Familial juvenile hyperuricemic nephropathy: Revisiting the SLC8A1 gene, in a family with a novel terminal gross deletion in the UMOD gene

IF 2 4区 医学 Q2 UROLOGY & NEPHROLOGY Nefrologia Pub Date : 2024-07-01 DOI:10.1016/j.nefro.2023.09.007
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Abstract

Autosomal dominant tubulointerstitial kidney disease (ADTKD) comprises a heterogeneous group of rare hereditary kidney diseases characterized by family history of progressive chronic kidney disease (CKD) with bland urine sediment, absence of significant proteinuria and normal or small-sized kidneys. Current diagnostic criteria require identification of a pathogenic variant in one of five genes – UMOD, MUC1, REN, HNF1β, SEC61A1. The most prevalent form of ADTKD is uromodulin-associated kidney disease (ADTKD-UMOD).

Genetic study of a Portuguese family diagnosed with familial juvenile hyperuricemic nephropathy (FJHN), one of the nosological entities in the spectrum of ADTKD, revealed a previously unreported large deletion in UMOD encompassing the entire terminal exon, which strictly cosegregated with CKD and hyperuricemia/gout, establishing the primary diagnosis of ADTKD-UMOD; as well as an ultra-rare nonsense SLC8A1 variant cosegregating with the UMOD deletion in patients that consistently exhibited an earlier onset of clinical manifestations.

Since the terminal exon of UMOD does not encode for any of the critical structural domains or amino acid residues of mature uromodulin, the molecular mechanisms underlying the pathogenicity of its deletion are unclear and require further research.

The association of the SLC8A1 locus with FJHN was first indicated by the results of a genome-wide linkage analysis in several multiplex families, but those data have not been subsequently confirmed. Our findings in this family revive that hypothesis.

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家族性幼年高尿酸血症肾病:在一个 UMOD 基因末端总缺失的家族中重新审视 SLC8A1 基因
常染色体显性肾小管间质性肾病(ADTKD)是一组异质性的罕见遗传性肾病,其特点是家族史中存在进行性慢性肾病(CKD),尿沉渣平淡,无明显蛋白尿,肾脏大小正常或较小。目前的诊断标准要求鉴定出 UMOD、MUC1、REN、HNF1β 和 SEC61A1 五个基因中的一个致病变体。最常见的 ADTKD 是尿调节蛋白相关性肾病(ADTKD-UMOD)。对一个被诊断为家族性幼年高尿酸血症肾病(FJHN)(ADTKD 病谱中的一个命名实体)的葡萄牙家族进行的遗传学研究发现,UMOD 中有一个以前未报道过的大缺失,包括整个末端外显子,该缺失与慢性肾脏病和高尿酸血症/痛风密切相关,从而确定了 ADTKD-UMOD 的初步诊断;还有一种超罕见的无义 SLC8A1 变异与 UMOD 缺失共存,患者的临床表现始终较早出现。由于 UMOD 的末端外显子不编码成熟尿调节蛋白的任何关键结构域或氨基酸残基,其缺失致病的分子机制尚不清楚,需要进一步研究。我们在这个家族中的研究结果重新提出了这一假设。
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来源期刊
Nefrologia
Nefrologia 医学-泌尿学与肾脏学
CiteScore
3.40
自引率
7.70%
发文量
148
审稿时长
47 days
期刊介绍: Nefrología is the official publication of the Spanish Society of Nephrology. The Journal publishes articles on basic or clinical research relating to nephrology, arterial hypertension, dialysis and kidney transplants. It is governed by the peer review system and all original papers are subject to internal assessment and external reviews. The journal accepts submissions of articles in English and in Spanish languages.
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