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脊髓长期增强作用与大鼠大脑中阿片类神经传递减少有关。

Spinal long-term potentiation is associated with reduced opioid neurotransmission in the rat brain.

作者信息

Hjornevik Trine, Schoultz Bent W, Marton János, Gjerstad Johannes, Drzezga Alexander, Henriksen Gjermund, Willoch Frode

机构信息

Centre for Molecular Biology and Neuroscience & Institute of Basic Medical Sciences, University of Oslo, Oslo, Norway.

出版信息

Clin Physiol Funct Imaging. 2010 Jul;30(4):285-93. doi: 10.1111/j.1475-097X.2010.00939.x.

Abstract

INTRODUCTION

Neuronal events leading to development of long-term potentiation (LTP) in the nociceptive pathways may be a cellular mechanism underlying hyperalgesia. In the present study, we examine if induction of spinal LTP may be associated with functional changes in the supraspinal opioidergic system. The opioid receptors (ORs) play a key role in nociceptive processing and controlling the descending modulatory system to the spinal cord.

METHODS

Spinal LTP was induced by electrical high-frequency stimulation (HFS) conditioning applied to the sciatic nerve, and the excitability at spinal level was verified by spinal field potential recordings. To study supraspinal changes in opioid neurotransmission following the same HFS conditioning, we used small animal positron emission tomography (PET) and [(11)C]Phenethyl-Orvinol ([(11)C]PEO). All rats included in the PET study were scanned at baseline and 150 min after HFS, and specific binding was calculated with a reference tissue model.

RESULTS

A clear C-fibre LTP, i.e. increased C-fibre response and reduced C-fibre threshold, was observed 150 min after HFS conditioning (t-test, P<0.05, n = 6). Moreover, increased OR binding, relative to baseline, was observed after the same type of HFS conditioning ipsilaterally in the amygdala, hippocampus, somatosensory cortex and superior colliculus, and bilaterally in the nucleus accumbens, caudate putamen and hypothalamus (paired t-test, HFS>baseline, P<0.05, n = 8).

CONCLUSIONS

HFS conditioning of the sciatic nerve resulted in both spinal LTP and functional changes in supraspinal opioidergic signalling. Our findings suggest that induction of spinal LTP may be associated with reduced opioid neurotransmission in brain regions involved in pain modulation and affective-emotional responses.

摘要

引言

伤害性感受通路中导致长时程增强(LTP)形成的神经元事件可能是痛觉过敏的一种细胞机制。在本研究中,我们探究脊髓LTP的诱导是否可能与脊髓上阿片能系统的功能变化相关。阿片受体(ORs)在伤害性感受处理以及控制脊髓下行调节系统中起关键作用。

方法

通过对坐骨神经施加高频电刺激(HFS)来诱导脊髓LTP,并通过脊髓场电位记录来验证脊髓水平的兴奋性。为了研究相同HFS条件下脊髓上阿片类神经传递的变化,我们使用了小动物正电子发射断层扫描(PET)和[(11)C]苯乙基 - 奥维诺([(11)C]PEO)。PET研究中纳入的所有大鼠在基线和HFS后150分钟进行扫描,并使用参考组织模型计算特异性结合。

结果

在HFS条件刺激后150分钟观察到明显的C纤维LTP,即C纤维反应增强和C纤维阈值降低(t检验,P<0.05,n = 6)。此外,在杏仁核、海马体、体感皮层和上丘同侧,以及伏隔核、尾状壳核和下丘脑双侧,在相同类型的HFS条件刺激后观察到相对于基线的OR结合增加(配对t检验,HFS>基线,P<0.05,n = 8)。

结论

坐骨神经的HFS条件刺激导致脊髓LTP和脊髓上阿片能信号传导的功能变化。我们的研究结果表明,脊髓LTP的诱导可能与参与疼痛调节和情感 - 情绪反应的脑区中阿片类神经传递减少有关。

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