Circadian rhythmicity and biopsychosocial characteristics influence opioid use in chronic low back pain.

Doriana Taccardi,Amanda M Zacharias,Hailey Gm Gowdy,Mitra Knezic,Marc Parisien,Etienne J Bisson,Zhi Yi Fang,Sara A Stickley,Elizabeth Brown,Daenis Camiré,Rosemary Wilson,Lesley N Singer,Jennifer Daly-Cyr,Manon Choinière,Zihang Lu,M Gabrielle Pagé,Luda Diatchenko,Qingling Duan,Nader Ghasemlou
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Abstract

BACKGROUNDInter- and intraindividual fluctuations in pain intensity pose a major challenge to treatment efficacy, with a majority of people perceiving their pain relief as inadequate. Recent preclinical studies have identified circadian rhythmicity as a potential contributor to these fluctuations and a therapeutic target.METHODSWe therefore sought to determine the impact of circadian rhythms in people with chronic low back pain (CLBP) through a detailed characterization, including questionnaires to evaluate biopsychosocial characteristics, ecological momentary assessment (7 day e-diaries at 8:00/14:00/20:00) to observe pain fluctuations, and intraday blood transcriptomics (at 8:00/20:00) to identify genes/pathways of interest.RESULTSWhile most individuals displayed constant or variable/mixed pain phenotypes, a distinct subset had daily fluctuations of increasing pain scores (>30% change in intensity over 12 hours in ≥4/7 days). This population had no opioid users, better biopsychosocial profiles, and differentially expressed transcripts relative to other pain phenotypes. The circadian-governed neutrophil degranulation pathway was particularly enriched among arrhythmic individuals; the link between neutrophil degranulation and opioid use was further confirmed in a separate CLBP cohort.CONCLUSIONOur findings identified pain rhythmicity and the circadian expression of neutrophil degranulation pathways as indicators of CLBP outcomes, which may help provide a personalized approach to phenotyping biopsychosocial characteristics and medication use. This highlights the need to better understand the impact of circadian rhythmicity across chronic pain conditions.FUNDINGThis work was funded by grants from the Canadian Institutes of Health Research (CIHR; grant PJT-190170, to NG and MGP) and the CIHR-Strategy for Patient-Oriented Research Chronic Pain Network (grant SCA-145102, to NG, QD, LD, MGP, and MC). DT was funded by a MS Canada endMS Doctoral Research Award, AMZ by an Ontario Graduate Scholarship, HGMG by a CIHR Doctoral Research Award, MGP by a Junior 2 Research Scholarship from the Fonds de recherche du Québec - Santé, and LD by a Canadian Excellence Research Chairs and Pfizer Canada Professorship in Pain Research.
昼夜节律性和生物心理社会特征影响阿片类药物在慢性腰痛中的使用。
背景:个体和个体疼痛强度的波动对治疗效果构成了重大挑战,大多数人认为他们的疼痛缓解不足。最近的临床前研究已经确定昼夜节律性是这些波动的潜在因素和治疗靶点。因此,我们试图通过详细的表征来确定昼夜节律对慢性腰痛(CLBP)患者的影响,包括评估生物心理社会特征的问卷调查,观察疼痛波动的生态瞬间评估(7天电子日记,8:00/14:00/20:00)和日间血液转录组学(8:00/20:00),以确定感兴趣的基因/途径。结果虽然大多数个体表现出恒定或可变/混合疼痛表型,但有一个独特的子集疼痛评分每日波动增加(≥4/7天内12小时内强度变化约30%)。该人群没有阿片类药物使用者,更好的生物心理社会特征,以及相对于其他疼痛表型的差异表达转录本。节律控制的中性粒细胞脱颗粒途径在心律失常个体中尤其丰富;中性粒细胞脱颗粒和阿片类药物使用之间的联系在一个单独的CLBP队列中得到进一步证实。结论:我们的研究发现疼痛节律性和中性粒细胞脱颗粒途径的昼夜表达是CLBP结果的指标,这可能有助于为生物、心理、社会特征和药物使用提供个性化的方法。这凸显了更好地理解昼夜节律对慢性疼痛状况的影响的必要性。本研究由加拿大卫生研究院(CIHR;授予PJT-190170, NG和MGP)和CIHR-以患者为导向的慢性疼痛研究网络策略(授予ca -145102, NG, QD, LD, MGP和MC)资助。DT获得了加拿大MS endMS博士研究奖,AMZ获得了安大略省研究生奖学金,HGMG获得了CIHR博士研究奖,MGP获得了qu- sant研究基金会的初级2级研究奖学金,LD获得了加拿大卓越研究主席和辉瑞加拿大疼痛研究教授的资助。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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