Identification of susceptibility loci and relevant cell type for IgA nephropathy in Han Chinese by integrative genome-wide analysis.

IF 3.9 3区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL Frontiers of Medicine Pub Date : 2024-10-01 Epub Date: 2024-09-30 DOI:10.1007/s11684-024-1086-2
Ming Li, Xingjie Hao, Dianchun Shi, Shanshan Cheng, Zhong Zhong, Lu Cai, Minghui Jiang, Lin Ding, Lanbo Ding, Chaolong Wang, Xueqing Yu
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Abstract

Although many susceptibility loci for IgA nephropathy (IgAN) have been identified, they only account for 11.0% of the overall IgAN variance. We performed a large genome-wide meta-analysis of IgAN in Han Chinese with 3616 cases and 10 417 controls to identify additional genetic loci of IgAN. Considering that inflammatory bowel disease (IBD) and asthma might share an etiology of dysregulated mucosal immunity with IgAN, we performed cross-trait integrative analysis by leveraging functional annotations of relevant cell type and the pleiotropic information from IBD and asthma. Among 8 669 456 imputed variants, we identified a novel locus at 4p14 containing the long noncoding RNA LOC101060498. Cell type enrichment analysis based on annotations suggested that PMA-I-stimulated CD4+CD25-IL17+ Th17 cell was the most relevant cell type for IgAN, which highlights the essential role of Th17 pathway in the pathogenesis of IgAN. Furthermore, we identified six more novel loci associated with IgAN, which included three loci showing pleiotropic effects with IBD or asthma (2q35/PNKD, 6q25.2/SCAF8, and 22q11.21/UBE2L3) and three loci specific to IgAN (14q32.32/TRAF3, 16q22.2/TXNL4B, and 21q21.3/LINC00113) in the pleiotropic analysis. Our findings support the involvement of mucosal immunity, especially T cell immune response and IL-17 signal pathway, in the development of IgAN and shed light on further investigation of IgAN.

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通过全基因组整合分析确定汉族人 IgA 肾病的易感基因位点和相关细胞类型
虽然已经发现了许多 IgA 肾病(IgAN)的易感基因位点,但它们只占 IgAN 整体变异的 11.0%。我们对 3616 例汉族 IgAN 病例和 10 417 例对照进行了大型全基因组荟萃分析,以确定 IgAN 的其他遗传位点。考虑到炎症性肠病(IBD)和哮喘可能与 IgAN 具有共同的粘膜免疫失调病因,我们利用相关细胞类型的功能注释以及来自 IBD 和哮喘的多效应信息进行了跨性状整合分析。在 8 669 456 个估算变异中,我们在 4p14 发现了一个包含长非编码 RNA LOC101060498 的新位点。基于注释的细胞类型富集分析表明,PMA-I刺激的CD4+CD25-IL17+ Th17细胞是与IgAN最相关的细胞类型,这突显了Th17通路在IgAN发病机制中的重要作用。此外,我们还发现了六个与IgAN相关的新位点,其中包括与IBD或哮喘有多效应的三个位点(2q35/PNKD、6q25.2/SCAF8和22q11.21/UBE2L3),以及在多效应分析中与IgAN特异的三个位点(14q32.32/TRAF3、16q22.2/TXNL4B和21q21.3/LINC00113)。我们的研究结果支持粘膜免疫,尤其是T细胞免疫反应和IL-17信号通路参与了IgAN的发病,并为进一步研究IgAN提供了启示。
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来源期刊
Frontiers of Medicine
Frontiers of Medicine ONCOLOGYMEDICINE, RESEARCH & EXPERIMENTAL&-MEDICINE, RESEARCH & EXPERIMENTAL
CiteScore
18.30
自引率
0.00%
发文量
800
期刊介绍: Frontiers of Medicine is an international general medical journal sponsored by the Ministry of Education of China. The journal is jointly published by the Higher Education Press and Springer. Since the first issue of 2010, this journal has been indexed in PubMed/MEDLINE. Frontiers of Medicine is dedicated to publishing original research and review articles on the latest advances in clinical and basic medicine with a focus on epidemiology, traditional Chinese medicine, translational research, healthcare, public health and health policies.
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