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首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Pattern-specific associative long-term potentiation induced by a sleep spindle-related spike train.
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Pattern-specific associative long-term potentiation induced by a sleep spindle-related spike train.

机译:由与睡眠纺锤相关的尖峰序列诱导的模式特异的关联性长期增强。

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摘要

Spindles are non-rapid eye movement (non-REM) sleep EEG rhythms (7-14 Hz) that occur independently or in association with slow oscillations (0.6-0.8 Hz). Despite their proposed function in learning and memory, their role in synaptic plasticity is essentially unknown. We studied the ability of a neuronal firing pattern underlying spindles in vivo to induce synaptic plasticity in neocortical pyramidal cells in vitro. A spindle stimulation pattern (SSP) was extracted from a slow oscillation upstate that was recorded in a cat anesthetized with ketamine-xylazine, which is known to induce a sleep-like state. To mimic the recurrence of spindles grouped by the slow oscillation, the SSP was repeated every 1.5 s (0.6 Hz). Whole-cell patch-clamp recordings were obtained from layer V pyramidal cells of rat somatosensory cortex with infrared videomicroscopy, and composite EPSPs were evoked within layers II-III. Trains of EPSPs and action potentials simultaneously triggered by the SSP induced an NMDA receptor-dependent short-term potentiation (STP) and an L-type Ca2+ channel-dependent long-term potentiation (LTP). The number of spindle sequences affected the amount of STP-LTP. In contrast, spindle trains of EPSPs alone led to long-term depression. LTP was not consistently induced by a regular firing pattern, a mirrored SSP, or a randomized SSP; however, a synthetic spindle pattern consisting of repetitive spike bursts at 10 Hz reliably induced STP-LTP. Our results show that spindle-associated spike discharges are efficient in modifying excitatory neocortical synapses according to a Hebbian rule. This is in support of a role for sleep spindles in memory consolidation.
机译:纺锤体是非快速眼动(non-REM)睡眠脑电图节律(7-14 Hz),其独立发生或与缓慢振荡相关(0.6-0.8 Hz)。尽管它们在学习和记忆中具有拟议的功能,但它们在突触可塑性中的作用基本上是未知的。我们研究了体内纺锤体下神经元放电模式在体外诱导新皮质锥体细胞中突触可塑性的能力。从缓慢振荡的上升状态中提取纺锤体刺激模式(SSP),该状态记录在用氯胺酮-甲苯噻嗪麻醉的猫中,已知它会诱发类似睡眠的状态。为了模拟由缓慢振荡分组的纺锤的重复出现,每1.5 s(0.6 Hz)重复SSP。使用红外视频显微镜从大鼠体感皮层的V层锥体细胞获得全细胞膜片钳记录,并在II-III层中诱发复合EPSP。由SSP同时触发的一系列EPSP和动作电位诱导了NMDA受体依赖性短期增强(STP)和L型Ca2 +通道依赖性长期增强(LTP)。纺锤序列的数量影响STP-LTP的数量。相反,仅EPSP的主轴列会导致长期抑郁。 LTP不是由规则的发射模式,镜像的SSP或随机的SSP一致诱导产生的;但是,由10 Hz的重复尖峰脉冲组成的合成主轴模式可以可靠地诱发STP-LTP。我们的研究结果表明,纺锤体相关的尖峰放电可有效地根据Hebbian规则修饰兴奋性新皮层突触。这支持了睡眠心轴在内存整合中的作用。

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