SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups

Alban Elouen Baruteau; Florence Kyndt; Elijah R. Behr; Arja S. Vink; Matthias Lachaud; Anna Gah-Mei Joong; Jean Jacques Schott; Minoru Horie; Isabelle Denjoy; Lia Crotti; Wataru Shimizu; Johan M. Bos; Elizabeth A. Stephenson; Leonie Wong; Dominic J. Abrams; Andrew M. Davis; Annika Winbo; Anne M. Dubin; Shubhayan Sanatani; Leonardo Liberman; Juan Pablo Kaski; Boris Rudic; Sit Yee Kwok; Claudine Rieubland; Jacob Tfelt-Hansen; George F. Van Hare; Béatrice Guyomarc'h-Delasalle; Nico A. Blom; Yanushi D. Wijeyeratne; Jean Baptiste Gourraud; Hervé Le Marec; Junichi Ozawa; Véronique Fressart; Jean Marc Lupoglazoff; Federica Dagradi; Carla Spazzolini; Takeshi Aiba; David J. Tester; Laura A. Zahavich; Virginie Beauséjour-Ladouceur; Mangesh Jadhav; Jonathan R. Skinner; Sonia Franciosi; Andrew D. Krahn; Mena Abdelsayed; Peter C. Ruben; Tak Cheung Yung; Michael J. Ackerman; Arthur A. Wilde; Peter J. Schwartz; Vincent Probst

doi:10.1093/eurheartj/ehy412

SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups

Alban Elouen Baruteau^*, Florence Kyndt, Elijah R. Behr, Arja S. Vink, Matthias Lachaud, Anna Gah-Mei Joong, Jean Jacques Schott, Minoru Horie, Isabelle Denjoy, Lia Crotti, Wataru Shimizu, Johan M. Bos, Elizabeth A. Stephenson, Leonie Wong, Dominic J. Abrams, Andrew M. Davis, Annika Winbo, Anne M. Dubin, Shubhayan Sanatani, Leonardo LibermanJuan Pablo Kaski, Boris Rudic, Sit Yee Kwok, Claudine Rieubland, Jacob Tfelt-Hansen, George F. Van Hare, Béatrice Guyomarc'h-Delasalle, Nico A. Blom, Yanushi D. Wijeyeratne, Jean Baptiste Gourraud, Hervé Le Marec, Junichi Ozawa, Véronique Fressart, Jean Marc Lupoglazoff, Federica Dagradi, Carla Spazzolini, Takeshi Aiba, David J. Tester, Laura A. Zahavich, Virginie Beauséjour-Ladouceur, Mangesh Jadhav, Jonathan R. Skinner, Sonia Franciosi, Andrew D. Krahn, Mena Abdelsayed, Peter C. Ruben, Tak Cheung Yung, Michael J. Ackerman, Arthur A. Wilde, Peter J. Schwartz, Vincent Probst

^*Corresponding author for this work

Pediatrics

Research output: Contribution to journal › Article › peer-review

29 Scopus citations

Abstract

Aims To clarify the clinical characteristics and outcomes of children with SCN5A-mediated disease and to improve their risk stratification. Methods and results A multicentre, international, retrospective cohort study was conducted in 25 tertiary hospitals in 13 countries between 1990 and 2015. All patients ≤16 years of age diagnosed with a genetically confirmed SCN5A mutation were included in the analysis. There was no restriction made based on their clinical diagnosis. A total of 442 children {55.7% boys, 40.3% probands, median age: 8.0 [interquartile range (IQR) 9.5] years} from 350 families were included; 67.9% were asymptomatic at diagnosis. Four main phenotypes were identified: isolated progressive cardiac conduction disorders (25.6%), overlap phenotype (15.6%), isolated long QT syndrome type 3 (10.6%), and isolated Brugada syndrome type 1 (1.8%); 44.3% had a negative electrocardiogram phenotype. During a median follow-up of 5.9 (IQR 5.9) years, 272 cardiac events (CEs) occurred in 139 (31.5%) patients. Patients whose mutation localized in the C-terminus had a lower risk. Compound genotype, both gain- and loss-of-function SCN5A mutation, age ≤1 year at diagnosis in probands and age ≤1 year at diagnosis in non-probands were independent predictors of CE. Conclusion In this large paediatric cohort of SCN5A mutation-positive subjects, cardiac conduction disorders were the most prevalent phenotype; CEs occurred in about one-third of genotype-positive children, and several independent risk factors were identified, including age ≤1 year at diagnosis, compound mutation, and mutation with both gain- and loss-of-function.

