Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant

Matthew J. O'Neill; Suet Nee Chen; Lynne Rumping; Renee Johnson; Marjon van Slegtenhorst; Andrew M. Glazer; Tao Yang; Joseph F. Solus; Julie Laudeman; Devyn W. Mitchell; Loren R. Vanags; Brett M. Kroncke; Katherine Anderson; Shanshan Gao; Job A. J. Verdonschot; Han Brunner; Debby Hellebrekers; Matthew R. G. Taylor; Dan M. Roden; Marja W. Wessels; Ronald H. Lekanne Dit Deprez; Diane Fatkin; Luisa Mestroni; M. Benjamin Shoemaker

doi:https://doi.org/10.1016/j.hrthm.2023.05.006

Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant

Matthew J. O'Neill, Suet Nee Chen, Lynne Rumping, Renee Johnson, Marjon van Slegtenhorst, Andrew M. Glazer, Tao Yang, Joseph F. Solus, Julie Laudeman, Devyn W. Mitchell, Loren R. Vanags, Brett M. Kroncke, Katherine Anderson, Shanshan Gao, Job A. J. Verdonschot, Han Brunner, Debby Hellebrekers, Matthew R. G. Taylor, Dan M. Roden, Marja W. WesselsRonald H. Lekanne Dit Deprez, Diane Fatkin, Luisa Mestroni, M. Benjamin Shoemaker

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

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Abstract

Background: Truncating variants in filamin C (FLNC) can cause arrhythmogenic cardiomyopathy (ACM) through haploinsufficiency. Noncanonical splice-altering variants may contribute to this phenotype. Objective: The purpose of this study was to investigate the clinical and functional consequences of a recurrent FLNC intronic variant of uncertain significance (VUS), c.970-4A>G. Methods: Clinical data in 9 variant heterozygotes from 4 kindreds were obtained from 5 tertiary health care centers. We used in silico predictors and functional studies with peripheral blood and patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs). Isolated RNA was studied by reverse transcription polymerase chain reaction. iPSC-CMs were further characterized at baseline and after nonsense-mediated decay (NMD) inhibition, using quantitative polymerase chain reaction (qPCR), RNA-sequencing, and cellular electrophysiology. American College of Medical Genetics and Genomics (ACMG) criteria were used to adjudicate variant pathogenicity. Results: Variant heterozygotes displayed a spectrum of disease phenotypes, spanning from mild ventricular dysfunction with palpitations to severe ventricular arrhythmias requiring device shocks or progressive cardiomyopathy requiring heart transplantation. Consistent with in silico predictors, the c.970-4A>G FLNC variant activated a cryptic splice acceptor site, introducing a 3-bp insertion containing a premature termination codon. NMD inhibition upregulated aberrantly spliced transcripts by qPCR and RNA-sequencing. Patch clamp studies revealed irregular spontaneous action potentials, increased action potential duration, and increased sodium late current in proband-derived iPSC-CMs. These findings fulfilled multiple ACMG criteria for pathogenicity. Conclusion: Clinical, in silico, and functional evidence support the prediction that the intronic c.970-4A>G VUS disrupts splicing and drives ACM, enabling reclassification from VUS to pathogenic.

Original language	English
Pages (from-to)	1158-1166
Number of pages	9
Journal	Heart Rhythm
Volume	20
Issue number	8
Early online date	2023
DOIs	https://doi.org/10.1016/j.hrthm.2023.05.006
Publication status	Published - Aug 2023

Keywords

Arrhythmia
Arrhythmogenic cardiomyopathy
Functional genetics
Nonsense-mediated decay
Splicing

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O'Neill, M. J., Chen, S. N., Rumping, L., Johnson, R., van Slegtenhorst, M., Glazer, A. M., Yang, T., Solus, J. F., Laudeman, J., Mitchell, D. W., Vanags, L. R., Kroncke, B. M., Anderson, K., Gao, S., Verdonschot, J. A. J., Brunner, H., Hellebrekers, D., Taylor, M. R. G., Roden, D. M., ... Shoemaker, M. B. (2023). Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant. Heart Rhythm, 20(8), 1158-1166. https://doi.org/10.1016/j.hrthm.2023.05.006

@article{46388a28eb3c412cafb59d30d2393178,

title = "Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant",

abstract = "Background: Truncating variants in filamin C (FLNC) can cause arrhythmogenic cardiomyopathy (ACM) through haploinsufficiency. Noncanonical splice-altering variants may contribute to this phenotype. Objective: The purpose of this study was to investigate the clinical and functional consequences of a recurrent FLNC intronic variant of uncertain significance (VUS), c.970-4A>G. Methods: Clinical data in 9 variant heterozygotes from 4 kindreds were obtained from 5 tertiary health care centers. We used in silico predictors and functional studies with peripheral blood and patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs). Isolated RNA was studied by reverse transcription polymerase chain reaction. iPSC-CMs were further characterized at baseline and after nonsense-mediated decay (NMD) inhibition, using quantitative polymerase chain reaction (qPCR), RNA-sequencing, and cellular electrophysiology. American College of Medical Genetics and Genomics (ACMG) criteria were used to adjudicate variant pathogenicity. Results: Variant heterozygotes displayed a spectrum of disease phenotypes, spanning from mild ventricular dysfunction with palpitations to severe ventricular arrhythmias requiring device shocks or progressive cardiomyopathy requiring heart transplantation. Consistent with in silico predictors, the c.970-4A>G FLNC variant activated a cryptic splice acceptor site, introducing a 3-bp insertion containing a premature termination codon. NMD inhibition upregulated aberrantly spliced transcripts by qPCR and RNA-sequencing. Patch clamp studies revealed irregular spontaneous action potentials, increased action potential duration, and increased sodium late current in proband-derived iPSC-CMs. These findings fulfilled multiple ACMG criteria for pathogenicity. Conclusion: Clinical, in silico, and functional evidence support the prediction that the intronic c.970-4A>G VUS disrupts splicing and drives ACM, enabling reclassification from VUS to pathogenic.",

