School of Nursing, University of Alabama at Birmingham, Birmingham, AL, USA.
Department of Psychology, University of Alabama at Birmingham, Birmingham, AL, USA.
Mol Pain. 2020 Jan-Dec;16:1744806920972889. doi: 10.1177/1744806920972889.
Chronic low back pain (cLBP) that cannot be attributable to a specific pathoanatomical change is associated with high personal and societal costs. Still, the underlying mechanism that causes and sustains such a phenotype is largely unknown. Emerging evidence suggests that epigenetic changes play a role in chronic pain conditions. Using reduced representation bisulfite sequencing (RRBS), we evaluated DNA methylation profiles of adults with non-specific cLBP (n = 50) and pain-free controls (n = 48). We identified 28,325 hypermethylated and 36,936 hypomethylated CpG sites (p < 0.05). After correcting for multiple testing, we identified 159 DMRs (q < 0.01and methylation difference > 10%), the majority of which were located in CpG island (50%) and promoter regions (48%) on the associated genes. The genes associated with the differentially methylated regions were highly enriched in biological processes that have previously been implicated in immune signaling, endochondral ossification, and G-protein coupled transmissions. Our findings support inflammatory alterations and the role of bone maturation in cLBP. This study suggests that epigenetic regulation has an important role in the pathophysiology of non-specific cLBP and a basis for future studies in biomarker development and targeted interventions.
慢性下背痛(cLBP)无法归因于特定的病理解剖变化,与个人和社会的高成本相关。然而,导致和维持这种表型的潜在机制在很大程度上尚不清楚。新出现的证据表明,表观遗传变化在慢性疼痛病症中起作用。使用简化代表性双硫代测序(RRBS),我们评估了 50 名非特异性 cLBP 患者(n=50)和无疼痛对照者(n=48)的 DNA 甲基化图谱。我们发现了 28,325 个高甲基化和 36,936 个低甲基化 CpG 位点(p<0.05)。在对多次测试进行校正后,我们鉴定出 159 个 DMR(q<0.01,甲基化差异>10%),其中大多数位于相关基因的 CpG 岛(50%)和启动子区域(48%)。与差异甲基化区域相关的基因在生物过程中高度富集,这些过程先前与免疫信号、软骨内骨化和 G 蛋白偶联转导有关。我们的研究结果支持了炎症改变和骨成熟在 cLBP 中的作用。这项研究表明,表观遗传调控在非特异性 cLBP 的病理生理学中具有重要作用,为未来的生物标志物开发和靶向干预研究提供了基础。
