首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Neuronal somatic ATP release triggers neuron-satellite glial cell communication in dorsal root ganglia
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Neuronal somatic ATP release triggers neuron-satellite glial cell communication in dorsal root ganglia

机译:神经元体ATP释放触发背根神经节中的神经元-卫星胶质细胞通讯

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摘要

It has been generally assumed that the cell body (soma) of a neuron, which contains the nucleus, is mainly responsible for synthesis of macromolecules and has a limited role in cell-to-cell communication. Using sniffer patch recordings, we show here that electrical stimulation of dorsal root ganglion (DRG) neurons elicits robust vesicular ATP release from their somata. The rate of release events increases with the frequency of nerve stimulation; external Ca~(2+) entry is required for the release. FM1-43 photoconversion analysis further reveals that small clear vesicles participate in exocytosis. In addition, the released ATP activates P2X7 receptors in satellite cells that enwrap each DRG neuron and triggers the communication between neuronal somata and glial cells. Blocking L-type Ca~(2+) channels completely eliminates the neuron-glia communication. We further show that activation of P2X7 receptors can lead to the release of tumor necrosis factor-α (TNFα) from satellite cells. TNFα in turn potentiates the P2X3 receptor-mediated responses and increases the excitability of DRG neurons. This study provides strong evidence that somata of DRG neurons actively release transmitters and play a crucial role in bidirectional communication between neurons and surrounding satellite glial cells. These results also suggest that, contrary to the conventional view, neuronal somata have a significant role in cell-cell signaling.
机译:通常认为,包含核的神经元的细胞体(soma)主要负责大分子的合成,并且在细胞间的通信中作用有限。使用嗅探器贴片录音,我们在这里显示了背根神经节(DRG)神经元的电刺激引起了从其躯体中释放出强大的囊泡ATP。释放事件的速率随着神经刺激频率的增加而增加。释放需要外部Ca〜(2+)条目。 FM1-43光转换分析进一步揭示了小的透明囊泡参与胞吐作用。此外,释放的ATP激活包裹每个DRG神经元的卫星细胞中的P2X7受体,并触发神经元体细胞和神经胶质细胞之间的通讯。阻断L型Ca〜(2+)通道完全消除了神经胶质细胞的通讯。我们进一步表明,P2X7受体的激活可以导致从卫星细胞释放肿瘤坏死因子-α(TNFα)。 TNFα继而增强了P2X3受体介导的反应并增加了DRG神经元的兴奋性。这项研究提供了有力的证据,表明DRG神经元的躯体会主动释放递质,并在神经元与周围的卫星神经胶质细胞之间的双向通讯中发挥关键作用。这些结果还表明,与传统观点相反,神经元躯体在细胞信号转导中具有重要作用。

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