DNA methylation of bone morphogenetic protein 7 in leukocytes as a possible biomarker for hand osteoarthritis: A pilot study

IF 2.1 3区 医学 Q2 ORTHOPEDICS
Takashi Kuroiwa, Yoshiki Tsuboi, Takehiro Michikawa, Kaori Tajima, Yuki Uraya, Atsushi Maeda, Kanae Shizu, Katsuji Suzuki, Koji Suzuki, Yusuke Kawano, Nobuyuki Fujita
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Abstract

Hand osteoarthritis (HOA), characterized by an earlier onset age and reduced susceptibility to mechanical stress compared with knee and hip osteoarthritis, is considered a suitable disease for identifying predictive biomarkers of osteoarthritis. In particular, DNA methylation variants, expected to contribute to HOA susceptibility, hold potential as osteoarthritis biomarkers. In this study, leukocyte DNA methylation patterns were analyzed in blood samples from patients with HOA, aiming to identify disease-specific biomarkers for osteoarthritis. Using DNA methylation microarrays, we analyzed samples from three subjects with HOA and three age- and gender-matched healthy individuals. For validation, pyrosequencing analysis was conducted using samples from 16 to 9 subjects with and without HOA, respectively. From 735,026 probes in the DNA methylation array, the Top 100 CpG sites associated with HOA, based on low adjusted P-values, including those targeting bone morphogenetic protein 7 (BMP7), SBF2-AS1, PLOD2, ICOS, and CSF1R were identified. Validation analysis revealed significantly higher methylation levels in the BMP7-related site in the HOA group compared with the control group, even after adjusting for age, gender, and body mass index (p = 0.037). In contrast, no significant difference was observed in the other selected CpG sites between the HOA and control groups. This study highlights the significantly increased frequency of methylation at the specific BMP7 site in leukocytes of patients with HOA, suggesting its potential as a biomarker for HOA. Measurement of methylation levels at the CpG sites identified in this study offers a potential approach to prevent future osteoarthritis progression, providing valuable insights into disease management.

Abstract Image

白细胞中骨形态发生蛋白 7 的 DNA 甲基化可能是手部骨关节炎的生物标志物:一项试点研究。
与膝关节和髋关节骨关节炎相比,手部骨关节炎(HOA)的特点是发病年龄较早、对机械应力的易感性较低,因此被认为是一种适合鉴定骨关节炎预测性生物标志物的疾病。特别是DNA甲基化变异,预计会导致HOA易感性,具有作为骨关节炎生物标志物的潜力。本研究分析了HOA患者血液样本中的白细胞DNA甲基化模式,旨在确定骨关节炎的疾病特异性生物标志物。我们使用 DNA 甲基化芯片分析了三名 HOA 患者和三名年龄与性别匹配的健康人的样本。为了进行验证,我们分别对 16 至 9 名患有和未患有 HOA 的受试者样本进行了热测序分析。从 DNA 甲基化阵列的 735,026 个探针中,根据低调整 P 值,确定了与 HOA 相关的前 100 个 CpG 位点,包括针对骨形态发生蛋白 7 (BMP7)、SBF2-AS1、PLOD2、ICOS 和 CSF1R 的位点。验证分析表明,HOA 组与对照组相比,BMP7 相关位点的甲基化水平明显更高,即使在调整年龄、性别和体重指数后也是如此(p = 0.037)。相比之下,在其他选定的 CpG 位点上,HOA 组和对照组没有观察到明显差异。这项研究强调,HOA 患者白细胞中特定 BMP7 位点的甲基化频率明显增加,表明其有可能成为 HOA 的生物标志物。测量本研究中发现的 CpG 位点的甲基化水平为预防未来骨关节炎的发展提供了一种潜在的方法,为疾病管理提供了宝贵的见解。
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来源期刊
Journal of Orthopaedic Research®
Journal of Orthopaedic Research® 医学-整形外科
CiteScore
6.10
自引率
3.60%
发文量
261
审稿时长
3-6 weeks
期刊介绍: The Journal of Orthopaedic Research is the forum for the rapid publication of high quality reports of new information on the full spectrum of orthopaedic research, including life sciences, engineering, translational, and clinical studies.
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