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不良生活事件与疼痛和脊髓伤害感受的内源性抑制之间的关系:来自美国原住民疼痛风险俄克拉荷马研究(OK-SNAP)的研究结果。

The Relationship Between Adverse Life Events and Endogenous Inhibition of Pain and Spinal Nociception: Findings From the Oklahoma Study of Native American Pain Risk (OK-SNAP).

机构信息

Department of Psychology; The University of Tulsa; Tulsa, Oklahoma.

Department of Psychology; The University of Tulsa; Tulsa, Oklahoma.

出版信息

J Pain. 2021 Sep;22(9):1097-1110. doi: 10.1016/j.jpain.2021.03.146. Epub 2021 Apr 2.

Abstract

Adverse life events (ALEs) are a risk factor for chronic pain; however, mechanisms underlying this association are not understood. This study examined whether cumulative ALE exposure impairs endogenous inhibition of pain (assessed from pain report) and spinal nociception (assessed from nociceptive flexion reflex; NFR) in healthy, pain-free Native Americans (n = 124) and non-Hispanic Whites (n = 129) during a conditioned pain modulation (CPM) task. Cumulative ALE exposure was assessed prior to testing by summing the number of potentially traumatic events experienced by each participant across their lifespan. Multilevel modeling found that ALEs were associated with NFR modulation during the CPM task even after controlling for general health, body mass index, sex, age, blood pressure, sleep quality, stimulation intensity, stimulus number, perceived stress, and psychological distress. Low exposure to ALEs was associated with NFR inhibition, whereas high exposure to ALEs was associated with NFR facilitation. By contrast, pain perception was inhibited during the CPM task regardless of the level of ALE exposure. Race/ethnicity did not moderate these results. Thus, ALEs may be pronociceptive for both Native Americans and non-Hispanic Whites by impairing descending inhibition of spinal nociception. This could contribute to a chronic pain risk phenotype involving latent spinal sensitization. PERSPECTIVE: This study found that adverse life events were associated with impaired descending inhibition of spinal nociception in a sample of Native Americans and non-Hispanic Whites. These findings expand on previous research linking adversity to chronic pain risk by identifying a proximate physiological mechanism for this association.

摘要

不良生活事件(ALE)是慢性疼痛的一个风险因素;然而,这种关联的机制尚不清楚。本研究旨在探讨累积 ALE 暴露是否会损害健康、无痛的美洲原住民(n=124)和非西班牙裔白人(n=129)的内源性疼痛抑制(通过疼痛报告评估)和脊髓伤害感受(通过伤害性屈反射;NFR 评估),并在条件性疼痛调制(CPM)任务中进行。在测试前,通过将每位参与者一生中经历的潜在创伤性事件的数量相加,来评估累积 ALE 暴露。多层次模型发现,即使在控制了一般健康状况、体重指数、性别、年龄、血压、睡眠质量、刺激强度、刺激次数、感知压力和心理困扰后,ALE 与 CPM 任务中的 NFR 调制仍相关。低水平的 ALE 暴露与 NFR 抑制相关,而高水平的 ALE 暴露与 NFR 易化相关。相比之下,无论 ALE 暴露水平如何,疼痛感知在 CPM 任务中均受到抑制。种族/民族并没有调节这些结果。因此,ALE 可能通过损害脊髓伤害感受的下行抑制作用,对美洲原住民和非西班牙裔白人都具有致痛作用。这可能导致涉及潜在脊髓致敏的慢性疼痛风险表型。观点:本研究发现,在美洲原住民和非西班牙裔白人群体中,不良生活事件与脊髓伤害感受的下行抑制受损有关。这些发现通过确定这种关联的一个接近的生理机制,扩展了先前将逆境与慢性疼痛风险联系起来的研究。

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