Mitochondrial genetic variation and risk of chronic kidney disease and acute kidney injury in UK Biobank participants.

IF 3.8 2区 生物学 Q2 GENETICS & HEREDITY Human Genetics Pub Date : 2024-02-01 Epub Date: 2024-02-13 DOI:10.1007/s00439-023-02615-4
Vasantha Jotwani, Stephanie Y Yang, Heather Thiessen-Philbrook, Chirag R Parikh, Ronit Katz, Gregory J Tranah, Joachim H Ix, Steve Cummings, Sushrut S Waikar, Michael G Shlipak, Mark J Sarnak, Samir M Parikh, Dan E Arking
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Abstract

Experimental models suggest an important role for mitochondrial dysfunction in the pathogenesis of chronic kidney disease (CKD) and acute kidney injury (AKI), but little is known regarding the impact of common mitochondrial genetic variation on kidney health. We sought to evaluate associations of inherited mitochondrial DNA (mtDNA) variation with risk of CKD and AKI in a large population-based cohort. We categorized UK Biobank participants who self-identified as white into eight distinct mtDNA haplotypes, which were previously identified based on their associations with phenotypes associated with mitochondrial DNA copy number, a measure of mitochondrial function. We used linear and logistic regression models to evaluate associations of these mtDNA haplotypes with estimated glomerular filtration rate by serum creatinine and cystatin C (eGFRCr-CysC, N = 362,802), prevalent (N = 416 cases) and incident (N = 405 cases) end-stage kidney disease (ESKD), AKI defined by diagnostic codes (N = 14,170 cases), and urine albumin/creatinine ratio (ACR, N = 114,662). The mean age was 57 ± 8 years and the mean eGFR was 90 ± 14 ml/min/1.73 m2. MtDNA haplotype was significantly associated with eGFR (p = 2.8E-12), but not with prevalent ESKD (p = 5.9E-2), incident ESKD (p = 0.93), AKI (p = 0.26), or urine ACR (p = 0.54). The association of mtDNA haplotype with eGFR remained significant after adjustment for diabetes mellitus and hypertension (p = 1.2E-10). When compared to the reference haplotype, mtDNA haplotypes I (β = 0.402, standard error (SE) = 0.111; p = 2.7E-4), IV (β = 0.430, SE = 0.073; p = 4.2E-9), and V (β = 0.233, SE = 0.050; p = 2.7E-6) were each associated with higher eGFR. Among self-identified white UK Biobank participants, mtDNA haplotype was associated with eGFR, but not with ESKD, AKI or albuminuria.

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英国生物库参与者的线粒体基因变异与慢性肾病和急性肾损伤的风险。
实验模型表明,线粒体功能障碍在慢性肾脏病(CKD)和急性肾损伤(AKI)的发病机制中起着重要作用,但人们对常见线粒体遗传变异对肾脏健康的影响知之甚少。我们试图在一个大型人群队列中评估遗传线粒体 DNA(mtDNA)变异与 CKD 和 AKI 风险的关系。我们将自认为是白人的英国生物库参与者分为 8 个不同的 mtDNA 单倍型,这些单倍型是之前根据它们与线粒体 DNA 拷贝数(线粒体功能的测量指标)相关表型的关系确定的。我们使用线性和逻辑回归模型评估了这些 mtDNA 单倍型与血清肌酐和胱抑素 C 估计肾小球滤过率(eGFRCr-CysC,N = 362 802)、流行性(N = 416 例)和偶发性(N = 405 例)终末期肾病(ESKD)、诊断代码定义的 AKI(N = 14 170 例)以及尿白蛋白/肌酐比值(ACR,N = 114 662)的相关性。平均年龄为 57 ± 8 岁,平均 eGFR 为 90 ± 14 ml/min/1.73 m2。mtDNA单倍型与eGFR(p = 2.8E-12)显著相关,但与流行性ESKD(p = 5.9E-2)、偶发性ESKD(p = 0.93)、AKI(p = 0.26)或尿液ACR(p = 0.54)无关。在对糖尿病和高血压进行调整后,mtDNA单倍型与eGFR的关系仍然显著(p = 1.2E-10)。与参考单倍型相比,mtDNA 单倍型 I(β = 0.402,标准误差 (SE) = 0.111;p = 2.7E-4)、IV(β = 0.430,SE = 0.073;p = 4.2E-9)和 V(β = 0.233,SE = 0.050;p = 2.7E-6)均与较高的 eGFR 相关。在自我认同的英国生物库白人参与者中,mtDNA单倍型与eGFR有关,但与ESKD、AKI或白蛋白尿无关。
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来源期刊
Human Genetics
Human Genetics 生物-遗传学
CiteScore
10.80
自引率
3.80%
发文量
94
审稿时长
1 months
期刊介绍: Human Genetics is a monthly journal publishing original and timely articles on all aspects of human genetics. The Journal particularly welcomes articles in the areas of Behavioral genetics, Bioinformatics, Cancer genetics and genomics, Cytogenetics, Developmental genetics, Disease association studies, Dysmorphology, ELSI (ethical, legal and social issues), Evolutionary genetics, Gene expression, Gene structure and organization, Genetics of complex diseases and epistatic interactions, Genetic epidemiology, Genome biology, Genome structure and organization, Genotype-phenotype relationships, Human Genomics, Immunogenetics and genomics, Linkage analysis and genetic mapping, Methods in Statistical Genetics, Molecular diagnostics, Mutation detection and analysis, Neurogenetics, Physical mapping and Population Genetics. Articles reporting animal models relevant to human biology or disease are also welcome. Preference will be given to those articles which address clinically relevant questions or which provide new insights into human biology. Unless reporting entirely novel and unusual aspects of a topic, clinical case reports, cytogenetic case reports, papers on descriptive population genetics, articles dealing with the frequency of polymorphisms or additional mutations within genes in which numerous lesions have already been described, and papers that report meta-analyses of previously published datasets will normally not be accepted. The Journal typically will not consider for publication manuscripts that report merely the isolation, map position, structure, and tissue expression profile of a gene of unknown function unless the gene is of particular interest or is a candidate gene involved in a human trait or disorder.
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