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抑制性突触何时发挥作用?

When is an inhibitory synapse effective?

作者信息

Qian N, Sejnowski T J

机构信息

Computational Neurobiology Laboratory, Salk Institute, La Jolla, CA 92037.

出版信息

Proc Natl Acad Sci U S A. 1990 Oct;87(20):8145-9. doi: 10.1073/pnas.87.20.8145.

Abstract

Interactions between excitatory and inhibitory synaptic inputs on dendrites determine the level of activity in neurons. Models based on the cable equation predict that silent shunting inhibition can strongly veto the effect of an excitatory input. The cable model assumes that ionic concentrations do not change during the electrical activity, which may not be a valid assumption, especially for small structures such as dendritic spines. We present here an analysis and computer simulations to show that for large Cl- conductance changes, the more general Nernst-Planck electrodiffusion model predicts that shunting inhibition on spines should be much less effective than that predicted by the cable model. This is a consequence of the large changes in the intracellular ionic concentration of Cl- that can occur in small structures, which would alter the reversal potential and reduce the driving force for Cl-. Shunting inhibition should therefore not be effective on spines, but it could be significantly more effective on the dendritic shaft at the base of the spine. In contrast to shunting inhibition, hyperpolarizing synaptic inhibition mediated by K+ currents can be very effective in reducing the excitatory synaptic potentials on the same spine if the excitatory conductance change is less than 10 nS. We predict that if the inhibitory synapses found on cortical spines are to be effective, then they should be mediated by K+ through GABAB receptors.

摘要

树突上兴奋性和抑制性突触输入之间的相互作用决定了神经元的活动水平。基于电缆方程的模型预测,沉默分流抑制可以强烈否决兴奋性输入的作用。电缆模型假设在电活动期间离子浓度不会改变,这可能不是一个有效的假设,特别是对于诸如树突棘等小结构。我们在此进行分析和计算机模拟,以表明对于大的Cl-电导变化,更通用的能斯特 - 普朗克电扩散模型预测,对树突棘的分流抑制应该比电缆模型预测的效果要差得多。这是小结构中Cl-细胞内离子浓度可能发生的巨大变化的结果,这会改变反转电位并降低Cl-的驱动力。因此,分流抑制对树突棘应该无效,但在树突棘基部的树突干上可能会明显更有效。与分流抑制相反,如果兴奋性电导变化小于10 nS,由K+电流介导的超极化突触抑制在降低同一树突棘上的兴奋性突触电位方面可能非常有效。我们预测,如果在皮质树突棘上发现的抑制性突触要有效,那么它们应该由K+通过GABAB受体介导。

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