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An Antibody Feeding Approach to Study Glutamate Receptor Trafficking in Dissociated Primary Hippocampal Cultures

机译:研究离体原代海马培养物中谷氨酸受体贩运的抗体喂养方法。

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摘要

Cellular responses to external stimuli heavily rely on the set of receptors expressed at the cell surface at a given moment. Accordingly, the population of surface-expressed receptors is constantly adapting and subject to strict mechanisms of regulation. The paradigmatic example and one of the most studied trafficking events in biology is the regulated control of the synaptic expression of glutamate receptors (GluRs). GluRs mediate the vast majority of excitatory neurotransmission in the central nervous system and control physiological activity-dependent functional and structural changes at the synaptic and neuronal levels (e.g., synaptic plasticity). Modifications in the number, location, and subunit composition of surface expressed GluRs deeply affect neuronal function and, in fact, alterations in these factors are associated with different neuropathies. Presented here is a method to study GluR trafficking in dissociated hippocampal primary neurons. An “antibody-feeding” approach is used to differentially visualize GluR populations expressed at the surface and internal membranes. By labeling surface receptors on live cells and fixing them at different times to allow for receptors endocytosis and/or recycling, these trafficking processes can be evaluated and selectively studied. This is a versatile protocol that can be used in combination with pharmacological approaches or overexpression of altered receptors to gain valuable information about stimuli and molecular mechanisms affecting GluR trafficking. Similarly, it can be easily adapted to study other receptors or surface expressed proteins.
机译:细胞对外部刺激的反应严重依赖于在给定时刻在细胞表面表达的受体。因此,表面表达受体的群体不断适应并受到严格的调节机制的影响。生物学上最典型的贩运事件之一就是范例,是谷氨酸受体(GluRs)突触表达的调控。 GluRs介导中枢神经系统中绝大多数兴奋性神经传递,并在突触和神经元水平(例如突触可塑性)控制依赖生理活动的功能和结构变化。表面表达的GluR的数量,位置和亚基组成的改变会深深影响神经元功能,实际上,这些因素的改变与不同的神经病变有关。这里介绍的是一种研究离体海马原代神经元中GluR转运的方法。 “抗体补给”方法用于差异显示在表面和内部膜上表达的GluR群体。通过在活细胞上标记表面受体并在不同时间固定它们,以使受体内吞和/或回收,可以评估和选择性研究这些运输过程。这是一种通用协议,可以与药理学方法或改变的受体的过表达结合使用,以获得有关影响GluR转运的刺激和分子机制的有价值的信息。同样,它可以轻松地用于研究其他受体或表面表达的蛋白质。

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