Discovery of new myositis genetic associations through leveraging other immune-mediated diseases.

IF 3.3 Q2 GENETICS & HEREDITY HGG Advances Pub Date : 2024-10-10 Epub Date: 2024-07-22 DOI:10.1016/j.xhgg.2024.100336
Guillermo Reales, Christopher I Amos, Olivier Benveniste, Hector Chinoy, Jan De Bleecker, Boel De Paepe, Andrea Doria, Peter K Gregersen, Janine A Lamb, Vidya Limaye, Ingrid E Lundberg, Pedro M Machado, Britta Maurer, Frederick W Miller, Øyvind Molberg, Lauren M Pachman, Leonid Padyukov, Timothy R Radstake, Ann M Reed, Lisa G Rider, Simon Rothwell, Albert Selva-O'Callaghan, Jiri Vencovský, Lucy R Wedderburn, Chris Wallace
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Abstract

Genome-wide association studies (GWASs) have been successful at finding associations between genetic variants and human traits, including the immune-mediated diseases (IMDs). However, the requirement of large sample sizes for discovery poses a challenge for learning about less common diseases, where increasing volunteer numbers might not be feasible. An example of this is myositis (or idiopathic inflammatory myopathies [IIM]s), a group of rare, heterogeneous autoimmune diseases affecting skeletal muscle and other organs, severely impairing life quality. Here, we applied a feature engineering method to borrow information from larger IMD GWASs to find new genetic associations with IIM and its subgroups. Combining this approach with two clustering methods, we found 17 IMDs genetically close to IIM, including some common comorbid conditions, such as systemic sclerosis and Sjögren's syndrome, as well as hypo- and hyperthyroidism. All IIM subtypes were genetically similar within this framework. Next, we colocalized IIM signals that overlapped IMD signals, and found seven potentially novel myositis associations mapped to immune-related genes, including BLK, IRF5/TNPO3, and ITK/HAVCR2, implicating a role for both B and T cells in IIM. This work proposes a new paradigm of genetic discovery in rarer diseases by leveraging information from more common IMD, and can be expanded to other conditions and traits beyond IMD.

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通过利用其他免疫介导疾病,发现新的肌炎基因关联。
全基因组关联研究(GWAS)成功地发现了基因变异与人类特征(包括免疫介导疾病)之间的关联。然而,发现疾病需要大量样本,这给了解不常见疾病带来了挑战,因为增加志愿者人数可能并不可行。肌炎(或特发性炎症性肌病,IIM)就是一个例子,这是一组罕见的异质性自身免疫性疾病,影响骨骼肌和其他器官,严重影响生活质量。在这里,我们采用了一种特征工程方法,从更大的 IMD GWAS 中借用信息,寻找与 IIM 及其亚群的新的遗传关联。将这种方法与两种聚类方法相结合,我们发现有 17 种 IMD 在遗传学上与 IIM 相似,其中包括一些常见的合并症,如系统性硬化症和斯约格伦综合征,以及甲状腺功能减退症和甲状腺功能亢进症。在这一框架内,所有 IIM 亚型在遗传学上都是相似的。接下来,我们对与 IMD 信号重叠的 IIM 信号进行了共定位,发现了与免疫相关基因(包括 BLK、IRF5/TNPO3 和 ITK/HAVCR2)相关的七种潜在的新型肌炎关联,这意味着 B 细胞和 T 细胞在 IIM 中都扮演着重要角色。这项研究利用更常见的肌萎缩性肌炎的信息,提出了一种发现罕见疾病基因的新模式,并可扩展到肌萎缩性肌炎以外的其他疾病和性状。
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
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
期刊最新文献
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