伴有 COL4A3 基因突变的家族性 IgAN 分析

IF 4.2 2区医学 Q2 IMMUNOLOGY

Journal of Inflammation Research Pub Date : 2024-11-20 eCollection Date: 2024-01-01 DOI:10.2147/JIR.S480279

Sen-Qing Lin, Jin-Xiu Deng, Hui Jiang, Shi-Hong Xiang, Wen-Jing Lin, Feng-Qi Qian, Sen-Chao Wu, Fu-Zhen Wang

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引用次数: 0

摘要

目的：IgA 肾病（IgAN）是全球最常见的原发性肾小球肾炎，也是导致慢性肾病发病并最终发展为终末期肾病的关键因素。本研究旨在探讨家族性 IgAN 病例中的突变基因，尤其是 COL4A3：方法：选取福建医科大学附属龙岩第一医院确诊为家族性 IgAN 的家系为研究对象，进行全外显子组测序。获得测序数据后，进行生物信息学分析，以发现潜在的突变基因。根据文献参考并按照美国医学遗传学和基因组学学院确定的遗传变异分类标准，使用 Sanger 测序法鉴定 IgAN 相关突变基因，从而验证了家族性血统中的这些发现：通过对家族性 IgAN 家系进行全外显子测序分析，共鉴定出 212,187 个单核苷酸变异/插入缺失突变位点，并使用 ANNOVAR 进行了注释。针对四个突变基因对这些位点进行了筛选，发现了三个意义不明的突变和一个致病突变：COL4A3（p.G1167R）中的一个杂合致病突变。该突变在该组的七个家庭成员中均有表现，包括确诊为肾病的家庭成员和正常携带者。值得注意的是，家族中还有一名 IgAN 患者没有出现致病突变：这项研究发现了四个可能与 IgAN 发病和进展有关的突变基因，进一步揭示了 IgAN 复杂的多基因遗传特征。这种疾病的潜在机制还需要进一步研究。此外，我们还发现了与已知遗传性肾病相关的潜在突变，如 COL4A3 突变。因此，我们建议对家族性 IgAN 病例进行全面的基因筛查，以提高疾病诊断水平，方便遗传咨询。

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Analysis of a Familial IgAN Accompanied by COL4A3 Mutation.

Objective: IgA nephropathy (IgAN) is the prevailing primary glomerulonephritis globally and is the key factor contributing to the onset of chronic kidney disease and eventual progression to end-stage renal disease. This study aims to explore the mutated gene in a familial case of IgAN, especially COL4A3.

Methods: Family lineages diagnosed with familial IgAN at the Longyan First Hospital of Fujian Medical University were selected for this study, followed by comprehensive whole exome sequencing. After obtaining the sequencing data, bioinformatics analyses were conducted to discern potential mutated genes. These findings within the familial lineages were validated using Sanger sequencing to identify IgAN-associated mutated genes, based on literature references and in accordance with the genetic variation classification criteria determined by the American College of Medical Genetics and Genomics.

Results: Whole exome sequencing analysis of familial IgAN family lineages led to the identification of a total of 212,187 single nucleotide variant/insertion-deletion mutation sites, annotated using ANNOVAR. These sites were screened targeting four mutated genes, revealing three mutations of undetermined significance along with a single disease-causing mutation: a heterozygous disease-causing mutation within COL4A3 (p.G1167R). This mutation manifested across seven family members within the group, encompassing both family members diagnosed with kidney disease and those serving as normal carriers. Notably, one additional family member with IgAN within the familial lineage exhibited an absence of the pathogenic mutation.

Conclusion: This study identified four mutated genes that may be involved in the onset and progression of IgAN, further revealing the complex multigenic inheritance characteristics of IgAN. The underlying mechanisms of the disease require further investigation. Additionally, we discovered potential mutations associated with known genetic kidney diseases, such as COL4A3 mutations. Therefore, we recommend comprehensive genetic screening in familial cases of IgAN to improve disease diagnosis and facilitate genetic counseling.

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来源期刊

Journal of Inflammation Research Immunology and Microbiology-Immunology

CiteScore

6.10

自引率

2.20%

发文量

658

审稿时长

16 weeks

期刊介绍： An international, peer-reviewed, open access, online journal that welcomes laboratory and clinical findings on the molecular basis, cell biology and pharmacology of inflammation.