Rare heterozygous variants in paediatric steroid resistant nephrotic syndrome - a population-based analysis of their significance.

IF 3.9 2区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES

Scientific Reports Pub Date : 2024-08-10 DOI:10.1038/s41598-024-68837-2

C J Platt, A Bierzynska, W Ding, S A Saleem, A Koziell, M A Saleem

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Abstract

Genetic testing in nephrotic syndrome may identify heterozygous predicted-pathogenic variants (HPPVs) in autosomal recessive (AR) genes that are known to cause disease in the homozygous or compound heterozygous state. In such cases, it can be difficult to define the variant's true significance and questions remain about whether a second pathogenic variant has been missed during analysis or whether the variant is an incidental finding. There are now known to be over 70 genes associated with nephrotic syndrome, the majority inherited as an AR trait. Knowledge of whether such HPPVs occur with equal frequency in patients compared to the general population would assist interpretation of their significance. Exome sequencing was performed on 187 Steroid-Resistant Nephrotic Syndrome (SRNS) paediatric patients recruited to a UK rare disease registry plus originating from clinics at Evelina, London. 59 AR podocytopathy linked genes were analysed in each patient and a list of HPPVs created. We compared the frequency of detected HPPVs with a 'control' population from the gnomAD database containing exome data from approximately 50,000 individuals. A bespoke filtering process was used for both patients and controls to predict 'likely pathogenicity' of variants. In total 130 Caucasian SRNS patients were screened across 59 AR genes and 201 rare heterozygous variants were identified. 17/201 (8.5%) were assigned as 'likely pathogenic' (HPPV) using our bespoke filtering method. Comparing each gene in turn, for SRNS patients with a confirmed genetic diagnosis, in 57 of the 59 genes we found no statistically significant difference in the frequency of these HPPVs between patients and controls (In genes ARHGDIA and TP53RK, we identified a significantly higher number of HPPVs in the control population compared with the patients when filtering was performed with 'high stringency' settings only). In the SRNS patients without a genetics diagnosis confirmed, there was no statistically significant difference identified in any gene between patient and control. In children with SRNS, we propose that identification of HPPV in AR podocytopathy linked genes is not necessarily representative of pathogenicity, given that the frequency is similar to that seen in controls for the majority. Whilst this may not exclude the presence of genetic kidney disease, this type of heterozygous variant is unlikely to be causal and each result must be interpreted in its clinical context.

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儿科类固醇耐药肾病综合征中的罕见杂合变异--基于人群的意义分析。

肾病综合征的基因检测可能会发现常染色体隐性（AR）基因中的杂合子预测致病变体（HPPV），已知这些变体在同合子或复合杂合子状态下会导致疾病。在这种情况下，很难确定变异体的真正意义，而且在分析过程中是否遗漏了第二个致病变异体或该变异体是否是偶然发现的问题依然存在。目前已知与肾病综合征相关的基因有 70 多个，其中大部分是作为 AR 性状遗传的。了解此类 HPPV 在患者中的发生频率是否与普通人群相同，将有助于解释其意义。我们对英国罕见病登记处招募的 187 名类固醇耐受性肾病综合征（SRNS）儿科患者进行了外显子组测序，这些患者来自伦敦埃维利纳诊所。我们对每位患者的 59 个与 AR 足细胞病相关的基因进行了分析，并创建了一份 HPPV 列表。我们将检测到的 HPPV 频率与 gnomAD 数据库中的 "对照 "人群进行了比较，gnomAD 数据库中包含约 50,000 人的外显子组数据。我们对患者和对照组都采用了定制的过滤程序，以预测变异的 "可能致病性"。总共对 130 名高加索 SRNS 患者的 59 个 AR 基因进行了筛查，发现了 201 个罕见杂合变异体。使用我们定制的筛选方法，17/201（8.5%）被定为 "可能致病"（HPPV）。在 59 个基因中的 57 个基因中，我们发现患者和对照组之间的 HPPV 频率没有显著的统计学差异（在 ARHGDIA 和 TP53RK 基因中，当仅使用 "高严格 "设置进行筛选时，我们在对照组人群中发现的 HPPV 数量明显高于患者）。在未确诊遗传学诊断的 SRNS 患者中，发现患者与对照组在任何基因上都没有统计学意义上的显著差异。在 SRNS 儿童中，我们认为，在与 AR podocytopathy 相关的基因中发现 HPPV 不一定代表致病性，因为大多数基因的频率与对照组相似。虽然这不能排除遗传性肾病的存在，但这类杂合变异不太可能是致病因素，因此必须根据临床情况来解释每个结果。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Scientific Reports Natural Science Disciplines-

CiteScore

7.50

自引率

4.30%

发文量

19567

审稿时长

3.9 months

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