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低频刺激在体诱导穿通纤维-齿状回突触的长时程压抑和慢起始长时程增强。

Low-frequency stimulation induces long-term depression and slow onset long-term potentiation at perforant path-dentate gyrus synapses in vivo.

机构信息

Department of Biology, Neurosciences Research Institute, University of Texas, San Antonio, Texas.

出版信息

J Neurophysiol. 2014 Mar;111(6):1259-73. doi: 10.1152/jn.00941.2012. Epub 2013 Dec 11.

Abstract

The expression of homosynaptic long-term depression (LTD) is thought to mediate a crucial role in sustaining memory function. Our in vivo investigations of LTD expression at lateral (LPP) and medial perforant path (MPP) synapses in the dentate gyrus (DG) corroborate prior demonstrations that PP-DG LTD is difficult to induce in intact animals. In freely moving animals, LTD expression occurred inconsistently among LPP-DG and MPP-DG responses. Interestingly, following acute electrode implantation in anesthetized rats, low-frequency stimulation (LFS; 900 pulses, 1 Hz) promotes slow-onset LTP at both MPP-DG and LPP-DG synapses that utilize distinct induction mechanisms. Systemic administration of the N-methyl-d-aspartate (NMDA) receptor antagonist (+/-)-cyclopiperidine-6-piperiperenzine (CPP; 10 mg/kg) 90 min before LFS selectively blocked MPP-DG but not LPP-DG slow onset LTP, suggesting MPP-DG synapses express a NMDA receptor-dependent slow onset LTP whereas LPP-DG slow onset LTP induction is NMDA receptor independent. In experiments where paired-pulse LFS (900 paired pulses, 200-ms paired-pulse interval) was used to induce LTD, paired-pulse LFS of the LPP resulted in rapid onset LTP of DG responses, whereas paired-pulse LFS of the MPP induced slow onset LTP of DG responses. Although LTD observations were very rare following acute electrode implantation in anesthetized rats, LPP-DG LTD was demonstrated in some anesthetized rats with previously implanted electrodes. Together, our data indicate in vivo PP-DG LTD expression is an inconsistent phenomenon that is primarily observed in recovered animals, suggesting perturbation of the dentate through surgery-related tissue trauma influences both LTD incidence and LTP induction at PP-DG synapses in vivo.

摘要

突触长时程抑制( LTD )的表达被认为在维持记忆功能中起关键作用。我们对齿状回(DG )外侧( LPP )和内侧穿通路径( MPP )突触 LTD 表达的体内研究证实了先前的研究结果,即在完整动物中很难诱导 PP-DG LTD 。在自由活动的动物中, LPP-DG 和 MPP-DG 反应之间的 LTD 表达不一致。有趣的是,在麻醉大鼠急性电极植入后,低频刺激( LFS ; 900 个脉冲, 1Hz )可促进 MPP-DG 和 LPP-DG 突触的缓慢起始 LTP ,而这些突触使用不同的诱导机制。在 LFS 之前 90 分钟系统给予 N-甲基-D-天冬氨酸( NMDA )受体拮抗剂( +/- )-环丙哌啶-6-哌啶嗪( CPP ; 10mg/kg )选择性阻断 MPP-DG ,但不阻断 LPP-DG 缓慢起始 LTP ,表明 MPP-DG 突触表达 NMDA 受体依赖性缓慢起始 LTP ,而 LPP-DG 缓慢起始 LTP 诱导与 NMDA 受体无关。在使用配对脉冲 LFS ( 900 对脉冲, 200ms 对脉冲间隔)诱导 LTD 的实验中, LPP 的配对脉冲 LFS 导致 DG 反应的快速起始 LTP ,而 MPP 的配对脉冲 LFS 诱导 DG 反应的缓慢起始 LTP 。尽管在麻醉大鼠急性电极植入后很少观察到 LTD ,但在先前植入电极的一些麻醉大鼠中也证明了 LPP-DG LTD 。总之,我们的数据表明,体内 PP-DG LTD 表达是一种不一致的现象,主要在恢复的动物中观察到,这表明与手术相关的组织创伤对齿状回的干扰既影响 LTD 的发生率,也影响体内 PP-DG 突触的 LTP 诱导。

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