首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Actions of endogenous opioids on NMDA receptor-independent long-term potentiation in area CA3 of the hippocampus.
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Actions of endogenous opioids on NMDA receptor-independent long-term potentiation in area CA3 of the hippocampus.

机译:内源性阿片类药物对海马CA3区NMDA受体非依赖性长时程增强的作用。

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摘要

The opioid peptides represent a major class of neurotransmitter in the vertebrate nervous system and are prevalent in the hippocampus. There is considerable interest in the physiological function of the opioids contained in the mossy fiber pathway. The release of opioids from mossy fibers shows a strong frequency dependence. Long-term potentiation (LTP) at this synapse, an NMDA receptor-independent form of LTP, also depends on high-frequency synaptic activity, and this has led to speculation that endogenous opioids may be a critical factor in LTP induction. Previous reports using extracellular recordings have provided evidence for and against a role for opioids in mossy fiber LTP. Using single-cell recording techniques, we have tested the hypothesis that endogenous opioids are required for mossy fiber LTP induction. We recorded from a defined population of synapses that had EPSCs with fast rise times, short latencies, and monophasic decays, consistent with a proximally terminating synapse. The opioid antagonist naloxone prevented mossy fiber LTP in the rat, but had no effect on the commissural/associational system, a nonopioid-containing pathway. The action of naloxone was not mediated through disinhibition because GABAA receptors were pharmacologically blocked in these experiments. We also tested the hypothesis that variations in postsynaptic receptor subtype distribution between species might explain previous controversies regarding the role of endogenous opioids. In contrast to the rat, LTP of the mossy fiber field potential in guinea pig was not blocked by naloxone. Our data suggest that opioids may be the presynaptically released, frequency-dependent, associative factor for mossy fiber LTP induction.
机译:阿片样物质肽代表脊椎动物神经系统中的一类主要的神经递质,在海马中普遍存在。苔藓纤维途径中包含的阿片样物质的生理功能引起了极大的兴趣。从长满苔藓的纤维中释放的阿片类药物显示出强烈的频率依赖性。 NMDA受体非依赖性LTP形式的这种突触的长时程增强(LTP)也取决于高频突触活性,这导致人们推测内源性阿片类药物可能是LTP诱导的关键因素。以前使用细胞外录音的报道为阿片类药物在长满苔藓的纤维LTP中的作用提供了支持和反对的证据。使用单细胞记录技术,我们已经测试了长生苔纤维LTP诱导需要内源性阿片类药物的假说。我们从已定义的突触群体中进行记录,这些突触具有EPSC,且上升时间短,潜伏期短,单相衰减,与近端终止的突触一致。阿片样物质拮抗剂纳洛酮可预防大鼠的苔藓纤维LTP,但对连合/结合系统(一种非阿片类药物途径)没有影响。纳洛酮的作用不是通过抑制作用来介导的,因为在这些实验中,GABAA受体在药理上被阻断。我们还检验了以下假设:物种之间的突触后受体亚型分布变化可能解释了先前关于内源性阿片类药物作用的争议。与大鼠相反,豚鼠的苔藓纤维场电位的LTP未被纳洛酮所阻断。我们的数据表明,阿片类药物可能是苔藓纤维LTP诱导的突触前释放的,频率依赖性的相关因子。

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