估计导致遗传性类固醇抵抗性肾病综合征的卡舒比特异性致病基因 NPHS2 变体的年龄表明它最近才起源于当地

IF 3.3 2区 医学 Q2 GENETICS & HEREDITY
M. Jankowski, P. Daca-Roszak, I. Bałasz-Chmielewska, A. Ustaszewski, A. Żurowska, B. S. Lipska-Ziętkiewicz, E. Ziętkiewicz
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引用次数: 0

摘要

类固醇耐受性肾病综合征(SRNS)是一种高度异质性的肾脏疾病,是由于基因异常或免疫系统功能障碍影响了肾小球滤过屏障的建立和维持。遗传性 SRNS 最常见的病因是 NPHS2 基因的双倍性致病变异,尤其是在婴儿或儿童期发病的患者中。NPHS2 缺陷的类型影响着疾病的进程和发病阶段,而且在不同人群中存在差异。在波兰 SRNS 患者队列中,来自波兰北部卡舒布人(Kashubs)居住区的患者发现了与疾病相关的 NPHS2 变异的独特特征。在卡舒布族家庭中,c.686G>A/c.1032delT复合杂合子和单一c.1032delT同源杂合子是SRNS的唯一潜在病因。c.1032delT 仅在卡舒比亚人中出现的局限性模式表明存在始祖效应,这促使我们对其单倍型背景进行详细分析,以估计 c.1032delT 的起源年龄。我们使用 Infinium Global Screening Array-24 对八个卡舒比 SRNS 家族进行了基因分型。单倍型背景分析是使用内部设计的管道进行的,旨在解决杂合基因型数据的阶段性问题。c.1032delT 突变的年龄是根据两个或两个以上携带该变异的个体共享的祖先单倍型的遗传长度,用伽马法计算得出的。我们的研究结果表明,c.1032delT 突变的起源很近(约 240 年)。在波兰普通人群中进行的基因筛查证实了这一假设,即该变异发生在特定的卡舒比单倍型背景上。确定卡舒比亚祖先特异性致病变体有助于制定有效的筛查和诊断策略,作为该地区个性化医疗方法的一部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Estimation of the Age of the Kashubian-Specific Pathogenic NPHS2 Variant Responsible for Hereditary Steroid-Resistant Nephrotic Syndrome Points to Its Recent Local Origin

Steroid-resistant nephrotic syndrome (SRNS) is a highly heterogenic kidney disorder resulting from genetic abnormalities or immune system dysfunction affecting the establishment and maintenance of the glomerular filtration barrier. The most common cause of genetic SRNS is biallelic pathogenic variants in NPHS2 gene, especially in individuals with an infantile or childhood onset. The type of the NPHS2 defect implies the course of the disease and the stage of its onset and differs across populations. In a cohort of Polish patients with SRNS, a unique profile of the disease-related NPHS2 variants was identified in patients from northern Poland inhabited by Kashubs, a minority West-Slavic ethnic group known for a local increase of the frequency of several pathogenic variants. Among Kashubian families, the compound heterozygotes c.686G>A/c.1032delT and a single c.1032delT homozygote were the only underlying cause of SRNS. The restricted, Kashubian-only pattern of c.1032delT occurrence, suggesting the founder effect, prompted us to conduct a detailed analysis of its haplotype background to estimate the age of the c.1032delT origin. Eight Kashubian SRNS families were genotyped using the Infinium Global Screening Array-24. The haplotype background analysis was performed using an in-house pipeline designed to solve the phase of the heterozygous genotype data. The age of the c.1032delT mutation was calculated using the gamma method based on the genetic length of ancestral haplotypes shared between two or more individuals carrying this variant. The results of our study indicated a very recent origin of the c.1032delT mutation (~240 years). Genetic screening performed in the general Polish population control corroborates the assumption that the mutation occurred on the specific Kashubian haplotype background. The identification of ancestry-specific Kashubian pathogenic variant can help to develop effective screening and diagnostic strategies as a part of personalized medicine approach in the region.

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来源期刊
Human Mutation
Human Mutation 医学-遗传学
CiteScore
8.40
自引率
5.10%
发文量
190
审稿时长
2 months
期刊介绍: Human Mutation is a peer-reviewed journal that offers publication of original Research Articles, Methods, Mutation Updates, Reviews, Database Articles, Rapid Communications, and Letters on broad aspects of mutation research in humans. Reports of novel DNA variations and their phenotypic consequences, reports of SNPs demonstrated as valuable for genomic analysis, descriptions of new molecular detection methods, and novel approaches to clinical diagnosis are welcomed. Novel reports of gene organization at the genomic level, reported in the context of mutation investigation, may be considered. The journal provides a unique forum for the exchange of ideas, methods, and applications of interest to molecular, human, and medical geneticists in academic, industrial, and clinical research settings worldwide.
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