Departments of Nephrology, Faculty of Medicine, School of Health Sciences, University of Thessaly, 41334 Larissa, Greece.
Laboratory of Neurogenetics, Department of Neurology, University of Thessaly, University Hospital of Larissa, 41334 Larissa, Greece.
Int J Mol Sci. 2023 Nov 15;24(22):16347. doi: 10.3390/ijms242216347.
The interleukin-1 gene cluster encodes cytokines, which modulate mesangial cell proliferation and matrix expansion, both constituting central factors in the development and progression of immunoglobulin A nephropathy (IgAN). A candidate-gene study was performed to examine the association of polymorphisms of the interleukin-1 gene cluster with the risk of progressive IgAN. To gain deeper insights into the involvement of interleukin genes in IgAN, a meta-analysis of genetic association studies (GAS) that examine the association between interleukin variants and IgAN was conducted. Association study: The case-control study consisted of 121 unrelated Caucasians with sporadic, histologically diagnosed IgAN and of 246 age- and sex-matched healthy controls. Persistent proteinuria (>2 g/24 h) and/or impaired kidney function (serum creatinine > 1.5 mg/dL) defined progressive (n = 67) vs. non-progressive (n = 54) IgAN cases. Genotypes were assessed for two promoter-region single-nucleotide polymorphisms, C-899T (rs1800587) in and C-511T (rs16944) in , and for one penta-allelic variable-length tandem repeat polymorphism (VNTR 86 bp intron 2) in . The association of these variants with the susceptibility of IgAN and the development of progressive IgAN (healthy status, IgAN, progressive IgAN) was tested using the generalized odds ratio (OR) metric. Linkage disequilibrium and haplotype analysis were also performed. Meta-analysis: We included in the meta-analysis 15 studies investigating association between 14 interleukin variants harbored in eight different genes and IgAN. The OR was used to evaluate the association between interleukin variants and IgAN using random effects models. The present case-control study revealed association of C-511T (rs16944) with the progression of IgAN ( = 0.041; OR = 2.11 (1.09-4.07)). On haplotype analysis, significant results were derived for the haplotypes C-C-1 ( = 0.005; OR = 0.456 (0.261~0.797)) and C-T-2 ( = 0.003; OR = 4.208 (1.545-11.50)). Regarding association and meta-analysis results, variants in (rs1143627 and rs16944), (rs928940, rs439154, and rs315951) and (rs1800871) were associated with IgAN based on either genotype or allele counts. Genetic variants and haplotypes in the , and genes might contribute to an increased risk for development and progression of IgAN.
白细胞介素-1 基因簇编码细胞因子,调节系膜细胞增殖和基质扩张,这两者都是免疫球蛋白 A 肾病(IgAN)发展和进展的核心因素。进行了候选基因研究,以检查白细胞介素基因簇的多态性与进行性 IgAN 的风险之间的关联。为了更深入地了解白细胞介素基因在 IgAN 中的参与,对检查白细胞介素变异与 IgAN 之间关联的遗传关联研究(GAS)进行了荟萃分析。关联研究:该病例对照研究包括 121 名无关的白种人,患有散发性、组织学诊断的 IgAN 和 246 名年龄和性别匹配的健康对照者。持续性蛋白尿(>2 g/24 h)和/或肾功能受损(血清肌酐>1.5 mg/dL)定义为进行性(n=67)与非进行性(n=54)IgAN 病例。为两个启动子区域单核苷酸多态性 C-899T(rs1800587)在 和 C-511T(rs16944)在 以及一个五等位基因可变长度串联重复多态性(VNTR 86 bp 内含子 2)进行基因型评估。使用广义优势比(OR)度量来测试这些变体与 IgAN 的易感性和进行性 IgAN(健康状况、IgAN、进行性 IgAN)的发展之间的关联。还进行了连锁不平衡和单倍型分析。荟萃分析:我们纳入了 15 项研究,这些研究调查了 8 个不同基因中 14 个白细胞介素变体与 IgAN 之间的关联。使用随机效应模型使用 OR 来评估白细胞介素变体与 IgAN 之间的关联。本病例对照研究显示 C-511T(rs16944)与 IgAN 的进展相关( = 0.041;OR = 2.11(1.09-4.07))。在单倍型分析中,C-C-1 单倍型( = 0.005;OR = 0.456(0.261~0.797))和 C-T-2 单倍型( = 0.003;OR = 4.208(1.545-11.50))得出了显著结果。关于关联和荟萃分析结果,基于基因型或等位基因计数, 中的变体(rs1143627 和 rs16944)、 (rs928940、rs439154 和 rs315951)和 (rs1800871)与 IgAN 相关。 、 和 基因中的遗传变异和单倍型可能导致 IgAN 发展和进展的风险增加。
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