Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias

Caroline Pham; Karolina Andrzejczyk; Sean J. Jurgens; Ronald Lekanne Deprez; Kaylin C. A. Palm; Alexa M. C. Vermeer; Janneke Nijman; Imke Christiaans; Daniela Q. C. M. Barge-Schaapveld; Pascal F. H. M. van Dessel; Leander Beekman; Seung Hoan Choi; Steven A. Lubitz; Doris Skoric-Milosavljevic; Lisa van den Bersselaar; Philip R. Jansen; Jaël S. Copier; Patrick T. Ellinor; Arthur A. M. Wilde; Connie R. Bezzina; Elisabeth M. Lodder

doi:https://doi.org/10.1161/CIRCGEN.122.003975

Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias

Caroline Pham, Karolina Andrzejczyk, Sean J. Jurgens, Ronald Lekanne Deprez, Kaylin C. A. Palm, Alexa M. C. Vermeer, Janneke Nijman, Imke Christiaans, Daniela Q. C. M. Barge-Schaapveld, Pascal F. H. M. van Dessel, Leander Beekman, Seung Hoan Choi, Steven A. Lubitz, Doris Skoric-Milosavljevic, Lisa van den Bersselaar, Philip R. Jansen, Jaël S. Copier, Patrick T. Ellinor, Arthur A. M. Wilde, Connie R. BezzinaElisabeth M. Lodder

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

2 Citations (Scopus)

Abstract

BACKGROUND: Genetic variants in TNNI3K (troponin-I interacting kinase) have previously been associated with dilated cardiomyopathy (DCM), cardiac conduction disease, and supraventricular tachycardias. However, the link between TNNI3K variants and these cardiac phenotypes shows a lack of consensus concerning phenotype and protein function. METHODS: We describe a systematic retrospective study of a cohort of patients undergoing genetic testing for cardiac arrhythmias and cardiomyopathy including TNNI3K. We further performed burden testing of TNNI3K in the UK Biobank. For 2 novel TNNI3K variants, we tested cosegregation. TNNI3K kinase function was estimated by TNNI3K autophosphorylation assays. RESULTS: We demonstrate enrichment of rare coding TNNI3K variants in DCM patients in the Amsterdam cohort. In the UK Biobank, we observed an association between TNNI3K missense (but not loss-of-function) variants and DCM and atrial fibrillation. Furthermore, we demonstrate genetic segregation for 2 rare variants, TNNI3K-p.Ile512Thr and TNNI3K-p.His592Tyr, with phenotypes consisting of DCM, cardiac conduction disease, and supraventricular tachycardia, together with increased autophosphorylation. In contrast, TNNI3K-p.Arg556_Asn590del, a likely benign variant, demonstrated depleted autophosphorylation. CONCLUSIONS: Our findings demonstrate an increased burden of rare coding TNNI3K variants in cardiac patients with DCM. Furthermore, we present 2 novel likely pathogenic TNNI3K variants with increased autophosphorylation, suggesting that enhanced autophosphorylation is likely to drive pathogenicity.

Original language	English
Pages (from-to)	328-336
Number of pages	9
Journal	Circulation. Genomic and precision medicine
Volume	16
Issue number	4
DOIs	https://doi.org/10.1161/CIRCGEN.122.003975
Publication status	Published - 1 Aug 2023

Keywords

cardiac arrhythmias
dilated cardiomyopathy
genetics
phosphorylation

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Pham, C., Andrzejczyk, K., Jurgens, S. J., Lekanne Deprez, R., Palm, K. C. A., Vermeer, A. M. C., Nijman, J., Christiaans, I., Barge-Schaapveld, D. Q. C. M., van Dessel, P. F. H. M., Beekman, L., Choi, S. H., Lubitz, S. A., Skoric-Milosavljevic, D., van den Bersselaar, L., Jansen, P. R., Copier, J. S., Ellinor, P. T., Wilde, A. A. M., ... Lodder, E. M. (2023). Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias. Circulation. Genomic and precision medicine, 16(4), 328-336. https://doi.org/10.1161/CIRCGEN.122.003975

@article{f5c3344339c248468654bbc03673396e,

title = "Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias",

abstract = "BACKGROUND: Genetic variants in TNNI3K (troponin-I interacting kinase) have previously been associated with dilated cardiomyopathy (DCM), cardiac conduction disease, and supraventricular tachycardias. However, the link between TNNI3K variants and these cardiac phenotypes shows a lack of consensus concerning phenotype and protein function. METHODS: We describe a systematic retrospective study of a cohort of patients undergoing genetic testing for cardiac arrhythmias and cardiomyopathy including TNNI3K. We further performed burden testing of TNNI3K in the UK Biobank. For 2 novel TNNI3K variants, we tested cosegregation. TNNI3K kinase function was estimated by TNNI3K autophosphorylation assays. RESULTS: We demonstrate enrichment of rare coding TNNI3K variants in DCM patients in the Amsterdam cohort. In the UK Biobank, we observed an association between TNNI3K missense (but not loss-of-function) variants and DCM and atrial fibrillation. Furthermore, we demonstrate genetic segregation for 2 rare variants, TNNI3K-p.Ile512Thr and TNNI3K-p.His592Tyr, with phenotypes consisting of DCM, cardiac conduction disease, and supraventricular tachycardia, together with increased autophosphorylation. In contrast, TNNI3K-p.Arg556_Asn590del, a likely benign variant, demonstrated depleted autophosphorylation. CONCLUSIONS: Our findings demonstrate an increased burden of rare coding TNNI3K variants in cardiac patients with DCM. Furthermore, we present 2 novel likely pathogenic TNNI3K variants with increased autophosphorylation, suggesting that enhanced autophosphorylation is likely to drive pathogenicity.",

