息

Neuropharmacology. 2000 Sep;39(12):2288-301. doi: 10.1016/s0028-3908(00)00076-9.

Abstract

In chemical synapses information flow is polarized. However, the postsynaptic cells can affect transmitter release via retrograde chemical signaling. Here we explored the hypothesis that, in large synapses, having large synaptic cleft resistance, transmitter release can be enhanced by electrical (ephaptic) signaling due to depolarization of the presynaptic release site induced by the excitatory postsynaptic current itself. The hypothesis predicts that, in such synapses, postsynaptic hyperpolarization would increase response amplitudes "supralinearly", i.e. stronger than predicted from the driving force shift. We found supralinear increases in the amplitude of minimal excitatory postsynaptic potential (EPSP) during hyperpolarization of CA3 pyramidal neurons. Failure rate, paired-pulse facilitation, coefficient of variation of the EPSP amplitude and EPSP quantal content were also modified. The effects were especially strong on mossy fiber EPSPs (MF-EPSPs) mediated by the activation of large synapses and identified pharmacologically or by their kinetics. The effects were weaker on commissural fiber EPSPs mediated by smaller and more remote synapses. Even spontaneous membrane potential fluctuations were associated with supralinear MF-EPSP increases and failure rate reduction. The results suggest the existence of a novel mechanism for retrograde control of synaptic efficacy from postsynaptic membrane potential and are consistent with the ephaptic feedback hypothesis.

摘要

在化学突触中,信息流是极化的。然而,突触后细胞可通过逆行化学信号传导影响递质释放。在此,我们探讨了这样一种假说:在具有较大突触间隙电阻的大型突触中,由于兴奋性突触后电流本身引起的突触前释放位点去极化,电(电突触)信号传导可增强递质释放。该假说预测,在这类突触中,突触后超极化将使反应幅度呈“超线性”增加,即比驱动力变化所预测的更强。我们发现,在CA3锥体神经元超极化期间,最小兴奋性突触后电位(EPSP)的幅度呈超线性增加。失败率、双脉冲易化、EPSP幅度的变异系数以及EPSP量子含量也发生了改变。这些效应在由大型突触激活介导的苔藓纤维EPSP(MF-EPSP)上尤为明显,这些大型突触可通过药理学方法或其动力学特性来识别。在由较小且距离更远的突触介导的联合纤维EPSP上,效应较弱。甚至自发膜电位波动也与MF-EPSP超线性增加和失败率降低有关。结果表明存在一种从突触后膜电位逆行控制突触效能的新机制,并且与电突触反馈假说相符。

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