首页> 美国卫生研究院文献>Frontiers in Pharmacology >Analgesic Effects of Triterpenoid Saponins From Stauntonia chinensis via Selective Increase in Inhibitory Synaptic Response in Mouse Cortical Neurons
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Analgesic Effects of Triterpenoid Saponins From Stauntonia chinensis via Selective Increase in Inhibitory Synaptic Response in Mouse Cortical Neurons

机译:鼠皮层神经元中选择性抑制抑制突触反应的增加,从五木中提取的三萜皂苷具有镇痛作用。

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摘要

Triterpenoid saponins from Stauntonia chinensis (TSS) are potential therapeutic agents because of its analgesic properties. However, the underlying mechanisms of the anti-nociceptive activity of TSS are largely unclear, especially in CNS. The present study confirmed the analgesic effect of TSS using four models of acute pain based on thermal or chemical stimuli. TSS treatment specifically impaired the threshold of thermal- and chemical-stimulated acute pain. Naloxone did not block the anti-nociceptive effects of TSS, which showed no participation of the opioid system. We investigated the electrical signal in cultured cortical neurons to explore whether TSS treatment directly affected synaptic transmission. TSS treatment selectively increased spontaneous inhibitory synaptic release and GABA induced charge transfer in mouse cortical neurons. The effects of TSS were maintained for at least 8 h in cultured neurons and in injected mice. Taken together, our results suggest that the analgesic role of TSS in cortex occurs via a particular increase in the inhibitory synaptic response at resting state, which supports TSS as a potential candidate for inflammatory pain relief.
机译:由于其镇痛作用,来自中国金盏花(TSS)的三萜皂苷是潜在的治疗剂。然而,TSS的抗伤害感受活性的潜在机制在很大程度上尚不清楚,尤其是在CNS中。本研究使用基于热或化学刺激的四种急性疼痛模型证实了TSS的镇痛作用。 TSS治疗特别损害了热刺激和化学刺激的急性疼痛的阈值。纳洛酮没有阻止TSS的抗伤害感受作用,表明没有阿片样物质系统的参与。我们调查了培养的皮质神经元中的电信号,以探讨TSS治疗是否直接影响突触传递。 TSS处理选择性增加了小鼠皮质神经元的自发抑制性突触释放和GABA诱导的电荷转移。在培养的神经元和注射的小鼠中,TSS的作用至少维持8小时。两者合计,我们的结果表明,TSS在皮质中的镇痛作用是通过静息状态下抑制性突触反应的特别增加而发生的,这支持了TSS作为炎症性疼痛缓解的潜在候选者。

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