Original language	English (US)
Pages (from-to)	2879-2887
Number of pages	9
Journal	European Heart Journal
Volume	39
Issue number	31
DOIs	https://doi.org/10.1093/eurheartj/ehy412
State	Published - Aug 1 2018

Keywords

Brugada syndrome
Genotype-phenotype correlation
Long QT syndrome
Progressive cardiac conduction disorders
SCN5A
Sodium channelopathy

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine

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10.1093/eurheartj/ehy412

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Baruteau, A. E., Kyndt, F., Behr, E. R., Vink, A. S., Lachaud, M., Joong, A. G-M., Schott, J. J., Horie, M., Denjoy, I., Crotti, L., Shimizu, W., Bos, J. M., Stephenson, E. A., Wong, L., Abrams, D. J., Davis, A. M., Winbo, A., Dubin, A. M., Sanatani, S., ... Probst, V. (2018). SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups. European Heart Journal, 39(31), 2879-2887. https://doi.org/10.1093/eurheartj/ehy412

@article{c28062c0f5b64ea2a71f96fcb740b7f5,

title = "SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups",

abstract = "Aims To clarify the clinical characteristics and outcomes of children with SCN5A-mediated disease and to improve their risk stratification. Methods and results A multicentre, international, retrospective cohort study was conducted in 25 tertiary hospitals in 13 countries between 1990 and 2015. All patients ≤16 years of age diagnosed with a genetically confirmed SCN5A mutation were included in the analysis. There was no restriction made based on their clinical diagnosis. A total of 442 children {55.7% boys, 40.3% probands, median age: 8.0 [interquartile range (IQR) 9.5] years} from 350 families were included; 67.9% were asymptomatic at diagnosis. Four main phenotypes were identified: isolated progressive cardiac conduction disorders (25.6%), overlap phenotype (15.6%), isolated long QT syndrome type 3 (10.6%), and isolated Brugada syndrome type 1 (1.8%); 44.3% had a negative electrocardiogram phenotype. During a median follow-up of 5.9 (IQR 5.9) years, 272 cardiac events (CEs) occurred in 139 (31.5%) patients. Patients whose mutation localized in the C-terminus had a lower risk. Compound genotype, both gain- and loss-of-function SCN5A mutation, age ≤1 year at diagnosis in probands and age ≤1 year at diagnosis in non-probands were independent predictors of CE. Conclusion In this large paediatric cohort of SCN5A mutation-positive subjects, cardiac conduction disorders were the most prevalent phenotype; CEs occurred in about one-third of genotype-positive children, and several independent risk factors were identified, including age ≤1 year at diagnosis, compound mutation, and mutation with both gain- and loss-of-function.",

keywords = "Brugada syndrome, Genotype-phenotype correlation, Long QT syndrome, Progressive cardiac conduction disorders, SCN5A, Sodium channelopathy",

author = "Baruteau, {Alban Elouen} and Florence Kyndt and Behr, {Elijah R.} and Vink, {Arja S.} and Matthias Lachaud and Joong, {Anna Gah-Mei} and Schott, {Jean Jacques} and Minoru Horie and Isabelle Denjoy and Lia Crotti and Wataru Shimizu and Bos, {Johan M.} and Stephenson, {Elizabeth A.} and Leonie Wong and Abrams, {Dominic J.} and Davis, {Andrew M.} and Annika Winbo and Dubin, {Anne M.} and Shubhayan Sanatani and Leonardo Liberman and Kaski, {Juan Pablo} and Boris Rudic and Kwok, {Sit Yee} and Claudine Rieubland and Jacob Tfelt-Hansen and {Van Hare}, {George F.} and B{\'e}atrice Guyomarc'h-Delasalle and Blom, {Nico A.} and Wijeyeratne, {Yanushi D.} and Gourraud, {Jean Baptiste} and Marec, {Herv{\'e} Le} and Junichi Ozawa and V{\'e}ronique Fressart and Lupoglazoff, {Jean Marc} and Federica Dagradi and Carla Spazzolini and Takeshi Aiba and Tester, {David J.} and Zahavich, {Laura A.} and Virginie Beaus{\'e}jour-Ladouceur and Mangesh Jadhav and Skinner, {Jonathan R.} and Sonia Franciosi and Krahn, {Andrew D.} and Mena Abdelsayed and Ruben, {Peter C.} and Yung, {Tak Cheung} and Ackerman, {Michael J.} and Wilde, {Arthur A.} and Schwartz, {Peter J.} and Vincent Probst",

