首页> 美国卫生研究院文献>The Journal of Neuroscience >NMDA Receptor Blockade Maintains Correlated Motor Neuron Firing and Delays Synapse Competition at Developing Neuromuscular Junctions
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NMDA Receptor Blockade Maintains Correlated Motor Neuron Firing and Delays Synapse Competition at Developing Neuromuscular Junctions

机译:NMDA受体阻滞维持相关的运动神经元放电并延缓神经肌肉连接处突触竞争。

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摘要

Mammalian neuromuscular synapses undergo an activity-dependent competitive transition from multiple to single innervation during postnatal life. The presence of temporally correlated motor neuron activity, which, in part, is controlled by gap junctional coupling within the spinal cord, appears to modulate synapse elimination. Postnatal injection of dizocilpine maleate (MK801), a specific NMDA antagonist, has been shown to maintain gap junctional coupling among motor neurons. Thus, we tested the hypothesis that MK801 would maintain correlated motor neuron activity and delay postnatal synapse elimination. Temporally correlated motor neuron activity, which is normally lost during the second postnatal week, was maintained and synaptic competition was delayed by several days in 2-week-old mice injected daily with MK801. MK801 appears to modulate motor neuron activity patterns through enhancing mRNA expression of multiple connexins within the spinal cord and delaying motor neuron growth. Our results suggest that MK801 injection preserves correlated neural activity via both synaptic mechanisms and maintenance of gap junctional coupling among neurons within the spinal cord, ultimately delaying synapse elimination.
机译:产后生活中,哺乳动物的神经肌肉突触经历了从多次神经支配到单一神经支配的活动依赖性竞争转变。时间相关的运动神经元活动的存在,部分地受脊髓内间隙连接偶联的控制,似乎调节突触消除。产后注射马来酸地佐西平(MK801)(一种特定的NMDA拮抗剂)已显示出可以维持运动神经元之间的间隙连接偶联。因此,我们测试了MK801将维持相关的运动神经元活动并延迟产后突触消除的假设。在每天注射MK801的2周龄小鼠中,维持了通常在产后第二周丧失的与时间相关的运动神经元活动,并且突触竞争被延迟了几天。 MK801似乎通过增强脊髓内多种连接蛋白的mRNA表达并延迟运动神经元生长来调节运动神经元活动模式。我们的研究结果表明,MK801注射通过突触机制和维持脊髓内神经元之间的间隙连接偶联而保持相关的神经活动,最终延迟了突触的消除。

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