keywords = "cardiac arrhythmias, dilated cardiomyopathy, genetics, phosphorylation",

author = "Caroline Pham and Karolina Andrzejczyk and Jurgens, {Sean J.} and {Lekanne Deprez}, Ronald and Palm, {Kaylin C. A.} and Vermeer, {Alexa M. C.} and Janneke Nijman and Imke Christiaans and Barge-Schaapveld, {Daniela Q. C. M.} and {van Dessel}, {Pascal F. H. M.} and Leander Beekman and Choi, {Seung Hoan} and Lubitz, {Steven A.} and Doris Skoric-Milosavljevic and {van den Bersselaar}, Lisa and Jansen, {Philip R.} and Copier, {Ja{\"e}l S.} and Ellinor, {Patrick T.} and Wilde, {Arthur A. M.} and Bezzina, {Connie R.} and Lodder, {Elisabeth M.}",

note = "Funding Information: This research was funded by the Netherlands CardioVascular Research Initiative: CVON2017-15 RESCUED, the Dutch Research Council: NWO Talent Scheme VIDI-91718361 (Drs Lodder, K. Andrzejczyk, and C. Pham), and the AMC funding scheme (J.S. Copier and Dr Lodder). S.J. Jurgens is supported by a Junior Clinical Scientist Fellowship (03-007-2022-0035) from the Dutch Heart Foundation, and by an Amsterdam UMC Doctoral Fellowship (Hartstichting). Dr Ellinor is supported by grants from the National Institutes of Health (1RO1HL092577, 1R01HL157635, 1R01HL157635), by a grant from the American Heart Association Strategically Focused Research Networks (18SFRN34110082), and by a grant from the European Union (MAESTRIA 965286). Dr Lubitz is a full-time employee of Novartis as of July 18, 2022. Prior to his employment at Novartis and during this work, he was supported by NIH grants R01HL139731, R01HL157635 and American Heart Association 18SFRN34250007. Publisher Copyright: {\textcopyright} 2021 Society of Trauma Nurses. Unauthorized reproduction of this article is prohibited.",

year = "2023",

month = aug,

day = "1",

doi = "https://doi.org/10.1161/CIRCGEN.122.003975",

language = "English",

volume = "16",

pages = "328--336",

journal = "Circulation. Genomic and precision medicine",

issn = "2574-8300",

publisher = "Lippincott Williams and Wilkins Ltd.",

number = "4",

}

Pham, C, Andrzejczyk, K, Jurgens, SJ , Lekanne Deprez, R, Palm, KCA, Vermeer, AMC, Nijman, J, Christiaans, I, Barge-Schaapveld, DQCM, van Dessel, PFHM, Beekman, L, Choi, SH, Lubitz, SA, Skoric-Milosavljevic, D, van den Bersselaar, L, Jansen, PR , Copier, JS, Ellinor, PT, Wilde, AAM , Bezzina, CR & Lodder, EM 2023, 'Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias', Circulation. Genomic and precision medicine, vol. 16, no. 4, pp. 328-336. https://doi.org/10.1161/CIRCGEN.122.003975

TY - JOUR

T1 - Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias

AU - Pham, Caroline

AU - Andrzejczyk, Karolina

AU - Jurgens, Sean J.

AU - Lekanne Deprez, Ronald

AU - Palm, Kaylin C. A.

AU - Vermeer, Alexa M. C.

AU - Nijman, Janneke

AU - Christiaans, Imke

AU - Barge-Schaapveld, Daniela Q. C. M.

AU - van Dessel, Pascal F. H. M.

AU - Beekman, Leander

AU - Choi, Seung Hoan

AU - Lubitz, Steven A.

AU - Skoric-Milosavljevic, Doris

AU - van den Bersselaar, Lisa

AU - Jansen, Philip R.

AU - Copier, Jaël S.

AU - Ellinor, Patrick T.

AU - Wilde, Arthur A. M.

AU - Bezzina, Connie R.

AU - Lodder, Elisabeth M.