year = "2018",

month = aug,

day = "1",

doi = "10.1093/eurheartj/ehy412",

language = "English (US)",

volume = "39",

pages = "2879--2887",

journal = "European Heart Journal",

issn = "0195-668X",

publisher = "Oxford University Press",

number = "31",

}

Baruteau, AE, Kyndt, F, Behr, ER, Vink, AS, Lachaud, M, Joong, AG-M, Schott, JJ, Horie, M, Denjoy, I, Crotti, L, Shimizu, W, Bos, JM, Stephenson, EA, Wong, L, Abrams, DJ, Davis, AM, Winbo, A, Dubin, AM, Sanatani, S, Liberman, L, Kaski, JP, Rudic, B, Kwok, SY, Rieubland, C, Tfelt-Hansen, J, Van Hare, GF, Guyomarc'h-Delasalle, B, Blom, NA, Wijeyeratne, YD, Gourraud, JB, Marec, HL, Ozawa, J, Fressart, V, Lupoglazoff, JM, Dagradi, F, Spazzolini, C, Aiba, T, Tester, DJ, Zahavich, LA, Beauséjour-Ladouceur, V, Jadhav, M, Skinner, JR, Franciosi, S, Krahn, AD, Abdelsayed, M, Ruben, PC, Yung, TC, Ackerman, MJ, Wilde, AA, Schwartz, PJ & Probst, V 2018, 'SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups', European Heart Journal, vol. 39, no. 31, pp. 2879-2887. https://doi.org/10.1093/eurheartj/ehy412

TY - JOUR

T1 - SCN5A mutations in 442 neonates and children

T2 - Genotype-phenotype correlation and identification of higher-risk subgroups

AU - Baruteau, Alban Elouen

AU - Kyndt, Florence

AU - Behr, Elijah R.

AU - Vink, Arja S.

AU - Lachaud, Matthias

AU - Joong, Anna Gah-Mei

AU - Schott, Jean Jacques

AU - Horie, Minoru

AU - Denjoy, Isabelle

AU - Crotti, Lia

AU - Shimizu, Wataru

AU - Bos, Johan M.

AU - Stephenson, Elizabeth A.

AU - Wong, Leonie

AU - Abrams, Dominic J.

AU - Davis, Andrew M.

AU - Winbo, Annika

AU - Dubin, Anne M.

AU - Sanatani, Shubhayan

AU - Liberman, Leonardo

AU - Kaski, Juan Pablo

AU - Rudic, Boris

AU - Kwok, Sit Yee

AU - Rieubland, Claudine

AU - Tfelt-Hansen, Jacob

AU - Van Hare, George F.

AU - Guyomarc'h-Delasalle, Béatrice

AU - Blom, Nico A.

AU - Wijeyeratne, Yanushi D.

AU - Gourraud, Jean Baptiste

AU - Marec, Hervé Le

AU - Ozawa, Junichi

AU - Fressart, Véronique

AU - Lupoglazoff, Jean Marc

AU - Dagradi, Federica

AU - Spazzolini, Carla

AU - Aiba, Takeshi

AU - Tester, David J.

AU - Zahavich, Laura A.

AU - Beauséjour-Ladouceur, Virginie

AU - Jadhav, Mangesh

AU - Skinner, Jonathan R.

AU - Franciosi, Sonia

AU - Krahn, Andrew D.

