全外显子组测序鉴定出与心律失常性心肌病相关的 TJP1 基因的致病性变异。

Whole-Exome Sequencing Identifies Pathogenic Variants in TJP1 Gene Associated With Arrhythmogenic Cardiomyopathy.

机构信息

Departments of Biology (M.D.B., G.P., M.C., A.L., G.V., A.R.).

Department of Medical Biology and Department of Clinical Genetics, Academic Medical Center, Amsterdam, The Netherlands (A.V.P.).

出版信息

Circ Genom Precis Med. 2018 Oct;11(10):e002123. doi: 10.1161/CIRCGEN.118.002123.

DOI:10.1161/CIRCGEN.118.002123

PMID:30354300

Abstract

BACKGROUND

Arrhythmogenic cardiomyopathy (ACM) is an inherited cardiac disease characterized by progressive fibro-fatty myocardial replacement, ventricular arrhythmia, heart failure, and sudden death. Causative mutations can be identified in 60% of patients, and most of them are found in genes encoding mechanical junction proteins of the intercalated disk.

METHODS

Whole-exome sequencing was performed on the proband of an ACM family. Sanger sequencing was used to screen for mutations the tight junction protein 1 ( TJP1) gene in unrelated patients. Predictions of local structure content and molecular dynamics simulations were performed to investigate the structural impact of the variants.

RESULTS

A novel c.2006A>G p.(Y669C) variant in TJP1 gene was identified by whole-exome sequencing in a patient with ACM. TJP1 encodes zonula occludens 1, an intercalated disk protein interacting with proteins of gap junctions and area composita. Additional rare TJP1 variants have been identified in 1 of 40 Italian probands (c.793C>T p.(R265W)) with arrhythmogenic right ventricular cardiomyopathy and in 2 of 43 Dutch/German patients (c. 986C>T, p.(S329L) and c.1079A>T, p.(D360V)) with dilated cardiomyopathy and recurrent ventricular tachycardia. The p.(D360V) variant was identified in a proband also carrying the p.(I156N) pathogenic variant in DSP. All 4 TJP1 variants are predicted to be deleterious and affect highly conserved amino acids, either at the GUK (guanylate kinase)-like domain (p.(Y669C)) or at the disordered region of the protein between the PDZ2 and PDZ3 domains (p.(R265W), p.(S329L), and p.(D360V)). The local unfolding induced by the former promotes structural rearrangements of the GUK domain, whereas the others are predicted to impair the function of the disordered region. Furthermore, rare variants in TJP1 are statistically enriched in patients with ACM relative to controls.

CONCLUSIONS

We provide here the first evidence linking likely pathogenic TJP1 variants to ACM. Prevalence and pathogenic mechanism of TJP1-mediated ACM remain to be determined.

摘要

背景

致心律失常性右室心肌病（ARVC）是一种遗传性心脏病，其特征为进行性纤维脂肪心肌替代、室性心律失常、心力衰竭和心源性猝死。在 60%的患者中可以发现致病突变，其中大多数位于闰盘机械连接蛋白的编码基因中。

方法

对一个 ARVC 家系的先证者进行全外显子组测序。对无关患者的紧密连接蛋白 1（TJP1）基因进行 Sanger 测序以筛选突变。对局部结构含量和分子动力学模拟进行预测，以研究变体的结构影响。

结果

通过全外显子组测序在一个 ARVC 患者中鉴定出 TJP1 基因的新型 c.2006A>G p.(Y669C) 变体。TJP1 编码连接蛋白 1，这是一种与缝隙连接和区域复合蛋白相互作用的闰盘蛋白。在意大利的 40 个先证者（c.793C>T p.(R265W)）中，有 1 个先证者被诊断为致心律失常性右室心肌病，在荷兰/德国的 43 个患者中（c.986C>T，p.(S329L)和 c.1079A>T，p.(D360V)）有 2 个患者患有扩张型心肌病和复发性室性心动过速，均发现了 TJP1 罕见变异。c.1079A>T p.(D360V) 变异在一个先证者中被发现，该先证者还携带 DSP 中的致病性 p.(I156N) 变异。所有 4 种 TJP1 变异均被预测为有害，并影响高度保守的氨基酸，一种位于 GUK（鸟苷酸激酶）样结构域（p.(Y669C)），另一种位于 PDZ2 和 PDZ3 结构域之间的无规卷曲区的蛋白（p.(R265W)，p.(S329L)和 p.(D360V)）。前者诱导的局部展开促进了 GUK 结构域的结构重排，而其他则可能会损害无规卷曲区的功能。此外，在 ARVC 患者中，TJP1 的罕见变异在统计学上比对照组更为丰富。