脑α峰频率:与慢性疼痛发作和疼痛调节的关系

Q2 Medicine
Felicitas A. Huber , Parker A. Kell , Joanna O. Shadlow , Jamie L. Rhudy
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引用次数: 0

摘要

慢性疼痛在美国非常普遍,并导致无数的负面后遗症和痛苦。解决慢性疼痛的一种方法是确定谁处于危险之中,并在症状发作之前进行干预。研究表明,在疼痛敏感性较高的健康个体和慢性疼痛患者中,静息α峰值频率(PAF),即静息时α振荡的速度较慢。因此,较慢的PAF可能表示慢性疼痛易感性。其他研究表明,慢性疼痛风险较高的个体表现出疼痛调节紊乱,即疼痛抑制效率较低,疼痛促进能力增强。目前,PAF预测慢性疼痛的能力及其与疼痛调节的关系研究尚不充分。本研究旨在通过表征PAF、慢性疼痛发作和疼痛调节之间的关系来解决这一差距。利用三个独立研究的档案数据,本研究评估了PAF减慢是否与预期确定的慢性疼痛发作、疼痛抑制减弱(即条件性疼痛调节受损、性诱发疼痛抑制受损)和疼痛促进增强(即疼痛时间累积增加、残肢诱发疼痛促进增强)相关。结果表明,较慢的PAF与脊柱(即伤害性屈曲反射)和棘上(即N2电位)对不愉快图像(即人体损伤图像)的伤害感觉的更大促进有关。这表明,较慢的PAF与威胁增强的脊髓和椎管上伤害感觉有关,可能与威胁系统中断的慢性疼痛有关。较慢的PAF与任何其他疼痛结果无关,包括前瞻性确定的慢性疼痛发作。然而,慢性疼痛的发作只能在一项研究中通过混合睁眼/闭眼记录进行评估,限制了这一发现的意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Cerebral peak alpha frequency: Associations with chronic pain onset and pain modulation
Chronic pain is highly prevalent in the U.S. and leads to myriad negative sequalae and suffering. One way to address chronic pain is to identify who is at risk and intervene prior to symptom onset. Research suggests resting peak alpha frequency (PAF), the speed of alpha oscillations at rest, is slower in healthy individuals with greater pain sensitivity and in chronic pain patients. Thus, slower PAF may denote chronic pain vulnerability. Other research has shown that individuals at higher risk of chronic pain exhibit disrupted pain modulation, i.e., less efficient pain inhibition and increased pain facilitation. Currently, the ability of PAF to predict chronic pain and its relation to pain modulation is under-researched. This investigation aimed to address this gap by characterizing associations between PAF, onset of chronic pain, and pain modulation. Using archival data from three independent studies, this investigation assessed whether slower PAF is associated with prospectively-determined chronic pain onset, decreased pain inhibition (i.e., impaired conditioned pain modulation, impaired erotica-induced pain inhibition), and increased pain facilitation (i.e., increased temporal summation of pain, augmented mutilation-induced pain facilitation). Results show that slower PAF was associated with greater facilitation of spinal (i.e., nociceptive flexion reflex) and supraspinal (i.e., N2 potential) nociception in response to unpleasant pictures (i.e., human injury images). This suggests that slower PAF is associated with threat-enhanced spinal and supraspinal nociception and may be relevant for chronic pain conditions with disrupted threat systems. Slower PAF was not associated with any other pain outcome, including prospectively determined chronic pain onset. However, chronic pain onset could only be assessed in one study with a mixed eyes open/eyes closed recording, limiting the significance of this finding.
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来源期刊
Neurobiology of Pain
Neurobiology of Pain Medicine-Anesthesiology and Pain Medicine
CiteScore
4.40
自引率
0.00%
发文量
29
审稿时长
54 days
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