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条件性疼痛调制、安慰剂和抵消性镇痛:抑制性、无反应性和易化性疼痛调制效应的行为表达率

Conditioned Pain Modulation, Placebo and Offset Analgesia: Rates of Behavioural Expression of Inhibitory, Nonresponse and Facilitatory Pain Modulatory Effects.

作者信息

Crawford Lewis S, Wake Ashleigh, Robertson Rebecca V, Peng Allan, Meylakh Noemi, Boorman Damien C, Sattarov Leana, Ramachandran Alister, Macefield Vaughan G, Keay Kevin A, Henderson Luke A

机构信息

School of Medical Sciences (Neuroscience), Brain and Mind Centre, University of Sydney, Sydney, New South Wales, Australia.

Westmead Hospital Pain Management Centre, Sydney, New South Wales, Australia.

出版信息

Eur J Pain. 2025 Aug;29(7):e70088. doi: 10.1002/ejp.70088.

Abstract

BACKGROUND

The brain is capable of powerfully inhibiting perceived pain intensity. Experimentally, three pain modulating phenomena have been well explored: placebo analgesia (PA), offset analgesia (OA) and conditioned pain modulation (CPM). While all three can reduce pain intensity, these paradigms are not often compared behaviourally, nor are their potentially common psychological or physiological mechanisms considered.

METHODS

Here, we present retrospective behavioural pain rating, psychological and demographic data in 273 pain-free control participants who underwent either PA (n = 100), OA (n = 37) or CPM (n = 136). Significant changes in pain intensities were assessed using permutation testing to derive cohorts where pain was significantly inhibited (inhibitory responders), unchanged (nonresponder) or increased (facilitatory responder) during the expression of each phenomenon. Psychological questionnaire scores, demography and pain perception variability were compared between response cohorts to all three phenomena.

RESULTS

We identified largely similar proportions of individuals categorised as either inhibitory responders, nonresponders or facilitatory responders to each of PA, OA and CPM-with no sex differences identified in any phenomena nor response category. Dispositional optimism and calibrated noxious temperature demonstrated a significant effect in PA and CPM responses, respectively-with inhibitory responders recording higher scores than facilitatory responders in PA, and inhibitory responders possessing lower thermal sensitivity to nonresponders in CPM.

CONCLUSION

A shared mechanism was identified between PA and OA, such that perceived pain variability to repeated identical noxious stimuli related to both phenomena's expression. This warrants further investigation given the suggested neural circuit differences between these two phenomena, and only PA is presently linked with Bayesian theorem.

SIGNIFICANCE STATEMENT

Humans are capable of inhibiting their own pain in several ways; however, the brain systems driving these analgesic mechanisms are complex and are known to diverge despite producing similar outcomes. Here we show core behavioural similarities between different forms of endogenous analgesic phenomena, with differences in psychological and physiological correlates.

摘要

背景

大脑能够有力地抑制所感知到的疼痛强度。在实验中,三种疼痛调节现象已得到充分研究:安慰剂镇痛(PA)、抵消性镇痛(OA)和条件性疼痛调节(CPM)。虽然这三种现象都能减轻疼痛强度,但这些范式在行为学上并不常被比较,其潜在的共同心理或生理机制也未被考虑。

方法

在此,我们呈现了273名无痛对照参与者的回顾性行为疼痛评分、心理和人口统计学数据,这些参与者分别接受了PA(n = 100)、OA(n = 37)或CPM(n = 136)。使用置换检验评估疼痛强度的显著变化,以确定在每种现象表达期间疼痛被显著抑制(抑制性反应者)、未改变(无反应者)或增加(易化性反应者)的队列。比较了对所有三种现象的反应队列之间的心理问卷分数、人口统计学和疼痛感知变异性。

结果

我们发现,被归类为PA, OA和CPM的抑制性反应者、无反应者或易化性反应者的个体比例在很大程度上相似,在任何现象或反应类别中均未发现性别差异。气质性乐观和校准后的有害温度分别在PA和CPM反应中显示出显著影响,在PA中,抑制性反应者的得分高于易化性反应者,在CPM中,抑制性反应者对无反应者的热敏感性较低。

结论

在PA和OA之间发现了一种共同机制,即对重复相同有害刺激的疼痛感知变异性与这两种现象的表达有关。鉴于这两种现象之间存在神经回路差异,且目前只有PA与贝叶斯定理相关联,因此有必要进一步研究。

意义声明

人类能够通过多种方式抑制自身疼痛;然而,驱动这些镇痛机制的脑系统很复杂,尽管产生相似的结果,但已知它们存在差异。在这里,我们展示了不同形式的内源性镇痛现象之间的核心行为相似性,以及心理和生理相关性的差异。

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