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Modulating the excitability of the visual cortex using a stimulation priming paradigm

机译:使用刺激引发范例调节视觉皮质的兴奋性

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BackgroundTranscranial random noise stimulation (tRNS) can cause long term increase of corticospinal excitability when used to prime the motor cortex, before measuring the motor response in the hand muscles with TMS (Terney et al., 2008). In cognitive studies, tRNS has been used to improve visual attention and mathematical skills, an enhancement effect that might suggest sustained cortical plasticity changes (Cappelletti et al., 2013; ). However, while the behavioral evidence of increased performance is becoming substantiated by empirical data, it still remains unclear whether tRNS over visual areas causes an increase in cortical excitability similar to what has been found in the motor cortex, and if that increase could be a potential physiological explanation for behavioral improvements found in visual tasks. Objective/hypothesisIn the present study, we aimed to investigate whether priming the visual cortex with tRNS leads to increased and sustained excitability as measured with visual phosphenes. MethodsWe measured phosphene thresholds (PTs) using an objective staircase method to quantify the magnitude of cortical excitability changes. Single-pulse TMS was used to elicit phosphenes before, immediately after, and every 10?min up to one hour after the end of 20?min tRNS, anodal tDCS (a-tDCS) or sham. ResultsResults showed that phosphene thresholds were significantly reduced up to 60?min post stimulation relative to baseline after tRNS, a behavioral marker of increased excitability of the visual cortex, while a-tDCS had no effect. This result is very similar in magnitude and duration to what has been found in the motor cortex. ConclusionsOur findings demonstrate promising potential of tRNS as a tool to increase and sustain cortical excitability to promote improvement of cognitive functions.
机译:背景技术当使用TMS肌肉中的电动机响应之前,在用TMS中的电动机响应之前,可以导致动机皮质的动机响应(Terney等,2008)中的电动机响应,导致动机皮质的长期兴奋性长期增加。在认知研究中,TRNS已被用于提高视觉关注和数学技能,这一增强效果可能会提出持续的皮质可塑性变化(Cappelletti等,2013;)。然而,虽然性能增加的行为证据是通过经验数据证实的,但仍然尚不清楚视觉区域的TRNS是否导致皮质兴奋的增加,而这种兴奋性类似于在电机皮质中发现的内容,并且如果增加可能是潜力视觉任务中发现的行为改进的生理解释。目的/假设本研究,我们旨在研究与TRNS的视觉皮质引发是否促使视觉皮质导致随着可视磷酸化测量的增加和持续的兴奋性。方法网络使用目标阶梯法测定磷烯阈值(PTS),以量化皮质兴奋性变化的大小。单脉冲TMS用于之前,在20?min TRNS末端,anoodal TDC(A-TDCS)或假的1小时后,每10次,每10次,每10次,每10次,以前。结果结果表明,在TRNS后,磷烯阈值显着降低了60?最小的刺激后刺激,这是对视觉皮质的兴奋性增加的行为标志物,而A-TDC没有效果。该结果的幅度和持续时间非常相似,在电机皮质中发现的持续时间。结论调查结果表明,TRNS作为一种增加和维持皮质兴奋的工具,以促进改善认知功能的工具。

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