Mutation analysis of  KCNJ1  gene and investigation of phenotype in 5 Chinese patients with Bartter syndrome type 2

Han Yue; Lang Yanhua; Xiao Shujiao; Shi Xiaomeng; Wang Sai; Zhang Ruixiao; Guo Wencong; Zhao Xiangzhong; Shao Leping

doi:10.3760/cma.j.issn.1001-7097.2020.02.008

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• 临床研究 •

中国5例2型巴特综合征KCNJ1基因变异分析和临床表型研究

中华肾脏病杂志, 2020,36(02) : 115-122. DOI: 10.3760/cma.j.issn.1001-7097.2020.02.008

摘要

目的

检测和分析中国2型巴特综合征（Bartter syndrome type 2，BS2）患者的KCNJ1基因变异，观察患者临床表型和药物治疗疗效。

方法

收集2012年6月至2019年1月经青岛市立医院确诊的5例BS2患者及其亲属临床资料和血标本。采用第2代高通量测序法行全外显子基因测序确定基因变异。根据2015年美国医学遗传学和基因组学学会（ACMG）分类标准和指南评估变异基因的致病性。回顾性分析患者临床表现和实验室检查结果，随访观察患者药物治疗疗效和病情转归。

结果

全外显子测序和Sanger测序验证共确定KCNJ1基因10个变异，其中6个为新发现变异，变异类型多为错义变异。5例患者常见的临床表现依次为：多饮多尿（5/5），其中1例尿崩；母体羊水增多和患儿早产（4/5）；生长迟缓（3/5）。2例患者初诊表现为低氯性代谢碱中毒合并低血钾（2/5），其余患者均无明显酸碱失衡，1例合并高血钾。1例患者存在明显的甲状旁腺素（PTH）抵抗[低血钙、高血磷和血全段PTH（iPTH）水平升高]；3例患者存在明显的PTH反应过度（高血钙、低血磷和血iPTH水平轻度升高）；1例患者血iPTH水平为正常值上限，血钙和血磷水平正常。5例患者均存在高尿钙或肾钙质沉积，其中1例患儿伴有肾结石。吲哚美辛对改善患者的多饮多尿、生长迟缓、电解质紊乱、高尿钙和血iPTH升高有明显疗效。

结论

共发现KCNJ1基因10个变异，其中6个为新变异，丰富了人类基因突变库。BS2患者临床表型表现多样，应注意与其他甲状旁腺疾病鉴别。

引用本文: 韩玥, 郎艳华, 肖淑佼, 等. 中国5例2型巴特综合征KCNJ1基因变异分析和临床表型研究 [J] . 中华肾脏病杂志,2020,36 (02): 115-122. DOI: 10.3760/cma.j.issn.1001-7097.2020.02.008

参考文献导出: Endnote NoteExpress RefWorks NoteFirst 医学文献王

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巴特综合征（Bartter syndrome，BS）是一种罕见的遗传性肾小管疾病，表现为水盐重吸收障碍导致的失盐性肾病。BS表型特征为低血钾、代谢性碱中毒、继发性醛固酮增多症和血压正常或偏低^[1]。我们收集了来自中国5个家系的5例2型BS（BS2）先证者及其亲属资料，采用第2代高通量测序法检测和分析全部外显子的基因变异，观察患者临床表型改变及药物治疗效果。

贡献者信息

韩玥

青岛市立医院肾内科，青岛　266071

郎艳华

青岛大学附属医院护理部，青岛　266003

肖淑佼

青岛大学附属医院护理部，青岛　266003

石晓梦

青岛市立医院肾内科，青岛　266071

望赛

青岛市立医院肾内科，青岛　266071

张瑞晓

青岛市立医院肾内科，青岛　266071

郭文聪

青岛市立医院肾内科，青岛　266071

赵向忠

青岛大学附属医院中心实验室，青岛　266071

邵乐平

青岛市立医院肾内科，青岛　266071

通信作者

邵乐平

青岛市立医院肾内科，青岛　266071

Email：lepingshao@163.com

关键词

巴特综合征; 基因型; 表型; KCNJ1基因;

基金项目

国家自然科学基金面上项目（81873594）

利益冲突

利益冲突　所有作者均声明不存在利益冲突

历史

出版日期：2020-02-15

收稿日期：2019-09-11

本文编辑

孙玉玲

Clinical Study

Mutation analysis of KCNJ1 gene and investigation of phenotype in 5 Chinese patients with Bartter syndrome type 2

Han Yue, Lang Yanhua, Xiao Shujiao, Shi Xiaomeng, Wang Sai, Zhang Ruixiao, Guo Wencong, Zhao Xiangzhong, Shao Leping

Published 2020-02-15

Cite as Chin J Nephrol, 2020,36(02): 115-122. DOI: 10.3760/cma.j.issn.1001-7097.2020.02.008

Abstract

Objective

To identify and analyze the variants of the KCNJ1 gene in five Chinese patients with Bartter syndrome type 2 (BS2), and to describe their clinical features as well as treatment results.

Methods

Data and blood samples of five BS2 patients and their relatives confirmed by Qingdao Municipal Hospital from June 2012 to January 2019 were collected. Whole-exome-sequencing (WES) based on the second generation high throughput sequencing was performed to detect variants. The 2015 American College of Medical Genetics and Genomics Standards and Guidelines were applied to analyze the pathogenicity of the variants. The clinical features and laboratory results were retrospectively studied. The response to treatment and follow-up data were reviewed.

Results

Ten variants including six novel ones of KCNJ1 gene were identified through WES and verified by Sanger dideoxy sequencing. Missense variants accounted for the highest proportion. The common symptoms and signs of five BS2 patients from high to low incidence were polydipsia and polyuria (5/5), one of them (1/5) presented with diabetes insipidus; maternal polyhydramnios and premature delivery (4/5); growth retardation (3/5). Initially, two patients presented with hypochloremic metabolic alkalosis and hypokalemia, whereas the acid-base disturbance was absent in the others. One patient experienced hyperkalemia. In terms of calcium-phosphorus metabolism, one patient had evident parathyroid hormone (PTH) resistance (hypocalcemia, hyperphosphatemia and markedly elevated serum intact PTH levels), three presented with PTH overacting (hypercalcemia, hypophosphatemia and mild elevated serum intact PTH levels), and one showed normal blood calcium and phosphorus concentrations with high-normal serum intact PTH levels. All patients had nephrocalcinosis or hypercalciuria, and one of them complicated with nephrolithiasis. Indomethacin helped to correct the growth retardation, halt polydipsia polyuria, decrease the elevated urinary calcium excretion, and normalize electrolyte disturbance as well as PTH parameters in some patients.

Conclusions

This investigation identifies ten variants of KCNJ1 gene, including six ones that have not been previously reported, which will enrich the human gene mutation database (HGMD). These patients in our study have atypical BS phenotype, so that careful differentiation from other parathyroid diseases will be required for clinicians.

Key words:

Bartter syndrome; Genotype; Phenotype; KCNJ1 gene

Contributor Information

Han Yue