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Neuromodulation of STDP through short-term changes in firing causality

机译:短期因果关系变化对STDP的神经调节

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Spike timing dependent plasticity (STDP) likely plays an important role in forming and changing connectivity patterns between neurons in our brain. In a unidirectional synaptic connection between two neurons, it uses the causal relation between spiking activity of a presynaptic input neuron and a postsynaptic output neuron to change the strength of this connection. While the nature of STDP benefits unsupervised learning of correlated inputs, any incorporation of value into the learning process needs some form of reinforcement. Chemical neuromodulators such as Dopamine or Acetylcholine are thought to signal changes between external reward and internal expectation to many brain regions, including the basal ganglia. This effect is often modelled through a direct inclusion of the level of Dopamine as a third factor into the STDP rule. While this gives the benefit of direct control over synaptic modification, it does not account for observed instantaneous effects in neuronal activity on application of Dopamine agonists. Specifically, an instant facilitation of neuronal excitability in the striatum can not be explained by the only indirect effect that dopamine-modulated STDP has on a neuron's firing pattern. We therefore propose a model for synaptic transmission where the level of neuromodulator does not directly influence synaptic plasticity, but instead alters the relative firing causality between preand postsynaptic neurons. Through the direct effect on postsynaptic activity, our rule allows indirect modulation of the learning outcome even with unmodulated, two-factor STDP. However, it also does not prohibit joint operation together with three-factor STDP rules.
机译:尖峰时序相关可塑性(STDP)可能在形成和改变大脑神经元之间的连接方式中起重要作用。在两个神经元之间的单向突触连接中,它使用突触前输入神经元和突触后输出神经元的尖峰活动之间的因果关系来更改此连接的强度。尽管STDP的性质使相关输入的无监督学习受益,但是将价值纳入学习过程的任何形式都需要某种形式的加强。化学神经调节剂(如多巴胺或乙酰胆碱)被认为可以向许多大脑区域(包括基底神经节)发出外部奖赏和内部期望之间的变化信号。通常通过直接将多巴胺水平作为第三个因素纳入STDP规则来模拟这种效果。虽然这提供了直接控制突触修饰的好处,但它不能解释在应用多巴胺激动剂后神经元活动中观察到的瞬时作用。具体地说,纹状体中神经元兴奋性的即时促进不能通过多巴胺调节的STDP对神经元放电模式的唯一间接作用来解释。因此,我们提出了一种突触传递模型,其中神经调节剂的水平不直接影响突触可塑性,而是改变突触前和突触后神经元之间的相对激发因果关系。通过对突触后活动的直接影响,我们的规则允许对学习结果进行间接调节,即使未调节的两因素STDP也是如此。但是,它也不禁止与三要素STDP规则一起进行联合操作。

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