RRAD mutation causes electrical and cytoskeletal defects in cardiomyocytes derived from a familial case of Brugada syndrome

被引:37
作者
Belbachir, Nadjet [1 ,2 ]
Portero, Vincent [1 ]
Al Sayed, Zeina R. [1 ]
Gourraud, Jean-Baptiste [1 ,3 ]
Dilasser, Florian [1 ]
Jesel, Laurence [4 ]
Guo, Hongchao [2 ]
Wu, Haodi [2 ]
Gaborit, Nathalie [1 ]
Guilluy, Christophe [5 ]
Girardeau, Aurore [1 ]
Bonnaud, Stephanie [1 ,3 ]
Simonet, Floriane [1 ,3 ]
Karakachoff, Matilde [1 ,3 ]
Pattier, Sabine [3 ]
Scott, Carol [6 ]
Burel, Sophie [1 ]
Marionneau, Celine [1 ]
Chariau, Caroline [7 ]
Gaignerie, Anne [7 ]
David, Laurent [7 ,8 ]
Genin, Emmanuelle [9 ]
Deleuze, Jean-Francois [10 ]
Dina, Christian [1 ,3 ]
Sauzeau, Vincent [1 ]
Loirand, Gervaise [1 ]
Baro, Isabelle [1 ]
Schott, Jean-Jacques [1 ,3 ]
Probst, Vincent [1 ,3 ]
Wu, Joseph C. [2 ]
Redon, Richard [1 ,3 ]
Charpentier, Flavien [1 ,3 ]
Le Scouarnec, Solena [1 ]
机构
[1] Univ Nantes, Inst Thorax, INSERM, CNRS, 8 Quai Moncousu, F-44007 Nantes 1, France
[2] Stanford Univ, Sch Med, Div Cardiovasc Med, Dept Med,Stanford Cardiovasc Inst,Inst Stem Cell, Stanford, CA USA
[3] CHU Nantes, Inst Thorax, Nantes, France
[4] CHU Strasbourg, Serv Cardiol, Strasbourg, France
[5] CNRS, Inst Adv Biosci, INSERM, Grenoble, France
[6] Wellcome Trust Sanger Inst, Cambridge, England
[7] Univ Nantes, CHU Nantes, SFR Francois Bonamy, INSERM,CNRS,iPSC Core Facil, Nantes, France
[8] Univ Nantes, Ctr Rech Transplantat & Immunol UMR 1064, INSERM, ITUN,CHU Nantes, Nantes, France
[9] Univ Brest, CHRU Brest, Inserm UMR 1078, Brest, France
[10] CEA, Inst Genom, Ctr Natl Rech Genom Humaine, Evry, France
来源
EUROPEAN HEART JOURNAL | 2019年 / 40卷 / 37期
基金
美国国家卫生研究院;
关键词
Brugada syndrome; RAD GTPase; Induced pluripotent stem cells; Sodium current; L-type calcium current; Actin cytoskeleton; ST-SEGMENT ELEVATION; VENTRICULAR-ARRHYTHMIAS; SUSCEPTIBILITY GENE; RAD; MANAGEMENT; VARIANTS; CARDIOMYOPATHY; ABNORMALITIES; MUSCLE; HEY2;
D O I
10.1093/eurheartj/ehz308
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Aims The Brugada syndrome (BrS) is an inherited cardiac disorder predisposing to ventricular arrhythmias. Despite considerable efforts, its genetic basis and cellular mechanisms remain largely unknown. The objective of this study was to identify a new susceptibility gene for BrS through familial investigation. Methods and results Whole-exome sequencing performed in a three-generation pedigree with five affected members allowed the identification of one rare non-synonymous substitution (p.R211H) in RRAD, the gene encoding the RAD GTPase, carried by all affected members of the family. Three additional rare missense variants were found in 3/186 unrelated index cases. We detected higher levels of RRAD transcripts in subepicardium than in subendocardium in human heart, and in the right ventricle outflow tract compared to the other cardiac compartments in mice. The p.R211H variant was then subjected to electrophysiological and structural investigations in human cardiomyocytes derived from induced pluripotent stem cells (iPSC-CMs). Cardiomyocytes derived from induced pluripotent stem cells from two affected family members exhibited reduced action potential upstroke velocity, prolonged action potentials and increased incidence of early after depolarizations, with decreased Na+ peak current amplitude and increased Na+ persistent current amplitude, as well as abnormal distribution of actin and less focal adhesions, compared with intra-familial control iPSC-CMs Insertion of p.R211H-RRAD variant in control iPSCs by genome editing confirmed these results. In addition, iPSC-CMs from affected patients exhibited a decreased L-type Ca2+ current amplitude. Conclusion This study identified a potential new BrS-susceptibility gene, RRAD. Cardiomyocytes derived from induced pluripotent stem cells expressing RRAD variant recapitulated single-cell electrophysiological features of BrS, including altered Na+ current, as well as cytoskeleton disturbances.
引用
收藏
页码:3081 / +
页数:14
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