细胞因子在重大肌肉骨骼手术后小儿急性和慢性术后疼痛中的作用

Vidya Chidambaran, Qing Duan, Valentina Pilipenko, Susan Glynn, Alyssa Sproles, Lisa J Martin, Michael Lacagnina, Christopher D King, Lili Ding
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After data preparation, relationships between pre- and post-surgical cytokine concentrations with acute (% time in moderate-severe pain over POD0-2) and chronic (pain score>3/10 beyond 3 months post-surgery) pain were analyzed. After adjusting for covariates, univariate/multivariate regression analyses were conducted to associate baseline cytokine concentrations with postoperative pain, and mixed effects models were used to associate longitudinal cytokine concentrations with pain outcomes.\nMain Results: Analyses included 3,164 measures of 16 cytokines from 112 subjects (median age 15.3, IQR 13.5-17.0, 54.5% female, 59.8% pectus). 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引用次数: 0

摘要

研究目的确定基线细胞因子及其在术后第 0-2 天(POD0-2)的变化是否可预测大手术后的急性和慢性术后疼痛(CPSP):前瞻性、观察性、纵向嵌套研究:地点:大学附属四级儿童医院:受试者:特发性脊柱侧凸患者(≥8 岁),接受脊柱融合术或鸡胸症患者,接受 Nuss 手术:收集人口统计学资料、手术、社会心理测量、疼痛评分以及POD0-2期间阿片类药物的使用情况。使用Luminex珠阵列分析手术前后(最多两周)采集的连续血样中细胞因子的浓度。数据准备完成后,分析了手术前后细胞因子浓度与急性疼痛(POD0-2 中度-重度疼痛时间百分比)和慢性疼痛(手术后 3 个月后疼痛评分>3/10)之间的关系。调整协变量后,进行单变量/多变量回归分析,将基线细胞因子浓度与术后疼痛联系起来,并使用混合效应模型将纵向细胞因子浓度与疼痛结果联系起来:分析包括对 112 名受试者(中位年龄为 15.3 岁,IQR 为 13.5-17.0 岁,54.5% 为女性,59.8% 为乳腺增生症患者)的 16 种细胞因子进行的 3,164 次测量。急性手术后疼痛与较高的 GM-CSF 基线浓度(β=0.95,SE 0.31;p=.003)、IL-1β(β=0.84,SE 0.36;p=.02)、IL-2(β=0.78,SE 0.34;p=.03)和 IL-12 p70(β=0.88,SE 0.40;p=.03)以及术后 GM-CSF(β=1.38,SE 0.57;p=.03)、IFNγ(β=1.36,SE 0.6;p=.03)、IL-1β(β=1.25,SE 0.59;p=.03)、IL-7(β=1.65,SE 0.7,p=.02)和 IL-12 p70(β=1.17,SE 0.58;p=.04)的纵向升高。相反,CPSP 与较低的 IL-8 基线浓度相关(β= -0.39,SE 0.17;p=.02),术后 IL-6 (β= -0.57,SE 0.26;p=.03)、IL-8 (β= -0.68,SE 0.24;p=.006)和 IL-13 (β= -0.48,SE 0.22;p=.03)纵向浓度较低的患者发生 CPSP 的风险升高。此外,在IL-2、IL-4、IL-5、IL-6、IL-8、IL-10和TNFα方面,女性(与男性相比)患CPSP的几率更高;在IL-8和IL-10方面,贲门(与脊柱)手术的几率更高:我们发现了与术后急性疼痛增加相关的促炎细胞因子和与 CPSP 风险降低相关的抗炎细胞因子,它们有可能成为预测和预后的生物标志物。
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The Role of Cytokines in Acute and Chronic Postsurgical Pain in Pediatric Patients after Major Musculoskeletal Surgeries
Study Objective: To determine if baseline cytokines and their changes over postoperative days 0-2 (POD0-2) predict acute and chronic postsurgical pain (CPSP) after major surgery. Design: Prospective, observational, longitudinal nested study. Setting: University-affiliated quaternary childrens hospital. Patients: Subjects (≥8 years old) with idiopathic scoliosis undergoing spine fusion or pectus excavatum undergoing Nuss procedure. Measurements: Demographics, surgical, psychosocial measures, pain scores, and opioid use over POD0-2 were collected. Cytokine concentrations were analyzed in serial blood samples collected before and after (up to two weeks) surgery, using Luminex bead arrays. After data preparation, relationships between pre- and post-surgical cytokine concentrations with acute (% time in moderate-severe pain over POD0-2) and chronic (pain score>3/10 beyond 3 months post-surgery) pain were analyzed. After adjusting for covariates, univariate/multivariate regression analyses were conducted to associate baseline cytokine concentrations with postoperative pain, and mixed effects models were used to associate longitudinal cytokine concentrations with pain outcomes. Main Results: Analyses included 3,164 measures of 16 cytokines from 112 subjects (median age 15.3, IQR 13.5-17.0, 54.5% female, 59.8% pectus). Acute postsurgical pain was associated with higher baseline concentrations of GM-CSF (β=0.95, SE 0.31; p=.003), IL-1β (β=0.84, SE 0.36; p=.02), IL-2 (β=0.78, SE 0.34; p=.03), and IL-12 p70 (β=0.88, SE 0.40; p=.03) and longitudinal postoperative elevations in GM-CSF (β=1.38, SE 0.57; p=.03), IFNγ (β=1.36, SE 0.6; p=.03), IL-1β(β=1.25, SE 0.59; p=.03), IL-7 (β=1.65, SE 0.7, p=.02), and IL-12 p70 (β=1.17, SE 0.58; p=.04). In contrast, CPSP was associated with lower baseline concentration of IL-8 (β= -0.39, SE 0.17; p=.02), and the risk of developing CPSP was elevated in patients with lower longitudinal postoperative concentrations of IL-6 (β= -0.57, SE 0.26; p=.03), IL-8 (β= -0.68, SE 0.24; p=.006), and IL-13 (β= -0.48, SE 0.22; p=.03). Furthermore, higher odds for CPSP were found for females (vs. males) for IL-2, IL-4, IL-5, IL-6, IL-8, IL-10, and TNFα ; and for pectus (vs. spine) surgery for IL-8 and IL-10. Conclusion: We identified pro-inflammatory cytokines associated with increased acute postoperative pain and anti-inflammatory cytokines associated with lower CPSP risk, with the potential to serve as predictive and prognostic biomarkers.
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