Department of Orthopedics, Shanghai Changzheng Hospital, Second Military Medical University, 415 Fengyang Road, Shanghai 200003, People's Republic of China.
Department of Orthopedics, Shanghai Changzheng Hospital, Second Military Medical University, 415 Fengyang Road, Shanghai 200003, People's Republic of China; Department of Medical Genetics, Second Military Medical University, 800 Xiangyin Road, Shanghai 200433, People's Republic of China.
EBioMedicine. 2018 Oct;36:489-496. doi: 10.1016/j.ebiom.2018.09.014. Epub 2018 Sep 18.
There is considerable discordance in the curve progression of adolescent idiopathic scoliosis (AIS) patients between monozygotic (MZ) twins, indicating that nongenetic factors must be involved in the curve progression of AIS patients. Epigenetic processes may constitute one of these factors and have not yet been investigated in relation to curve progression in AIS patients.
The genome and methylome of peripheral monocytes were compared between MZ twins discordant for curve progression. Sets of differentially methylated sites were validated using the MassARRAY platform of Sequenome on additional samples.
In the discovery study, we found evidence suggesting a lack of differences at the genome sequence level and the presence of epigenetic differences related to the curve progression of AIS patients. The top 4 differentially methylated CpG sites associated with curve severity were tested, and only site cg01374129 (CpG site located at chr8:122583383, Hg19) was confirmed in two replication cohorts. The methylation levels of site cg01374129 were significantly lower in the progression group than in the nonprogression group. Cox regression analysis demonstrated that hypo-methylation of site cg01374129 was an independent prognostic factor for curve severity. Site cg01374129 methylation as a marker achieved a sensitivity of 76.4% and a specificity of 85.6% in differentiating between samples from patients with and without curve progression (AUC = 0.827; 95% CI: 0.780 to 0.876).
Increased curvature is associated with decreased methylation at site cg01374129. Our results indicate that methylation of site cg01374129 may therefore serve as a promising biomarker in differing between patients with and without curve progression.
同卵双胞胎(MZ)青少年特发性脊柱侧凸(AIS)患者的曲线进展存在显著差异,这表明非遗传因素必然参与 AIS 患者的曲线进展。表观遗传过程可能构成这些因素之一,但尚未在 AIS 患者的曲线进展中进行研究。
比较了 MZ 双胞胎中曲线进展不一致的外周单核细胞的基因组和甲基组。使用 Sequenome 的 MassARRAY 平台在额外的样本中验证了差异甲基化位点的集合。
在发现研究中,我们发现证据表明在基因组序列水平上没有差异,并且存在与 AIS 患者曲线进展相关的表观遗传差异。对与曲线严重程度相关的前 4 个差异甲基化 CpG 位点进行了测试,只有位于 chr8:122583383,Hg19 的 CpG 位点 cg01374129 在两个复制队列中得到证实。进展组中该位点的甲基化水平明显低于非进展组。Cox 回归分析表明,该位点 cg01374129 的低甲基化是曲线严重程度的独立预后因素。该位点的甲基化作为标志物在区分有进展和无进展患者的样本时具有 76.4%的敏感性和 85.6%的特异性(AUC=0.827;95%CI:0.780 至 0.876)。
曲率增加与 cg01374129 位点的甲基化减少有关。我们的结果表明,cg01374129 位点的甲基化可能因此成为区分有进展和无进展患者的有前途的生物标志物。
Zotero 插件
