DNA methylation differences within INS, PTPN22 and IL2RA promoters in lymphocyte subsets in children with type 1 diabetes and controls.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
ACS Applied Electronic Materials Pub Date : 2023-12-01 Epub Date: 2023-09-19 DOI:10.1080/08916934.2023.2259118
Sirpa Pahkuri, Ilse Ekman, Céline Vandamme, Kirsti Näntö-Salonen, Jorma Toppari, Riitta Veijola, Mikael Knip, Tuure Kinnunen, Jorma Ilonen, Johanna Lempainen
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引用次数: 0

Abstract

We elucidated the effect of four known T1D-susceptibility associated single nucleotide polymorphism (SNP) markers in three genes (rs12722495 and rs2104286 in IL2RA, rs689 in INS and rs2476601 in PTPN22) on CpG site methylation of their proximal promoters in different lymphocyte subsets using pyrosequencing. The study cohort comprised 25 children with newly diagnosed T1D and 25 matched healthy controls. The rs689 SNP was associated with methylation at four CpG sites in INS promoter: -234, -206, -102 and -69. At all four CpG sites, the susceptibility genotype AA was associated with a higher methylation level compared to the other genotypes. We also found an association between rs12722495 and methylation at CpG sites -373 and -356 in IL2RA promoter in B cells, where the risk genotype AA was associated with lower methylation level compared to the AG genotype. The other SNPs analyzed did not demonstrate significant associations with CpG site methylation in the examined genes. Additionally, we compared the methylation between children with T1D and controls, and found statistically significant methylation differences at CpG -135 in INS in CD8+ T cells (p = 0.034), where T1D patients had a slightly higher methylation compared to controls (87.3 ± 7.2 vs. 78.8 ± 8.9). At the other CpG sites analyzed, the methylation was similar. Our results not only confirm the association between INS methylation and rs689 discovered in earlier studies but also report this association in sorted immune cells. We also report an association between rs12722495 and IL2RA promoter methylation in B cells. These results suggest that at least part of the genetic effect of rs689 and rs12722495 on T1D pathogenesis may be conveyed by DNA methylation.

1型糖尿病儿童和对照组淋巴细胞亚群中INS、PTPN22和IL2RA启动子的DNA甲基化差异。
我们使用焦磷酸测序阐明了三个基因中四个已知的T1D易感性相关单核苷酸多态性(SNP)标记物(IL2RA中的rs12722495和rs2104286,INS中的rs689和PTPN22中的rs2476601)对不同淋巴细胞亚群中其近端启动子CpG位点甲基化的影响。研究队列包括25名新诊断为T1D的儿童和25名匹配的健康对照。rs689 SNP与INS启动子中的四个CpG位点甲基化有关:-234、-206、-102和-69。在所有四个CpG位点,与其他基因型相比,易感基因型AA与更高的甲基化水平相关。我们还发现rs12722495与B细胞IL2RA启动子CpG位点-373和-356的甲基化之间存在关联,其中风险基因型AA与AG基因型相比甲基化水平较低有关。所分析的其他SNPs没有显示出与所检查基因中CpG位点甲基化的显著相关性。此外,我们比较了T1D儿童和对照组之间的甲基化,发现CD8+T细胞中INS中CpG-135的甲基化差异具有统计学意义(p = 0.034),其中T1D患者与对照组相比甲基化程度略高(87.3 ± 7.2对78.8 ± 8.9)。在所分析的其他CpG位点,甲基化是相似的。我们的结果不仅证实了早期研究中发现的INS甲基化和rs689之间的关联,而且还报道了分选免疫细胞中的这种关联。我们还报道了rs12722495与B细胞中IL2RA启动子甲基化之间的关联。这些结果表明,rs689和rs12722495在T1D发病机制中的至少部分遗传效应可能通过DNA甲基化来传递。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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