α2,3-唾液酸化和岩藻糖基化与快速进展的间质性肺病诱导的更严重的抗MDA5阳性皮肌炎相关。

IF 3.7 Q2 GENETICS & HEREDITY
Phenomics (Cham, Switzerland) Pub Date : 2023-03-07 eCollection Date: 2023-10-01 DOI:10.1007/s43657-023-00096-z
Rongrong Zhang, Li Guo, Jichen Sha, Shuwai Chang, Jiangfeng Zhao, Kaiwen Wang, Jiucun Wang, Jianxin Gu, Jing Liu, Shifang Ren
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引用次数: 0

摘要

皮肌炎(DM)是一种与多种肌炎特异性抗体(MSAs)相关的异质性自身免疫性疾病,其中具有抗黑色素瘤分化相关基因5阳性(MDA5 + DM)是一种独特的DM亚型,其发展为不同程度间质性肺病(ILD)的风险较高。糖基化是与许多自身免疫性疾病相关的蛋白质的复杂翻译后修饰。然而,血浆总N-糖组(TPNG)与DM,尤其是MDA5的相关性 + DM仍然未知。94名糖尿病患者和168名对照者的TPNG通过质谱法进行分析,采用内部可靠的定量方法称为仿生糖组分法。经年龄和性别调整后的Logistic回归用于揭示糖尿病的异常糖基化以及TPNG和MDA5的相关性 + 伴有或不伴有快速进行性ILD(RPILD)的DM。使用弹性网模型来评估聚糖在区分RPLID和非RPILD方面的性能,并通过Kaplan-Meier生存分析用N-糖酵解评分分析生存分析。研究发现,与对照组相比,DM患者的血浆蛋白N-糖组表现出更高的岩藻糖基化和二等分,更低的唾液酸化(α2,3-非α2,6-连接)和半乳糖基化。在MDA5中 + DM,更严重的疾病状况与唾液酸化减少(特别是α2,3-岩藻糖基化分析)有关,同时伴有H6N5S3和H5N4FSx升高,半乳糖基化减少和岩藻糖基化增加以及N-聚糖的复杂性。此外,糖基化特征比临床特征具有更好的区分RPILD和非RPILD的能力,AUC为0.922,并且是MDA5独立性的。MDA5的生存优势 + 糖尿病患者的N-糖基化评分较低(p = 3e-04)。我们的研究首次揭示了糖尿病的异常糖基化,并表明糖基化与MDA5中ILD引起的疾病严重程度有关 + DM,可能被认为是RPILD早期诊断和MDA5生存评估的潜在生物标志物 + DM.补充信息:在线版本包含补充材料,可访问10.1007/s43657-023-00096-z。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
α2,3-Sialylation with Fucosylation Associated with More Severe Anti-MDA5 Positive Dermatomyositis Induced by Rapidly Progressive Interstitial Lung Disease.

Dermatomyositis (DM) is a heterogeneous autoimmune disease associated with numerous myositis specific antibodies (MSAs) in which DM with anti-melanoma differentiation-associated gene 5-positive (MDA5 + DM) is a unique subtype of DM with higher risk of developing varying degrees of Interstitial lung disease (ILD). Glycosylation is a complex posttranslational modification of proteins associated with many autoimmune diseases. However, the association of total plasma N-glycome (TPNG) and DM, especially MDA5 + DM, is still unknown. TPNG of 94 DM patients and 168 controls were analyzed by mass spectrometry with in-house reliable quantitative method called Bionic Glycome method. Logistic regression with age and sex adjusted was used to reveal the aberrant glycosylation of DM and the association of TPNG and MDA5 + DM with or without rapidly progressive ILD (RPILD). The elastic net model was used to evaluate performance of glycans in distinguishing RPLID from non-RPILD, and survival analysis was analyzed with N-glycoslyation score by Kaplan-Meier survival analysis. It was found that the plasma protein N-glycome in DM showed higher fucosylation and bisection, lower sialylation (α2,3- not α2,6-linked) and galactosylation than controls. In MDA5 + DM, more severe disease condition was associated with decreased sialylation (specifically α2,3-sialylation with fucosylation) while accompanying elevated H6N5S3 and H5N4FSx, decreased galactosylation and increased fucosylation and the complexity of N-glycans. Moreover, glycosylation traits have better discrimination ability to distinguish RPILD from non-RPILD with AUC 0.922 than clinical features and is MDA5-independent. Survival advantage accrued to MDA5 + DM with lower N-glycosylation score (p = 3e-04). Our study reveals the aberrant glycosylation of DM for the first time and indicated that glycosylation is associated with disease severity caused by ILD in MDA5 + DM, which might be considered as the potential biomarker for early diagnosis of RPILD and survival evaluation of MDA5 + DM.

Supplementary information: The online version contains supplementary material available at 10.1007/s43657-023-00096-z.

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