白塞氏综合征中 HLA-B 基因的甲基化和表达:表观遗传学在发病机制中的潜在作用。

IF 3.4 4区 医学 Q2 RHEUMATOLOGY
Merve Özkılınç Önen, Elif Everest, Turna Demirci, Pelinsu Köprülü Şen, Esra Kızıltepe Kısakesen, Yeşim Özgüler, Sinem Nihal Esatoğlu, Emire Seyahi, Eda Tahir Turanlı
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引用次数: 0

摘要

研究目的HLA-B51位点与白塞氏综合征(BS)的关系最为密切。方法:通过序列特异性 PCR 对 15 例家族性白塞氏综合征病例、17 例患病亲属、26 例未患病亲属、46 例散发性白塞氏综合征病例和 41 例健康对照进行 HLA-B51 基因分型。使用 Zymo OneStep qMethyl 试剂盒测定 HLA-B 甲基化水平,并通过定量实时 PCR 评估 14 例家族性 BS 病例、15 例患病亲属、15 例未患病亲属、11 例散发性 BS 病例和 10 例健康对照的 HLA-B51 mRNA 水平:结果:HLA-B51携带者比例在家族性病例中为13/15,在患病亲属中为13/17,在未患病亲属中为22/26,在健康对照组中为8/25,在散发性BS病例中为35/47。HLA-B51+ BS病例的HLA-B51表达水平比未受影响的亲属高2.2倍(P=0.0149),比健康对照组高1.3倍(P=0.0188),而散发性BS病例的表达水平比健康对照组高2.7倍(P=0.0487)。HLA-B启动子甲基化在HLA-B51+家族性BS病例中明显低于未受影响的亲属(0.4倍,p=0.01)、受影响的亲属(0.36倍,p=0.0219)和健康对照组(0.34倍,p=0.0371),而在HLA-B51+散发性BS病例中则略低于健康对照组(0.71倍,p=0.2347)。在HLA-B51+散发性BS病例中,HLA-B启动子甲基化与HLA-B51表达呈反相关(p=0.0164):本研究表明,在家族性和散发性 BS 病例中,HLA-B51 基因座都与表观遗传学有关。要证实我们的研究结果,还需要更多样本量的进一步研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
HLA-B gene methylation and expression in Behçet's syndrome: a potential role of epigenetics in the pathogenesis.

Objectives: The HLA-B51 locus has the strongest association with Behçet's syndrome (BS). The presence of a CpG island in the HLA-B gene led us to examine the role of epigenetic regulation in BS.

Methods: HLA-B51 genotyping was performed via sequence-specific PCR in 15 index familial BS cases, 17 affected relatives, 26 unaffected relatives, 46 sporadic BS cases, and 41 healthy controls. HLA-B methylation level was determined using the Zymo OneStep qMethyl kit, and HLA-B51 mRNA level was assessed by quantitative real-time PCR in 14 index familial BS cases, 15 affected relatives, 15 unaffected relatives, 11 sporadic BS cases, and 10 healthy controls.

Results: HLA-B51 carrier ratio was 13/15 in index familial cases, 13/17 in affected relatives, 22/26 in unaffected relatives, 8/25 in healthy controls, and 35/47 in sporadic BS cases. HLA-B51 expression level in HLA-B51+ BS cases was 2.2-fold higher than in their unaffected relatives (p=0.0149) and 1.3-fold higher than in healthy controls (p=0.0188), while sporadic BS cases had a 2.7-fold higher level than healthy controls (p=0.0487). HLA-B promoter methylation was significantly lower in HLA-B51+ familial BS cases than in unaffected relatives (0.4-fold, p=0.01), affected relatives (0.36-fold, p=0.0219), and healthy controls (0.34-fold, p=0.0371) and slightly lower in HLA-B51+ sporadic BS cases than in healthy controls (0.71-fold, p=0.2347). There was an inverse correlation between HLA-B promoter methylation and HLA-B51 expression in HLA-B51+ sporadic BS cases (p=0.0164).

Conclusions: This study indicates epigenetic involvement associated with the HLA-B51 locus in BS, both in familial and sporadic cases. Further studies with larger sample sizes are needed to confirm our results.

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来源期刊
CiteScore
6.10
自引率
18.90%
发文量
377
审稿时长
3-6 weeks
期刊介绍: Clinical and Experimental Rheumatology is a bi-monthly international peer-reviewed journal which has been covering all clinical, experimental and translational aspects of musculoskeletal, arthritic and connective tissue diseases since 1983.
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