Whole Blood DNA Methylation Changes Are Associated with Anti-TNF Drug Concentration in Patients with Crohn's Disease.

IF 8.3 2区医学 Q1 GASTROENTEROLOGY & HEPATOLOGY Journal of Crohns & Colitis Pub Date : 2024-08-14 DOI:10.1093/ecco-jcc/jjad133

Simeng Lin, Eilis Hannon, Mark Reppell, Jeffrey F Waring, Nizar Smaoui, Valerie Pivorunas, Heath Guay, Neil Chanchlani, Claire Bewshea, Benjamin Y H Bai, Nicholas A Kennedy, James R Goodhand, Jonathan Mill, Tariq Ahmad

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Abstract

Background and aims: Anti-tumour necrosis factor [TNF] treatment failure in patients with inflammatory bowel disease [IBD] is common and frequently related to low drug concentrations. In order to identify patients who may benefit from dose optimisation at the outset of anti-TNF therapy, we sought to define epigenetic biomarkers in whole blood at baseline associated with anti-TNF drug concentrations at week 14.

Methods: DNA methylation from 1104 whole blood samples from 385 patients in the Personalised Anti-TNF Therapy in Crohn's disease [PANTS] study were assessed using the Illumina EPIC Beadchip [v1.0] at baseline and weeks 14, 30, and 54. We compared DNA methylation profiles in anti-TNF-treated patients who experienced primary non-response at week 14 if they were assessed at subsequent time points and were not in remission at week 30 or 54 [infliximab n = 99, adalimumab n = 94], with patients who responded at week 14 and when assessed at subsequent time points were in remission at week 30 or 54 [infliximab n = 99, adalimumab n = 93].

Results: Overall, between baseline and week 14, we observed 4999 differentially methylated positions [DMPs] annotated to 2376 genes following anti-TNF treatment. Pathway analysis identified 108 significant gene ontology terms enriched in biological processes related to immune system processes and responses. Epigenome-wide association [EWAS] analysis identified 323 DMPs annotated to 210 genes at baseline associated with higher anti-TNF drug concentrations at Week 14. Of these, 125 DMPs demonstrated shared associations with other common traits [proportion of shared CpGs compared with DMPs] including body mass index [23.2%], followed by C-reactive protein [CRP] [11.5%], smoking [7.4%], alcohol consumption per day [7.1%], and IBD type [6.8%]. EWAS of primary non-response to anti-TNF identified 20 DMPs that were associated with both anti-TNF drug concentration and primary non-response to anti-TNF with a strong correlation of the coefficients [Spearman's rho = -0.94, p <0.001].

Conclusion: Baseline DNA methylation profiles may be used as a predictor for anti-TNF drug concentration at week 14 to identify patients who may benefit from dose optimisation at the outset of anti-TNF therapy.

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克罗恩病患者全血 DNA 甲基化变化与抗肿瘤坏死因子药物浓度有关。

背景和目的：炎症性肠病（IBD）患者抗肿瘤坏死因子（anti-TNF）治疗失败很常见，而且经常与药物浓度低有关。为了在抗肿瘤坏死因子（anti-TNF）治疗初期确定哪些患者可从剂量优化中获益，我们试图确定基线全血中与第 14 周时抗肿瘤坏死因子药物浓度相关的表观遗传生物标志物：使用 Illumina EPIC Beadchip（v1.0）评估了克罗恩病个性化抗肿瘤坏死因子疗法（PANTS）研究中 385 名患者在基线、第 14 周、第 30 周和第 54 周的 1104 份全血样本中的 DNA 甲基化情况。我们比较了抗肿瘤坏死因子治疗患者的DNA甲基化图谱，这些患者在第14周出现原发性无应答，如果在随后的时间点进行评估，则在第30周或第54周没有缓解（英夫利昔单抗n=99，阿达木单抗n=94），与在第14周出现应答，在随后的时间点进行评估，则在第30周或第54周缓解的患者（英夫利昔单抗n=99，阿达木单抗n=93）：总体而言，从基线到第14周，我们观察到4999个差异甲基化探针（DMPs）注释在抗肿瘤坏死因子治疗后的2376个基因上。全表观基因组关联（EWAS）分析发现，基线时注释在 210 个基因上的 323 个 DMPs 与第 14 周时较高的抗肿瘤坏死因子药物浓度有关。其中，125 个 DMPs 与其他共同特征（与 DMPs 相比，共享 CpGs 的比例）有共同关联，包括体重指数（23.2%），其次是 CRP（11.5%）、吸烟（7.4%）、每日饮酒量（7.1%）和 IBD 类型（6.8%）。抗肿瘤坏死因子原发性无应答EWAS确定了20个与抗肿瘤坏死因子药物浓度和抗肿瘤坏死因子原发性无应答相关的DMPs，其系数具有很强的相关性（Spearman's rho = -0.94，p < 0.001）：基线DNA甲基化图谱可用作第14周抗TNF药物浓度的预测因子，以识别可能在抗TNF治疗初期从剂量优化中获益的患者。

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

Journal of Crohns & Colitis 医学-胃肠肝病学

CiteScore

15.50

自引率

7.50%

发文量

1048

审稿时长

1 months

期刊介绍： Journal of Crohns and Colitis is concerned with the dissemination of knowledge on clinical, basic science and innovative methods related to inflammatory bowel diseases. The journal publishes original articles, review papers, editorials, leading articles, viewpoints, case reports, innovative methods and letters to the editor.