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突触可塑性简化生物物理模型的汇聚证据。

Converging evidence for a simplified biophysical model of synaptic plasticity.

作者信息

Shouval Harel Z, Castellani Gastone C, Blais Brian S, Yeung Luk C, Cooper Leon N

机构信息

Institute for Brain and Neural Systems, Brown University, 02912, USA.

出版信息

Biol Cybern. 2002 Dec;87(5-6):383-91. doi: 10.1007/s00422-002-0362-x.

Abstract

Different mechanisms that could form the molecular basis for bi-directional synaptic plasticity have been identified experimentally and corresponding biophysical models can be constructed. However, such models are complex and therefore it is hard to deduce their consequences to compare them to existing abstract models of synaptic plasticity. In this paper we examine two such models: a phenomenological one inspired by the phenomena of AMPA receptor insertion, and a more complex biophysical model based on the phenomena of AMPA receptor phosphorylation. We show that under certain approximations both these models can be mapped on to an equivalent, calcium-dependent, differential equation. Intracellular calcium concentration varies locally in each postsynaptic compartment, thus the plasticity rule we extract is a single-synapse rule. We convert this single synapse plasticity equation to a multi-synapse rule by incorporating a model of the NMDA receptor. Finally we suggest a mathematical embodiment of metaplasticity, which is consistent with observations on NMDA receptor properties and dependence on cellular activity. These results, in combination with some of our previous results, produce converging evidence for the calcium control hypothesis including a dependence of synaptic plasticity on the level of intercellular calcium as well as on the temporal pattern of calcium transients.

摘要

实验已确定了可构成双向突触可塑性分子基础的不同机制,并能构建相应的生物物理模型。然而,此类模型很复杂,因此难以推断其结果并与现有的突触可塑性抽象模型进行比较。在本文中,我们研究了两个这样的模型:一个受AMPA受体插入现象启发的唯象模型,以及一个基于AMPA受体磷酸化现象的更复杂的生物物理模型。我们表明,在某些近似条件下,这两个模型都可以映射到一个等效的、钙依赖的微分方程。细胞内钙浓度在每个突触后小室中局部变化,因此我们提取的可塑性规则是一个单突触规则。通过纳入NMDA受体模型,我们将这个单突触可塑性方程转换为多突触规则。最后,我们提出了一种元可塑性的数学体现,它与关于NMDA受体特性及其对细胞活动依赖性的观察结果一致。这些结果与我们之前的一些结果相结合,为钙控制假说提供了越来越多的证据,包括突触可塑性对细胞间钙水平以及钙瞬变时间模式的依赖性。

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