The causal role of immune cells in primary Sjögren's syndrome: A two-sample Mendelian randomization

IF 2.4 4区医学 Q2 RHEUMATOLOGY International Journal of Rheumatic Diseases Pub Date : 2024-11-18 DOI:10.1111/1756-185X.15350

Yang Liu, Jie Kang, Yazhen Su, Xiuying Fan, Dan Ma, Zewen Wu, Xueyan Gong, Junkang Zhao, Liyun Zhang

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Abstract

Background

Primary Sjögren's syndrome (pSS) is an autoimmune disease characterized by the destruction of exocrine glands primarily via T-cell-mediated B-cell over-activation and cytokine production. This leads to pronounced dryness of the mouth and eyes and can result in multi-systemic involvement affecting the kidneys, lungs, and blood. In recent years, there has been increasing attention on the role of immune cells in pSS. However, studies investigating the causal role of immune cells in pSS have been relatively limited.

Methods

In this study, we employed a two-way two-sample Mendelian randomization approach to assess the causal relationship between immune cells and pSS. Utilizing publicly available genome-wide association study (GWAS) data, we explored the causal links between 731 immunophenotypically labeled immune cells and the risk of pSS.

Results

Through the use of instrumental variables derived from GWAS data and corrected for false discovery rate (FDR), we identified three immune cells with increased levels that were causally associated with pSS risk (FDR < 0.05). These included IgD+ CD38br AC B cells, CD27 on IgD+ CD38− unswitched memory B cells, and Granulocyte % leukocyte. Additionally, three immune cells with reduced levels were found to be causally associated with pSS risk, namely CD4+ CD8dim %lymphocyte, CD4+ CD8dim %leukocyte, and CD28 on activated and secreting regulatory T cells (Tregs). Furthermore, the development of pSS was associated with elevated levels of CD33br HLA DR+ CD14− % CD33br HLA DR+ in myeloid cells.

Conclusion

This study demonstrates that immune responses influence the progression of pSS in a complex pattern. Our findings may provide new insights into the immunology of pSS pathogenesis and more experimental studies should be conducted to further explore the potential mechanisms between identified immune features and pSS risk, which may provide a basis for exploring early intervention methods for pSS and developing targeted therapeutic strategies or even reshaping immune homeostasis.

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免疫细胞在原发性斯约格伦综合征中的因果作用：双样本孟德尔随机试验

背景原发性斯约格伦综合征（pSS）是一种自身免疫性疾病，主要通过 T 细胞介导的 B 细胞过度激活和细胞因子的产生破坏外分泌腺体。这种疾病会导致明显的口眼干燥，并可累及肾脏、肺部和血液等多系统。近年来，人们越来越关注免疫细胞在 pSS 中的作用。然而，有关免疫细胞在 pSS 中的因果作用的研究却相对有限。方法在本研究中，我们采用了双向双样本孟德尔随机方法来评估免疫细胞与 pSS 之间的因果关系。利用公开的全基因组关联研究（GWAS）数据，我们探讨了 731 个免疫表型标记的免疫细胞与 pSS 风险之间的因果关系。结果通过使用来自 GWAS 数据的工具变量并校正误发现率 (FDR)，我们确定了三种免疫细胞水平的升高与 pSS 风险存在因果关系（FDR < 0.05）。这些免疫细胞包括 IgD+ CD38br AC B 细胞、IgD+ CD38- unswitched 记忆 B 细胞上的 CD27 和粒细胞%白细胞。此外，还发现三种免疫细胞水平降低与 pSS 风险有因果关系，即 CD4+ CD8dim %淋巴细胞、CD4+ CD8dim %白细胞和活化分泌调节性 T 细胞（Tregs）上的 CD28。此外，pSS 的发生与骨髓细胞中 CD33br HLA DR+ CD14- % CD33br HLA DR+ 水平升高有关。结论本研究表明，免疫反应以一种复杂的模式影响着 pSS 的进展。我们的研究结果可能会为 pSS 发病的免疫学提供新的见解，因此应开展更多的实验研究，进一步探讨已发现的免疫特征与 pSS 风险之间的潜在机制，从而为探索 pSS 早期干预方法、开发靶向治疗策略甚至重塑免疫稳态提供依据。

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来源期刊

International Journal of Rheumatic Diseases RHEUMATOLOGY-

CiteScore

3.70

自引率

4.00%

发文量

362

审稿时长

1 months

期刊介绍： The International Journal of Rheumatic Diseases (formerly APLAR Journal of Rheumatology) is the official journal of the Asia Pacific League of Associations for Rheumatology. The Journal accepts original articles on clinical or experimental research pertinent to the rheumatic diseases, work on connective tissue diseases and other immune and allergic disorders. The acceptance criteria for all papers are the quality and originality of the research and its significance to our readership. Except where otherwise stated, manuscripts are peer reviewed by two anonymous reviewers and the Editor.