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海马体中GABA能中间神经元的抑制性控制。

Inhibitory control of GABAergic interneurons in the hippocampus.

作者信息

Freund T F, Gulyás A I

机构信息

Institute of Experimental Medicine, Hungarian Academy of Sciences, Budapest, Hungary.

出版信息

Can J Physiol Pharmacol. 1997 May;75(5):479-87.

PMID:9250381
Abstract

Hippocampal GABAergic interneurons are responsible for controlling the output and efficacy of synaptic input of large principal cell populations and, thereby, determine the oscillatory discharge patterns and synaptic plasticity in the hippocampus. Single interneurons are able to prevent repetitive firing of postsynaptic pyramidal cells (R. Miles, K. Tóth, A.I. Gulyás, N. Hájos, and T.F. Freund. Neuron, 16: 815-823, 1996), whereas on occasion a single pyramidal cell may be able to activate an interneuron under in vitro conditions (A.I. Gulyás, R. Miles, A. Sik, K. Tóth, N. Tamamaki, and T.F. Freund. Nature (London), 366: 683-687, 1993). Inhibition is therefore extremely powerful. Transient suppression of interneuronal activity allows the precise timing and synchronization of inhibitory postsynaptic potentials arriving at principal cells. A rhythmic suppression or modulation of interneuron discharge may be brought about by input from at least two major sources: (i) from other local interneurons or (ii) from subcortical centers. Of the possible local sources, in the present review particular attention will be paid to GABAergic neurons specialized to innervate other interneurons. Subcortical pathways known to modulate specific inhibitory functions in the hippocampus, i.e., the GABAergic and cholinergic septohippocampal and the serotonergic raphe hippocampal pathways, will also be reviewed. Roles of these control mechanisms may include the generation of theta and higher frequency oscillations and the selective removal of inhibition from the termination zone of specific excitatory afferents, thereby increasing their efficacy and (or) plasticity.

摘要

海马体中的γ-氨基丁酸能中间神经元负责控制大量主细胞群体突触输入的输出和效能,从而决定海马体中的振荡放电模式和突触可塑性。单个中间神经元能够阻止突触后锥体细胞的重复放电(R. 迈尔斯、K. 托特、A.I. 古利亚什、N. 哈约什和T.F. 弗伦德。《神经元》,16: 815 - 823,1996年),而在体外条件下,单个锥体细胞有时可能能够激活一个中间神经元(A.I. 古利亚什、R. 迈尔斯、A. 西克、K. 托特、N. 玉巻和T.F. 弗伦德。《自然》(伦敦),366: 683 - 687,1993年)。因此,抑制作用极其强大。中间神经元活动的短暂抑制可使到达主细胞的抑制性突触后电位实现精确计时和同步。中间神经元放电的节律性抑制或调节可能由至少两个主要来源的输入引起:(i)来自其他局部中间神经元,或(ii)来自皮层下中枢。在本综述中,对于可能的局部来源,将特别关注专门支配其他中间神经元的γ-氨基丁酸能神经元。已知可调节海马体中特定抑制功能的皮层下通路,即γ-氨基丁酸能和胆碱能的隔海马通路以及5-羟色胺能的中缝海马通路,也将进行综述。这些控制机制的作用可能包括产生θ波和更高频率的振荡,以及选择性地消除特定兴奋性传入纤维终末区域的抑制,从而提高其效能和(或)可塑性。

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