Unraveling The Genetics of Shared Clinical and Serological Manifestations in Systemic Inflammatory Autoimmune Diseases

IF 11.4 1区医学 Q1 RHEUMATOLOGY Arthritis & Rheumatology Pub Date : 2024-09-17 DOI:10.1002/art.42988

Matteo Bianchi, Sergey V. Kozyrev, Antonella Notarnicola, Johanna K. Sandling, Mats Pettersson, Dag Leonard, Christopher Sjöwall, Iva Gunnarsson, Solbritt Rantapää‐Dahlqvist, Anders A. Bengtsson, Andreas Jönsen, Elisabet Svenungsson, Helena Enocsson, Marika Kvarnström, Helena Forsblad‐d'Elia, Sara Magnusson Bucher, Katrine B. Norheim, Eva Baecklund, Roland Jonsson, Daniel Hammenfors, Per Eriksson, Thomas Mandl, Roald Omdal, Leonid Padyukov, Helena Andersson, Øyvind Molberg, Louise Pyndt Diederichsen, Ann‐Christine Syvänen, Marie Wahren‐Herlenius, Gunnel Nordmark, Ingrid E. Lundberg, Lars Rönnblom, Kerstin Lindblad‐Toh

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引用次数: 0

Abstract

OBJECTIVESSystemic inflammatory autoimmune diseases (SIADs) such as systemic lupus erythematosus (SLE), primary Sjögren's syndrome (pSS) and idiopathic inflammatory myopathies (myositis) are complex conditions characterized by shared circulating autoantibodies and clinical manifestations, including skin rashes, among others. This study aimed at elucidating the genetics underlying these common features.METHODSWe performed targeted DNA sequencing of coding and regulatory regions from ~1,900 immune‐related genes in a large SIAD cohort of 2,292 well‐characterized Scandinavian patients with SLE, pSS and myositis, as well as 1,252 controls. A gene‐based functionally‐weighted genetic score for aggregate testing of all genetic variants, including rare variants, was complemented by in‐silico functional analyses and in‐vitro reporter experiments.RESULTSCase‐control association analysis detected known and potentially novel genetic loci in agreement with previous genetic and transcriptomics findings linked to the SIAD autoimmune background. Intriguingly, case‐case comparisons between patient subgroups with and without specific autoantibodies revealed that the subgroups defined by ANA and anti‐dsDNA antibodies have unique genetic profiles reflecting their heterogeneity. When focusing on clinical features, we overall showed that DUSP1 protective genetic variants lead to increased gene expression and potentially to anti‐inflammatory effects on the SIAD‐associated skin phenotype. This is consistent with recent genetic findings on eczema and with the previously reported downregulation of the MAPK signaling‐related gene DUSP1 in other skin disorders.CONCLUSIONTogether, this suggests common molecular mechanisms potentially underlying overlapping clinical manifestations shared among different disorders and informs clinical heterogeneity, which could be translated to improve disease diagnostic and treatment, also in more generalized disease frameworks.

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揭示系统性炎症性自身免疫疾病共同临床和血清学表现的遗传学原理

目的系统性红斑狼疮（SLE）、原发性斯约格伦综合征（pSS）和特发性炎症性肌病（肌炎）等系统性炎症性自身免疫病（SIADs）是一种复杂的疾病，其特点是具有共同的循环自身抗体和临床表现，包括皮疹等。本研究旨在阐明这些共同特征的遗传学基础。方法我们在一个由 2292 名特征明确的斯堪的纳维亚系统性红斑狼疮、特发性炎症性肌病和肌炎患者以及 1252 名对照者组成的大型 SIAD 队列中，对约 1900 个免疫相关基因的编码区和调控区进行了有针对性的 DNA 测序。结果病例对照关联分析发现了已知和潜在的新基因位点，这与之前与 SIAD 自身免疫背景相关的基因和转录组学发现一致。耐人寻味的是，对有和无特异性自身抗体的患者亚组进行病例比较后发现，由ANA和抗dsDNA抗体定义的亚组具有独特的遗传特征，反映了其异质性。在关注临床特征时，我们总体上表明，DUSP1 保护性遗传变异会导致基因表达增加，并可能对 SIAD 相关皮肤表型产生抗炎作用。这与最近关于湿疹的基因研究结果以及之前报道的其他皮肤疾病中 MAPK 信号相关基因 DUSP1 的下调结果一致。结论：这一研究结果表明，在不同疾病的重叠临床表现背后可能存在共同的分子机制，并为临床异质性提供了信息，这些信息可用于改善疾病诊断和治疗，也可用于更广泛的疾病框架中。

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来源期刊

Arthritis & Rheumatology RHEUMATOLOGY-

CiteScore

20.90

自引率

3.00%

发文量

371

期刊介绍： Arthritis & Rheumatology is the official journal of the American College of Rheumatology and focuses on the natural history, pathophysiology, treatment, and outcome of rheumatic diseases. It is a peer-reviewed publication that aims to provide the highest quality basic and clinical research in this field. The journal covers a wide range of investigative areas and also includes review articles, editorials, and educational material for researchers and clinicians. Being recognized as a leading research journal in rheumatology, Arthritis & Rheumatology serves the global community of rheumatology investigators and clinicians.