在胰岛自身免疫起始过程中 DNA 甲基化的纵向变化可区分胰岛自身免疫的逆转与进展。
Longitudinal changes in DNA methylation during the onset of islet autoimmunity differentiate between reversion versus progression of islet autoimmunity.
机构信息
Colorado Program for Musculoskeletal Research, Department of Orthopedics, University of Colorado, Aurora, CO, United States.
Department of Epidemiology, Colorado School of Public Health, Aurora, CO, United States.
出版信息
Front Immunol. 2024 Jun 10;15:1345494. doi: 10.3389/fimmu.2024.1345494. eCollection 2024.
BACKGROUND
Type 1 diabetes (T1D) is preceded by a heterogenous pre-clinical phase, islet autoimmunity (IA). We aimed to identify pre vs. post-IA seroconversion (SV) changes in DNAm that differed across three IA progression phenotypes, those who lose autoantibodies (reverters), progress to clinical T1D (progressors), or maintain autoantibody levels (maintainers).
METHODS
This epigenome-wide association study (EWAS) included longitudinal DNAm measurements in blood (Illumina 450K and EPIC) from participants in Diabetes Autoimmunity Study in the Young (DAISY) who developed IA, one or more islet autoantibodies on at least two consecutive visits. We compared - individuals who sero-reverted, negative for all autoantibodies on at least two consecutive visits and did not develop T1D (n=41); continued to test positive for autoantibodies but did not develop T1D (n=60); developed clinical T1D (n=42). DNAm data were measured before (pre-SV visit) and after IA (post-SV visit). Linear mixed models were used to test for differences in pre- vs post-SV changes in DNAm across the three groups. Linear mixed models were also used to test for group differences in average DNAm. Cell proportions, age, and sex were adjusted for in all models. Median follow-up across all participants was 15.5 yrs. (interquartile range (IQR): 10.8-18.7).
RESULTS
The median age at the pre-SV visit was 2.2 yrs. (IQR: 0.8-5.3) in progressors, compared to 6.0 yrs. (IQR: 1.3-8.4) in reverters, and 5.7 yrs. (IQR: 1.4-9.7) in maintainers. Median time between the visits was similar in reverters 1.4 yrs. (IQR: 1-1.9), maintainers 1.3 yrs. (IQR: 1.0-2.0), and progressors 1.8 yrs. (IQR: 1.0-2.0). Changes in DNAm, pre- vs post-SV, differed across the groups at one site (cg16066195) and 11 regions. Average DNAm (mean of pre- and post-SV) differed across 22 regions.
CONCLUSION
Differentially changing DNAm regions were located in genomic areas related to beta cell function, immune cell differentiation, and immune cell function.
背景
1 型糖尿病(T1D)之前存在异质的临床前阶段,即胰岛自身免疫(IA)。我们旨在确定在三种 IA 进展表型中,自身抗体血清学转换(SV)前后的 DNAm 变化,这些表型包括自身抗体丢失的个体(逆转者)、进展为临床 T1D 的个体(进展者)或维持自身抗体水平的个体(维持者)。
方法
本项基于表观基因组的关联研究(EWAS)纳入了糖尿病自身免疫研究中的年轻人(DAISY)参与者的纵向血液 DNAm 测量值(Illumina 450K 和 EPIC),这些参与者出现了 IA,至少在两次连续就诊时出现了一种或多种胰岛自身抗体。我们比较了 - 血清学逆转的个体,至少在两次连续就诊时自身抗体均为阴性且未发生 T1D(n=41); 继续检测出自身抗体阳性但未发生 T1D(n=60); 发生临床 T1D(n=42)。DNAm 数据在 IA 之前(SV 前就诊)和之后(SV 后就诊)进行测量。线性混合模型用于检验三组间 DNAm 改变的 SV 前与 SV 后差异。线性混合模型还用于检验各组间平均 DNAm 的差异。所有模型均调整了细胞比例、年龄和性别。所有参与者的中位随访时间为 15.5 年(四分位距(IQR):10.8-18.7)。
结果
进展者的 SV 前就诊时年龄中位数为 2.2 岁(IQR:0.8-5.3),与逆转者的 6.0 岁(IQR:1.3-8.4)和维持者的 5.7 岁(IQR:1.4-9.7)相比。逆转者两次就诊之间的中位时间为 1.4 年(IQR:1-1.9),维持者为 1.3 年(IQR:1.0-2.0),进展者为 1.8 年(IQR:1.0-2.0)。SV 前后的 DNAm 改变,在一个位点(cg16066195)和 11 个区域存在差异。22 个区域的平均 DNAm(SV 前后的平均值)存在差异。
结论
差异变化的 DNAm 区域位于与胰岛功能、免疫细胞分化和免疫细胞功能相关的基因组区域。
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