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Acute nociceptive stimuli rapidly induce the activity of serotonin and noradrenalin neurons in the brain stem of awake mice

机译:急性伤害性刺激迅速唤醒清醒小鼠脑干中的5-羟色胺和去甲肾上腺素神经元活性

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摘要

Nociception is an important type of perception that has major influence on daily human life. There are some descending pathways related to pain management and modulation, which are collectively known as the descending antinociceptive system (DAS). Noradrenalin (NA) in the locus coeruleus (LC) and serotonin (5-HT) in the rostral ventromedial medulla (RVM) are components of the DAS. Most 5-HT neurons in the dorsal raphe (DR) have ascending projections rather than descending projections, and they project to the thalamus that modulates nociception. Both the DAS and the DR are believed to be involved in pain-emotion symptoms. In this study, we utilized a fiber photometry system to specifically examine the activity of LC NA neurons and RVM/DR 5-HT neurons using mice carrying tetracycline-controlled transactivator transgene (tTA) under the control of either a dopamine β-hydroxylase promoter or a tryptophan hydroxylase-2 promoter and site-specific infection of an adeno-associated virus carrying a TetO G-CaMP6 gene. After confirmation of specific expression of G-CaMP6 in the target populations, changes in green fluorescent signal intensity were recorded in awake mice upon exposure to acute nociceptive stimulation consisting of a pinch and application of heat (55 °C) to the tail. Both stimuli resulted in rapid and transient (<15 s) increases in the activity of LC NA neurons and RVM/DR 5-HT neurons while the control stimuli did not induce any changes. The present results clearly indicate that acute nociceptive stimuli increase the activity of LC NA neurons and RVM/DR 5 H T neurons and suggest a possible therapeutic target for pain treatment.
机译:伤害感受是一种重要的感知类型,会对日常生活产生重大影响。有一些与疼痛控制和调节有关的下降途径,统称为下降抗伤害感受系统(DAS)。 DAS的组成部分是蓝斑脑(LC)中的去甲肾上腺素(NA)和延髓腹侧延髓(RVM)中的5-羟色胺(5-HT)。背脊(DR)中的大多数5-HT神经元具有递增的投影而不是递减的投影,并且它们投射到调节伤害感受的丘脑。 DAS和DR均被认为与疼痛感症状有关。在这项研究中,我们利用纤维光度测定系统,通过在多巴胺β-羟化酶启动子或多巴胺β-羟化酶启动子的控制下携带四环素控制的反式激活子转基因(tTA)的小鼠,专门检查LC NA神经元和RVM / DR 5-HT神经元的活性。色氨酸羟化酶2启动子和带有TetO G-CaMP6基因的腺相关病毒的定点感染。在确认目标人群中G-CaMP6的特异性表达后,在清醒的小鼠受到急性伤害性刺激(包括捏和向尾巴加热(55°C))后记录了绿色荧光信号强度的变化。两种刺激均导致LC NA神经元和RVM / DR 5-HT神经元的活动快速且短暂(<15 s)增加,而对照刺激未引起任何变化。目前的结果清楚地表明,急性伤害性刺激会增加LC NA神经元和RVM / DR 5 H T神经元的活性,并为疼痛治疗提供可能的治疗靶点。

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