A novel nonsense mutation in the β-subunit of the epithelial sodium channel causing Liddle syndrome.

IF 1.8 4区医学

Blood Pressure Pub Date : 2021-10-01 Epub Date: 2021-07-05 DOI:10.1080/08037051.2021.1942785

Štěpán Mareš, Jan Filipovský, Kateřina Vlková, Martin Pešta, Václava Černá, Jaroslav Hrabák, Jitka Mlíková Seidlerová, Otto Mayer

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引用次数: 4

Abstract

Purpose: Liddle syndrome is a hereditary form of arterial hypertension caused by mutations in the genes coding of the epithelial sodium channel - SCNN1A, SCNN1B and SCNN1G. It is characterised by early onset of hypertension and variable biochemical features such as hypokalaemia and low plasma concentrations of renin and aldosterone. Phenotypic variability is large and, therefore, LS is probably underdiagnosed. Our objective was to examine a family suspected from Liddle syndrome including genetic testing and evaluate clinical and biochemical features of affected family members.

Materials and methods: Thirteen probands from the Czech family, related by blood, underwent physical examination, laboratory tests, and genetic testing. Alleles of SCNN1B and SCNN1G genes were examined by PCR amplification and Sanger sequencing of amplicons.

Results: We identified a novel mutation in the β-subunit of an epithelial sodium channel coded by the SCNN1B gene, causing the nonsense mutation in the protein sequence p.Tyr604*. This mutation was detected in 7 members of the family. The mutation carriers differed in the severity of hypertension and hypokalaemia which appeared only after diuretics in most of them; low aldosterone level (< 0.12 nmol/l) was, however, present in all.

Conclusions: This finding expands the spectrum of known mutations causing Liddle syndrome. Hypoaldosteronemia was 100% sensitive sign in the mutation carriers. Low levels are observed especially in the Caucasian population reaching 96% sensitivity. Assessment of plasma aldosterone concentration is helpful for differential diagnosis of arterial hypertension.

Condensed abstract: Liddle syndrome is a hereditary form of arterial hypertension caused by mutations in the genes encoding the epithelial sodium channel's α-, β- and γ-subunit. It is usually manifested by early onset of hypertension accompanied by low potassium and aldosterone levels. We performed a physical examination, laboratory tests and genetic screening in 13 members of a Czech family. We found a new mutation of the SCNN1B gene which encodes the β-subunit of the epithelial sodium channel. We describe the variability of each family member phenotype and point out the relevance of using aldosterone levels as a high sensitivity marker of Liddle syndrome in Caucasians.

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上皮钠通道β亚基的一种新的无义突变导致Liddle综合征。

目的:Liddle综合征是一种由上皮钠通道SCNN1A、SCNN1B和SCNN1G编码基因突变引起的遗传性动脉高血压。它的特点是早发性高血压和可变的生化特征，如低钾血症和低血浆肾素和醛固酮浓度。表型变异性很大，因此，LS可能未被充分诊断。我们的目的是检查一个疑似Liddle综合征的家庭，包括基因检测和评估患病家庭成员的临床和生化特征。材料和方法:来自捷克家族的13名先证者进行了身体检查、实验室检测和基因检测。采用PCR扩增和Sanger测序方法检测SCNN1B和SCNN1G基因的等位基因。结果:我们在SCNN1B基因编码的上皮钠通道β-亚基中发现了一个新的突变，导致蛋白序列p.t tyr604 *发生无义突变。该突变在该家族的7名成员中检测到。突变携带者在高血压和低钾血症的严重程度上存在差异，大多数突变携带者在利尿剂后才出现低钾血症;醛固酮水平低(< 0.12 nmol/l)。结论:这一发现扩大了已知突变引起Liddle综合征的范围。低醛固酮血症在突变携带者中为100%敏感征候。特别是在高加索人群中观察到低水平，灵敏度达到96%。血浆醛固酮浓度的测定有助于动脉性高血压的鉴别诊断。摘要:Liddle综合征是一种由上皮钠通道α-、β-和γ-亚基编码基因突变引起的遗传性动脉高血压。它通常表现为早发性高血压并伴有低钾和醛固酮水平。我们对一个捷克家庭的13名成员进行了身体检查、实验室测试和基因筛查。我们发现了一个新的SCNN1B基因突变，该基因编码上皮钠通道的β亚基。我们描述了每个家庭成员表型的可变性，并指出使用醛固酮水平作为白种人Liddle综合征的高灵敏度标志物的相关性。

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

Blood Pressure Medicine-Cardiology and Cardiovascular Medicine

CiteScore

3.20

自引率

5.60%

发文量

期刊介绍： For outstanding coverage of the latest advances in hypertension research, turn to Blood Pressure, a primary source for authoritative and timely information on all aspects of hypertension research and management. Features include: • Physiology and pathophysiology of blood pressure regulation • Primary and secondary hypertension • Cerebrovascular and cardiovascular complications of hypertension • Detection, treatment and follow-up of hypertension • Non pharmacological and pharmacological management • Large outcome trials in hypertension.