Centre for Genomics and Personalised Health and School of Biomedical Sciences, Queensland University of Technology, Brisbane, QLD, Australia.
Centre of chronic disease, Faculty of Medicine, University of Queensland, Brisbane, QLD, Australia.
Genome Med. 2024 Feb 12;16(1):29. doi: 10.1186/s13073-024-01299-3.
Chronic kidney disease (CKD) is highly prevalent among Indigenous Australians, especially those in remote regions. The Tiwi population has been isolated from mainland Australia for millennia and exhibits unique genetic characteristics that distinguish them from other Indigenous and non-Indigenous populations. Notably, the rate of end-stage renal disease is up to 20 times greater in this population compared to non-Indigenous populations. Despite the identification of numerous genetic loci associated with kidney disease through GWAS, the Indigenous population such as Tiwi remains severely underrepresented and the increased prevalence of CKD in this population may be due to unique disease-causing alleles/genes.
We used albumin-to-creatinine ratio (ACR) and estimated glomerular filtration rate (eGFR) to estimate the prevalence of kidney disease in the Tiwi population (N = 492) in comparison to the UK Biobank (UKBB) (N = 134,724) database. We then performed an exploratory factor analysis to identify correlations among 10 CKD-related phenotypes and identify new multi-phenotype factors. We subsequently conducted a genome-wide association study (GWAS) on all single and multiple phenotype factors using mixed linear regression models, adjusted for age, sex, population stratification, and genetic relatedness between individuals.
Based on ACR, 20.3% of the population was at severely increased risk of CKD progression and showed elevated levels of ACR compared to the UKBB population independent of HbA1c. A GWAS of ACR revealed novel association loci in the genes MEG3 (chr14:100812018:T:A), RAB36 (rs11704318), and TIAM2 (rs9689640). Additionally, multiple phenotypes GWAS of ACR, eGFR, urine albumin, and serum creatinine identified a novel variant that mapped to the gene MEIS2 (chr15:37218869:A:G). Most of the identified variants were found to be either absent or rare in the UKBB population.
Our study highlights the Tiwi population's predisposition towards elevated ACR, and the collection of novel genetic variants associated with kidney function. These associations may prove valuable in the early diagnosis and treatment of renal disease in this underrepresented population. Additionally, further research is needed to comprehensively validate the functions of the identified variants/genes.
慢性肾脏病(CKD)在澳大利亚原住民中发病率很高,尤其是在偏远地区。提维人已经与世隔绝了几千年,他们有着独特的遗传特征,与其他原住民和非原住民群体不同。值得注意的是,该人群终末期肾病的发病率比非原住民群体高 20 倍。尽管通过全基因组关联研究(GWAS)已经确定了许多与肾脏疾病相关的遗传位点,但提维人等原住民群体的代表性仍然严重不足,而该人群 CKD 的高发率可能是由于独特的致病等位基因/基因所致。
我们使用白蛋白与肌酐比值(ACR)和估计肾小球滤过率(eGFR)来评估提维人群(N=492)的肾脏疾病患病率,并与英国生物银行(UKBB)(N=134724)数据库进行比较。然后,我们进行了探索性因素分析,以确定 10 种与 CKD 相关表型之间的相关性,并确定新的多表型因素。随后,我们使用混合线性回归模型对所有单一和多表型因素进行全基因组关联研究(GWAS),并对个体年龄、性别、人群分层和遗传相关性进行了调整。
根据 ACR,20.3%的人群患有严重的 CKD 进展风险,并且与 UKBB 人群相比,ACR 水平升高,与 HbA1c 无关。ACR 的 GWAS 揭示了 MEG3(chr14:100812018:T:A)、RAB36(rs11704318)和 TIAM2(rs9689640)基因中的新关联位点。此外,ACR、eGFR、尿白蛋白和血清肌酐的多表型 GWAS 确定了一个新的变异,该变异映射到 MEIS2 基因(chr15:37218869:A:G)。大多数鉴定的变异在 UKBB 人群中要么不存在,要么罕见。
我们的研究强调了提维人群对 ACR 升高的易感性,以及与肾功能相关的新遗传变异的发现。这些关联可能对该代表性不足的人群中肾脏疾病的早期诊断和治疗具有重要意义。此外,还需要进一步研究来全面验证鉴定出的变异/基因的功能。
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