Causal relationships between immune cell phenotypes and primary glomerular diseases: genetic evidence from bidirectional Mendelian randomization study.

IF 3.9 2区医学 Q1 UROLOGY & NEPHROLOGY

Clinical Kidney Journal Pub Date : 2025-02-24 eCollection Date: 2025-03-01 DOI:10.1093/ckj/sfaf057

Wenhao Tang, Qiu Li, Xueying Yang, Haiping Yang

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引用次数: 0

Abstract

Background: Primary glomerular diseases (PGDs), including nephrotic syndrome (NS), membranous nephropathy (MN), and IgA nephropathy (IgAN), are complex renal conditions influenced by immune system dysregulation. Although associations between immune cell phenotypes and PGDs have been observed, the precise causal relationships have not been fully elucidated.

Methods: Utilizing genetic association data from genome-wide association studies (GWASs), we investigated 731 immunophenotypes in relation to PGDs. A bidirectional two-sample Mendelian randomization (MR) approach, primarily employing inverse variance weighting (IVW), was conducted to establish causality. MR-Egger, weighted median, simple mode, and weighted mode were used as complementary methods to reinforce the robustness and validity of the results. Sensitivity analyses further validated the sensitivity and stability of our results.

Results: We identified 38 immunophenotypes suggestively related to IgAN, with 20 as risk factors and 18 as protective effects. Six immunophenotypes remained significant after Bonferroni correction: The percentage of CD25hi among T cells; the percentage of CD25hi CD45RA^- CD4 not T regulatory (Treg) among T cells; the percentage of CD25hi CD45RA^- CD4 not Treg within the CD4⁺ T cell population; CX3CR1 expression on monocytes; CD40 expression on monocytes; and CD64 expression on CD14⁺ CD16^- monocytes. In the validation analysis of IgAN, CD3 expression on effector memory CD4⁺ T cells further confirmed the predisposing risk role of effector memory T cells in the development of IgAN. Additionally, the MR analysis demonstrated suggestive associations between 25 immunophenotypes and MN (8 risk factors and 17 protective factors), as well as between 22 immunophenotypes and NS (10 risk factors and 12 protective factors). Last, by intersecting the immunophenotypes showing suggestive associations with PGDs, we identified two common immunophenotypes shared by IgAN and MN, three by IgAN and NS, and one by MN and NS.

Conclusions: This genetic-level investigation uncovers causal associations between immunophenotypes and PGDs, providing valuable insights into the immunological underpinnings of PGDs. Our findings suggest potential targets for treatment strategies, thereby facilitating more personalized and effective therapeutic approaches in PGDs management.

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免疫细胞表型与原发性肾小球疾病之间的因果关系：双向孟德尔随机化研究的遗传证据

背景：原发性肾小球疾病（PGDs），包括肾病综合征（NS）、膜性肾病（MN）和IgA肾病（IgAN），是由免疫系统失调影响的复杂肾脏疾病。虽然已经观察到免疫细胞表型和pgd之间的关联，但精确的因果关系尚未完全阐明。方法：利用全基因组关联研究（GWASs）的遗传关联数据，研究了731种与PGDs相关的免疫表型。采用双向双样本孟德尔随机化（MR）方法，主要采用逆方差加权（IVW）来确定因果关系。采用MR-Egger、加权中位数、简单模型和加权模型作为补充方法，以增强结果的稳健性和有效性。敏感性分析进一步验证了结果的敏感性和稳定性。结果：我们确定了38种与IgAN相关的免疫表型，其中20种为危险因素，18种为保护作用。经Bonferroni校正后，6种免疫表型仍然显著：T细胞中CD25hi的百分比；T细胞中CD25hi - CD45RA- CD4非T调节性（Treg）百分比；CD4+ T细胞群中CD25hi CD45RA- CD4非Treg的百分比；CX3CR1在单核细胞中的表达；CD40在单核细胞中的表达；CD14+ CD16-单核细胞中CD64的表达。在IgAN的验证分析中，CD3在效应记忆CD4+ T细胞上的表达进一步证实了效应记忆T细胞在IgAN发生发展中的易感风险作用。此外，MR分析显示，25种免疫表型与MN（8个危险因素和17个保护因素）以及22种免疫表型与NS（10个危险因素和12个保护因素）之间存在相关性。最后，通过交叉显示与PGDs相关的免疫表型，我们确定了IgAN和MN共有的两种常见免疫表型，IgAN和NS共有的三种，MN和NS共有的一种。结论：这项遗传学水平的研究揭示了免疫表型与PGDs之间的因果关系，为PGDs的免疫学基础提供了有价值的见解。我们的研究结果提示了治疗策略的潜在目标，从而促进了更个性化和有效的治疗方法在PGDs管理中。

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

Clinical Kidney Journal Medicine-Transplantation

CiteScore

6.70

自引率

10.90%

发文量

242

审稿时长

8 weeks

期刊介绍： About the Journal Clinical Kidney Journal: Clinical and Translational Nephrology (ckj), an official journal of the ERA-EDTA (European Renal Association-European Dialysis and Transplant Association), is a fully open access, online only journal publishing bimonthly. The journal is an essential educational and training resource integrating clinical, translational and educational research into clinical practice. ckj aims to contribute to a translational research culture among nephrologists and kidney pathologists that helps close the gap between basic researchers and practicing clinicians and promote sorely needed innovation in the Nephrology field. All research articles in this journal have undergone peer review.