光控单突触激活对 AMPA 受体运输和降解的稳态调节。
Homeostatic regulation of AMPA receptor trafficking and degradation by light-controlled single-synaptic activation.
机构信息
Department of Biology, Boston University, 5 Cummington Street, Boston, MA 02215, USA.
出版信息
Neuron. 2011 Dec 8;72(5):806-18. doi: 10.1016/j.neuron.2011.10.011.
Abstract
During homeostatic adjustment in response to alterations in neuronal activity, synaptic expression of AMPA receptors (AMPARs) is globally tuned up or down so that the neuronal activity is restored to a physiological range. Given that a central neuron receives multiple presynaptic inputs, whether and how AMPAR synaptic expression is homeostatically regulated at individual synapses remain unclear. In cultured hippocampal neurons we report that when activity of an individual presynaptic terminal is selectively elevated by light-controlled excitation, AMPAR abundance at the excited synapses is selectively downregulated in an NMDAR-dependent manner. The reduction in surface AMPARs is accompanied by enhanced receptor endocytosis and dependent on proteasomal activity. Synaptic activation also leads to a site-specific increase in the ubiquitin ligase Nedd4 and polyubiquitination levels, consistent with AMPAR ubiquitination and degradation in the spine. These results indicate that AMPAR accumulation at individual synapses is subject to autonomous homeostatic regulation in response to synaptic activity.
摘要
在响应神经元活动变化的体内平衡调节过程中,AMPA 受体(AMPAR)的突触表达会被全局上调或下调,从而使神经元活动恢复到生理范围。鉴于中枢神经元接收多个突触前输入,单个突触处的 AMPAR 突触表达是否以及如何进行体内平衡调节仍不清楚。在培养的海马神经元中,我们报告称,当通过光控激发选择性地升高单个突触前末梢的活动时,兴奋突触处的 AMPAR 丰度会以 NMDA 受体依赖性方式选择性地下调。表面 AMPAR 的减少伴随着受体内吞作用的增强,并且依赖于蛋白酶体活性。突触激活还导致泛素连接酶 Nedd4 和多泛素化水平的特异性增加,与棘突中的 AMPAR 泛素化和降解一致。这些结果表明,单个突触处的 AMPAR 积累会针对突触活动进行自主的体内平衡调节。
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