N1 - Funding Information: This research was funded by the Netherlands CardioVascular Research Initiative: CVON2017-15 RESCUED, the Dutch Research Council: NWO Talent Scheme VIDI-91718361 (Drs Lodder, K. Andrzejczyk, and C. Pham), and the AMC funding scheme (J.S. Copier and Dr Lodder). S.J. Jurgens is supported by a Junior Clinical Scientist Fellowship (03-007-2022-0035) from the Dutch Heart Foundation, and by an Amsterdam UMC Doctoral Fellowship (Hartstichting). Dr Ellinor is supported by grants from the National Institutes of Health (1RO1HL092577, 1R01HL157635, 1R01HL157635), by a grant from the American Heart Association Strategically Focused Research Networks (18SFRN34110082), and by a grant from the European Union (MAESTRIA 965286). Dr Lubitz is a full-time employee of Novartis as of July 18, 2022. Prior to his employment at Novartis and during this work, he was supported by NIH grants R01HL139731, R01HL157635 and American Heart Association 18SFRN34250007. Publisher Copyright: © 2021 Society of Trauma Nurses. Unauthorized reproduction of this article is prohibited.

PY - 2023/8/1

Y1 - 2023/8/1

N2 - BACKGROUND: Genetic variants in TNNI3K (troponin-I interacting kinase) have previously been associated with dilated cardiomyopathy (DCM), cardiac conduction disease, and supraventricular tachycardias. However, the link between TNNI3K variants and these cardiac phenotypes shows a lack of consensus concerning phenotype and protein function. METHODS: We describe a systematic retrospective study of a cohort of patients undergoing genetic testing for cardiac arrhythmias and cardiomyopathy including TNNI3K. We further performed burden testing of TNNI3K in the UK Biobank. For 2 novel TNNI3K variants, we tested cosegregation. TNNI3K kinase function was estimated by TNNI3K autophosphorylation assays. RESULTS: We demonstrate enrichment of rare coding TNNI3K variants in DCM patients in the Amsterdam cohort. In the UK Biobank, we observed an association between TNNI3K missense (but not loss-of-function) variants and DCM and atrial fibrillation. Furthermore, we demonstrate genetic segregation for 2 rare variants, TNNI3K-p.Ile512Thr and TNNI3K-p.His592Tyr, with phenotypes consisting of DCM, cardiac conduction disease, and supraventricular tachycardia, together with increased autophosphorylation. In contrast, TNNI3K-p.Arg556_Asn590del, a likely benign variant, demonstrated depleted autophosphorylation. CONCLUSIONS: Our findings demonstrate an increased burden of rare coding TNNI3K variants in cardiac patients with DCM. Furthermore, we present 2 novel likely pathogenic TNNI3K variants with increased autophosphorylation, suggesting that enhanced autophosphorylation is likely to drive pathogenicity.

AB - BACKGROUND: Genetic variants in TNNI3K (troponin-I interacting kinase) have previously been associated with dilated cardiomyopathy (DCM), cardiac conduction disease, and supraventricular tachycardias. However, the link between TNNI3K variants and these cardiac phenotypes shows a lack of consensus concerning phenotype and protein function. METHODS: We describe a systematic retrospective study of a cohort of patients undergoing genetic testing for cardiac arrhythmias and cardiomyopathy including TNNI3K. We further performed burden testing of TNNI3K in the UK Biobank. For 2 novel TNNI3K variants, we tested cosegregation. TNNI3K kinase function was estimated by TNNI3K autophosphorylation assays. RESULTS: We demonstrate enrichment of rare coding TNNI3K variants in DCM patients in the Amsterdam cohort. In the UK Biobank, we observed an association between TNNI3K missense (but not loss-of-function) variants and DCM and atrial fibrillation. Furthermore, we demonstrate genetic segregation for 2 rare variants, TNNI3K-p.Ile512Thr and TNNI3K-p.His592Tyr, with phenotypes consisting of DCM, cardiac conduction disease, and supraventricular tachycardia, together with increased autophosphorylation. In contrast, TNNI3K-p.Arg556_Asn590del, a likely benign variant, demonstrated depleted autophosphorylation. CONCLUSIONS: Our findings demonstrate an increased burden of rare coding TNNI3K variants in cardiac patients with DCM. Furthermore, we present 2 novel likely pathogenic TNNI3K variants with increased autophosphorylation, suggesting that enhanced autophosphorylation is likely to drive pathogenicity.

KW - cardiac arrhythmias

KW - dilated cardiomyopathy

KW - genetics

KW - phosphorylation

UR - http://www.scopus.com/inward/record.url?scp=85168222844&partnerID=8YFLogxK

U2 - https://doi.org/10.1161/CIRCGEN.122.003975

DO - https://doi.org/10.1161/CIRCGEN.122.003975

M3 - Article

C2 - 37199186

SN - 2574-8300

VL - 16

SP - 328

EP - 336

JO - Circulation. Genomic and precision medicine

JF - Circulation. Genomic and precision medicine

IS - 4

ER -

Genetic Burden of TNNI3K in Diagnostic Testing of Patients With Dilated Cardiomyopathy and Supraventricular Arrhythmias

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Keywords

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