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与引导意象治疗慢性疼痛的有效性相关的生物学机制。

Biological mechanisms related to the effectiveness of guided imagery for chronic pain.

机构信息

College of Nursing, Kent State University, Kent, OH 44242, USA.

出版信息

Biol Res Nurs. 2011 Oct;13(4):364-75. doi: 10.1177/1099800410386475. Epub 2010 Nov 26.

DOI:10.1177/1099800410386475
PMID:21112919
Abstract

Specific aims of this pilot study were to (a) determine the effect of a guided imagery (GI) intervention over an 8-week period on pain and pain disability in a sample of persons with chronic noncancer pain (CNCP) and (b) analyze the mediating effects of neuroendocrine and neuroimmune functioning on the effectiveness of GI on outcome variables. A simple interrupted time-series design (12-week period) was used. GI was introduced at Week 4 and used daily by 25 participants for the remaining 8 weeks. Measures of pain and pain disability were obtained at the beginning of the study period and at six repeated 2-week intervals. Measures of hypothalamic-pituitary-adrenal (HPA) axis activation (plasma cortisol), immune-mediated analgesia (lymphocyte subset counts and proliferation), and immune-mediated hyperalgesia (interleukin-1β) were obtained at the beginning of the study and at Week 11. Usual pain levels were lower after the introduction of GI at Week 4 (Wilks' λ = 52.31; df = 2, 22; p = .000). Pain disability levels were lower after the introduction of GI at Week 4 (Wilks' λ = 5.98; df = 6, 18; p = .001). Correlation coefficients between change scores of dependent variables and mediating variables were not significant. GI was effective in reducing pain intensity and pain disability over an 8-week period; however, the results did not support the expected effects of decreased HPA axis activation, improved immune-mediated analgesia, and reduced immune-mediated hyperalgesia in mediating these outcomes. These findings may be related to procedural and theoretical issues and limitations related to the study design.

摘要

本研究的具体目的是

(a) 确定在 8 周的时间内,指导意象干预对慢性非癌性疼痛患者(CNCP)疼痛和疼痛残疾的影响;(b) 分析神经内分泌和神经免疫功能对指导意象对结果变量的有效性的中介作用。使用了简单的中断时间序列设计(12 周周期)。指导意象在第 4 周引入,25 名参与者在接下来的 8 周内每天使用。在研究开始时和六个重复的 2 周间隔期获得疼痛和疼痛残疾的测量值。在研究开始时和第 11 周获得下丘脑-垂体-肾上腺(HPA)轴激活(血浆皮质醇)、免疫介导的镇痛(淋巴细胞亚群计数和增殖)和免疫介导的痛觉过敏(白细胞介素-1β)的测量值。在第 4 周引入指导意象后,疼痛水平降低(Wilks' λ = 52.31;df = 2,22;p =.000)。在第 4 周引入指导意象后,疼痛残疾水平降低(Wilks' λ = 5.98;df = 6,18;p =.001)。因变量和中介变量变化分数之间的相关系数不显著。指导意象在 8 周的时间内有效降低了疼痛强度和疼痛残疾;然而,结果并不支持 HPA 轴激活减少、免疫介导的镇痛改善和免疫介导的痛觉过敏减少对这些结果的预期影响。这些发现可能与研究设计的程序和理论问题和限制有关。

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