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皮质酮对海马齿状回长时程增强的β-肾上腺素能效应具有时间依赖性调节作用。

Corticosterone time-dependently modulates beta-adrenergic effects on long-term potentiation in the hippocampal dentate gyrus.

作者信息

Pu Zhenwei, Krugers Harm J, Joëls Marian

机构信息

Swammerdam Institute for Life Sciences, Center for NeuroScience, University of Amsterdam, SM Amsterdam, The Netherlands.

出版信息

Learn Mem. 2007 May 3;14(5):359-67. doi: 10.1101/lm.527207. Print 2007 May.

Abstract

Previous experiments in the hippocampal CA1 area have shown that corticosterone can facilitate long-term potentiation (LTP) in a rapid non-genomic fashion, while the same hormone suppresses LTP that is induced several hours after hormone application. Here, we elaborated on this finding by examining whether corticosterone exerts opposite effects on LTP depending on the timing of hormone application in the dentate gyrus as well. Moreover, we tested rapid and delayed actions by corticosterone on beta-adrenergic-dependent changes in LTP. Unlike the CA1 region, our in vitro field potential recordings show that rapid effects of corticosterone do not influence LTP induced by mild tetanization in the hippocampal dentate gyrus, unless GABA(A) receptors are blocked. In contrast, the beta-adrenergic agonist isoproterenol does initiate a slow-onset, limited amount of potentiation. When corticosterone was applied concurrently with isoproterenol, a further enhancement of synaptic strength was identified, especially during the early stage of potentiation. Yet, treatment with corticosterone several hours in advance of isoproterenol fully prevented any effect of isoproterenol on LTP. This emphasizes that corticosterone can regulate beta-adrenergic modulation of synaptic plasticity in opposite directions, depending on the timing of hormone application.

摘要

先前在海马体CA1区进行的实验表明,皮质酮能够以快速的非基因组方式促进长时程增强(LTP),而同样的激素会抑制在激素应用数小时后诱导产生的LTP。在此,我们通过研究皮质酮是否也会根据激素在齿状回中的应用时间对LTP产生相反作用,对这一发现进行了详细阐述。此外,我们测试了皮质酮对LTP中β-肾上腺素能依赖性变化的快速和延迟作用。与CA1区不同,我们的体外场电位记录显示,皮质酮的快速作用不会影响海马齿状回中轻度强直刺激诱导的LTP,除非γ-氨基丁酸A(GABA(A))受体被阻断。相反,β-肾上腺素能激动剂异丙肾上腺素确实会引发缓慢起效、程度有限的增强作用。当皮质酮与异丙肾上腺素同时应用时,突触强度会进一步增强,尤其是在增强作用的早期阶段。然而,在异丙肾上腺素应用数小时前用皮质酮进行处理,可完全阻止异丙肾上腺素对LTP的任何作用。这强调了皮质酮可根据激素应用时间以相反方向调节突触可塑性的β-肾上腺素能调节。

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