AU - Abdelsayed, Mena

AU - Ruben, Peter C.

AU - Yung, Tak Cheung

AU - Ackerman, Michael J.

AU - Wilde, Arthur A.

AU - Schwartz, Peter J.

AU - Probst, Vincent

PY - 2018/8/1

Y1 - 2018/8/1

N2 - Aims To clarify the clinical characteristics and outcomes of children with SCN5A-mediated disease and to improve their risk stratification. Methods and results A multicentre, international, retrospective cohort study was conducted in 25 tertiary hospitals in 13 countries between 1990 and 2015. All patients ≤16 years of age diagnosed with a genetically confirmed SCN5A mutation were included in the analysis. There was no restriction made based on their clinical diagnosis. A total of 442 children {55.7% boys, 40.3% probands, median age: 8.0 [interquartile range (IQR) 9.5] years} from 350 families were included; 67.9% were asymptomatic at diagnosis. Four main phenotypes were identified: isolated progressive cardiac conduction disorders (25.6%), overlap phenotype (15.6%), isolated long QT syndrome type 3 (10.6%), and isolated Brugada syndrome type 1 (1.8%); 44.3% had a negative electrocardiogram phenotype. During a median follow-up of 5.9 (IQR 5.9) years, 272 cardiac events (CEs) occurred in 139 (31.5%) patients. Patients whose mutation localized in the C-terminus had a lower risk. Compound genotype, both gain- and loss-of-function SCN5A mutation, age ≤1 year at diagnosis in probands and age ≤1 year at diagnosis in non-probands were independent predictors of CE. Conclusion In this large paediatric cohort of SCN5A mutation-positive subjects, cardiac conduction disorders were the most prevalent phenotype; CEs occurred in about one-third of genotype-positive children, and several independent risk factors were identified, including age ≤1 year at diagnosis, compound mutation, and mutation with both gain- and loss-of-function.

AB - Aims To clarify the clinical characteristics and outcomes of children with SCN5A-mediated disease and to improve their risk stratification. Methods and results A multicentre, international, retrospective cohort study was conducted in 25 tertiary hospitals in 13 countries between 1990 and 2015. All patients ≤16 years of age diagnosed with a genetically confirmed SCN5A mutation were included in the analysis. There was no restriction made based on their clinical diagnosis. A total of 442 children {55.7% boys, 40.3% probands, median age: 8.0 [interquartile range (IQR) 9.5] years} from 350 families were included; 67.9% were asymptomatic at diagnosis. Four main phenotypes were identified: isolated progressive cardiac conduction disorders (25.6%), overlap phenotype (15.6%), isolated long QT syndrome type 3 (10.6%), and isolated Brugada syndrome type 1 (1.8%); 44.3% had a negative electrocardiogram phenotype. During a median follow-up of 5.9 (IQR 5.9) years, 272 cardiac events (CEs) occurred in 139 (31.5%) patients. Patients whose mutation localized in the C-terminus had a lower risk. Compound genotype, both gain- and loss-of-function SCN5A mutation, age ≤1 year at diagnosis in probands and age ≤1 year at diagnosis in non-probands were independent predictors of CE. Conclusion In this large paediatric cohort of SCN5A mutation-positive subjects, cardiac conduction disorders were the most prevalent phenotype; CEs occurred in about one-third of genotype-positive children, and several independent risk factors were identified, including age ≤1 year at diagnosis, compound mutation, and mutation with both gain- and loss-of-function.

KW - Brugada syndrome

KW - Genotype-phenotype correlation

KW - Long QT syndrome

KW - Progressive cardiac conduction disorders

KW - SCN5A

KW - Sodium channelopathy

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UR - http://www.scopus.com/inward/citedby.url?scp=85055420900&partnerID=8YFLogxK

U2 - 10.1093/eurheartj/ehy412

DO - 10.1093/eurheartj/ehy412

M3 - Article

C2 - 30059973

SN - 0195-668X

VL - 39

SP - 2879

EP - 2887

JO - European Heart Journal

JF - European Heart Journal

IS - 31

ER -

SCN5A mutations in 442 neonates and children: Genotype-phenotype correlation and identification of higher-risk subgroups

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