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Thalamic model of awake alpha oscillations and implications for stimulus processing

机译:清醒的α振荡的丘脑模型及其对刺激处理的影响

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We describe a unique conductance-based model of awake thalamic alpha and some of its implications for function. The full model includes a model for a specialized class of high-threshold thalamo-cortical cells (HTC cells), which burst at the alpha frequency at depolarized membrane potentials (~-56 mV). Our model generates alpha activity when the actions of either muscarinic acetylcholine receptor (mAChR) or metabotropic glutamate receptor 1 (mGluRI) agonists on thalamic reticular (RE), thalamocortical (TC), and HTC cells are mimicked. In our model of mGluRI-induced alpha, TC cells are equally likely to fire during any phase of alpha, consistent with in vitro experiments. By contrast, in our model of mAChR-induced alpha, TC cells tend to fire either at the peak or the trough of alpha, depending on conditions. Our modeling suggests that low levels of mGluRI activation on a background of mAChR agonists may be able to initiate alpha activity that biases TC cells to fire at certain phases of alpha, offering a pathway for cortical control. If we introduce a strong stimulus by increasing the frequency of excitatory post-synaptic potentials (EPSPs) to TC cells, an increase in alpha power is needed to mimic the level of phasing of TC cells observed in vivo. This increased alpha power reduces the probability that TC cells spike near the trough of alpha. We suggest that mAChR-induced alpha may contribute to grouping TC activity into discrete perceptual units for processing, whereas mGluRI-induced alpha may serve the purpose of blocking unwanted stimuli from reaching the cortex.
机译:我们描述了一个独特的基于电导的清醒丘脑α模型及其对功能的某些影响。完整的模型包括一个专门的高阈值丘脑皮质细胞(HTC细胞)模型,该模型在去极化膜电位(〜-56 mV)下以α频率爆炸。当模仿毒蕈碱型乙酰胆碱受体(mAChR)或代谢型谷氨酸受体1(mGluRI)激动剂对丘脑网状细胞(RE),丘脑皮质(TC)和HTC细胞的作用时,我们的模型会产生alpha活性。在我们的mGluRI诱导的α模型中,与体外实验一致,TC细胞在α的任何阶段均可能激发。相比之下,在我们的mAChR诱导的α模型中,取决于条件,TC细胞倾向于在α的高峰或低谷激发。我们的模型表明,在mAChR激动剂的背景下,低水平的mGluRI激活可能能够启动α活性,从而使TC细胞偏向在α的某些阶段着火,从而为皮层控制提供了途径。如果我们通过增加对TC细胞的兴奋性突触后电位(EPSP)的频率引入强烈刺激,则需要增加α功率来模仿体内观察到的TC细胞的定相水平。这种增加的alpha功率降低了TC细胞在alpha谷附近刺突的可能性。我们建议,mAChR诱导的alpha可能有助于将TC活性分组为离散的感知单位进行处理,而mGluRI诱导的alpha可能起到阻止不需要的刺激到达皮层的目的。

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