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Spine microdomains for postsynaptic signaling and plasticity

机译:脊柱微区的突触后信号和可塑性。

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Changes in the molecular composition and signaling properties of excitatory glutamatergic synapses onto dendritic spines mediate learning-related plasticity in the mammalian brain. This molecular adaptation serves as the most celebrated cell biological model for learning and memory. Within their micron-sized dimensions, dendritic spines restrict the diffusion of signaling molecules and spatially confine the activation of signal transduction pathways. Much of this local regulation occurs by spatial compartmentalization of glutamate receptors. Here, we review recently identified cell biological mechanisms regulating glutamate receptor mobility within individual dendritic spines. We discuss the emerging functions of glutamate receptors residing within sub-spine microdomains and propose a model for distinct signaling platforms with specialized functions in synaptic plasticity.
机译:兴奋性谷氨酸能突触到树突棘的分子组成和信号传导特性的变化介导了哺乳动物脑中与学习相关的可塑性。这种分子适应性是最著名的学习和记忆细胞生物学模型。在其微米大小的尺寸内,树突棘限制了信号分子的扩散,并在空间上限制了信号转导通路的激活。这种局部调节的大部分是通过谷氨酸受体的空间分隔而发生的。在这里,我们回顾了最近确定的调节个体树突棘内谷氨酸受体迁移的细胞生物学机制。我们讨论了位于亚脊柱微域内的谷氨酸受体的新兴功能,并提出了具有特殊功能的突触可塑性的不同信号平台的模型。

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