Maria Carla Gerra, Cristina Dallabona, Matteo Manfredini, Rocco Giordano, Camilla Capriotti, Alberto González-Villar, Yolanda Triñanes, Lars Arendt-Nielsen, Maria Teresa Carrillo-de-la-Peña
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引用次数: 0
Abstract
Abstract: The single-nucleotide polymorphism (SNP) rs4680 in the catechol-O-methyltransferase gene ( COMT ) is a missense variant (Val158Met) associated with altered activity of the COMT enzyme and suggested as a predictive feature for developing some chronic pain conditions. However, there are controversial results on its role in fibromyalgia (FM). Here, the SNP Val158Met was analyzed in 294 FM patients (without comorbidities) and 209 healthy controls (without chronic pain). The concurrent impact of Val158Met genotypes and FM comorbid disorders (depression and sleep impairment) on FM risk were tested. In addition, the genotypic distribution of FM patients in relation to pain intensity was evaluated. The G allele (Val) resulted in being more represented in the FM group (57.8%) compared with the control group (48.8%; P = 0.037). Logistic regression highlighted that having the G/G (Val/Val) homozygous genotype was associated with 2 times higher risk of having FM compared with the A/A (Met/Met) carriers ( P = 0.038), whereas depression and sleep impairment increased FM risk by 12 and 8 times, respectively ( P < 0.001). However, considering only the FM patient group, the A/A homozygous genotype was significantly associated with severe pain intensity ( P = 0.007). This study highlighted associations between the SNP Val158Met and both FM and pain intensity, suggesting a link between dopaminergic dysfunction and vulnerability to chronic pain. Further studies should explore this SNP in FM patients in conjunction with COMT enzymatic activity and other symptoms connected with the dopaminergic system such as depression or sleep impairment.
摘要:儿茶酚-O-甲基转移酶基因(COMT)中的单核苷酸多态性(SNP)rs4680是一种错义变异(Val158Met),与COMT酶活性的改变有关,被认为是一些慢性疼痛疾病的预测特征。然而,关于它在纤维肌痛(FM)中的作用却存在争议。本文对 294 名纤维肌痛患者(无合并症)和 209 名健康对照者(无慢性疼痛)的 SNP Val158Met 进行了分析。测试了 Val158Met 基因型和 FM 并发症(抑郁症和睡眠障碍)对 FM 风险的并发影响。此外,还评估了 FM 患者的基因型分布与疼痛强度的关系。与对照组(48.8%;P = 0.037)相比,G 等位基因(Val)在 FM 组(57.8%)中的比例更高。逻辑回归结果表明,与A/A(Met/Met)携带者相比,G/G(Val/Val)同源基因型携带者患 FM 的风险要高出 2 倍(P = 0.038),而抑郁和睡眠障碍则使患 FM 的风险分别增加了 12 倍和 8 倍(P < 0.001)。然而,仅考虑 FM 患者组,A/A 同源基因型与剧烈疼痛强度显著相关(P = 0.007)。这项研究强调了 SNP Val158Met 与 FM 和疼痛强度之间的关联,表明多巴胺能功能障碍与易患慢性疼痛之间存在联系。进一步的研究应结合 COMT 酶活性和其他与多巴胺能系统有关的症状(如抑郁或睡眠障碍),探讨 FM 患者的这一 SNP。
期刊介绍:
PAIN® is the official publication of the International Association for the Study of Pain and publishes original research on the nature,mechanisms and treatment of pain.PAIN® provides a forum for the dissemination of research in the basic and clinical sciences of multidisciplinary interest.