keywords = "Arrhythmia, Arrhythmogenic cardiomyopathy, Functional genetics, Nonsense-mediated decay, Splicing",

author = "O'Neill, {Matthew J.} and Chen, {Suet Nee} and Lynne Rumping and Renee Johnson and {van Slegtenhorst}, Marjon and Glazer, {Andrew M.} and Tao Yang and Solus, {Joseph F.} and Julie Laudeman and Mitchell, {Devyn W.} and Vanags, {Loren R.} and Kroncke, {Brett M.} and Katherine Anderson and Shanshan Gao and Verdonschot, {Job A. J.} and Han Brunner and Debby Hellebrekers and Taylor, {Matthew R. G.} and Roden, {Dan M.} and Wessels, {Marja W.} and {Lekanne Dit Deprez}, {Ronald H.} and Diane Fatkin and Luisa Mestroni and Shoemaker, {M. Benjamin}",

note = "Funding Information: This research was funded by American Heart Association (AHA) 907581 to Matthew J. O{\textquoteright}Neill; NIH 1F30HL163923-01 to Matthew J. O{\textquoteright}Neill; R01HL149826 to Dr Roden; NSW Health and Australian Genomics to Dr Fatkin; R01HL147064 to Drs Taylor and Mestroni; Boettcher Investigator Webb-Waring Biomedical Research Award to Dr Chen; T32 Fellowship to Dr Gao; AHA 20SCG35540034 to Dr Shoemaker; and R01HL155197 to Dr Shoemaker. Flow Cytometry experiments were performed in the VMC Flow Cytometry Shared Resource, which is supported by the Vanderbilt Ingram Cancer Center (P30 CA68485) and the Vanderbilt Digestive Disease Research Center (DK058404). Funding Information: Dr Shoemaker has received sponsored research funding from Roche Pharmaceuticals to Vanderbilt University Medical Center . All other author have no conflicts of interest to disclose. Publisher Copyright: {\textcopyright} 2023",

year = "2023",

month = aug,

doi = "https://doi.org/10.1016/j.hrthm.2023.05.006",

language = "English",

volume = "20",

pages = "1158--1166",

journal = "Heart Rhythm",

issn = "1547-5271",

publisher = "Elsevier",

number = "8",

}

O'Neill, MJ, Chen, SN, Rumping, L, Johnson, R, van Slegtenhorst, M, Glazer, AM, Yang, T, Solus, JF, Laudeman, J, Mitchell, DW, Vanags, LR, Kroncke, BM, Anderson, K, Gao, S, Verdonschot, JAJ, Brunner, H, Hellebrekers, D, Taylor, MRG, Roden, DM, Wessels, MW, Lekanne Dit Deprez, RH, Fatkin, D, Mestroni, L & Shoemaker, MB 2023, 'Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant', Heart Rhythm, vol. 20, no. 8, pp. 1158-1166. https://doi.org/10.1016/j.hrthm.2023.05.006

TY - JOUR

T1 - Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant

AU - O'Neill, Matthew J.

AU - Chen, Suet Nee

AU - Rumping, Lynne

AU - Johnson, Renee

AU - van Slegtenhorst, Marjon

AU - Glazer, Andrew M.

AU - Yang, Tao

AU - Solus, Joseph F.

AU - Laudeman, Julie

AU - Mitchell, Devyn W.

AU - Vanags, Loren R.

AU - Kroncke, Brett M.

AU - Anderson, Katherine

AU - Gao, Shanshan

AU - Verdonschot, Job A. J.

AU - Brunner, Han

AU - Hellebrekers, Debby

AU - Taylor, Matthew R. G.

AU - Roden, Dan M.

AU - Wessels, Marja W.

AU - Lekanne Dit Deprez, Ronald H.

AU - Fatkin, Diane

AU - Mestroni, Luisa

AU - Shoemaker, M. Benjamin

N1 - Funding Information: This research was funded by American Heart Association (AHA) 907581 to Matthew J. O’Neill; NIH 1F30HL163923-01 to Matthew J. O’Neill; R01HL149826 to Dr Roden; NSW Health and Australian Genomics to Dr Fatkin; R01HL147064 to Drs Taylor and Mestroni; Boettcher Investigator Webb-Waring Biomedical Research Award to Dr Chen; T32 Fellowship to Dr Gao; AHA 20SCG35540034 to Dr Shoemaker; and R01HL155197 to Dr Shoemaker. Flow Cytometry experiments were performed in the VMC Flow Cytometry Shared Resource, which is supported by the Vanderbilt Ingram Cancer Center (P30 CA68485) and the Vanderbilt Digestive Disease Research Center (DK058404). Funding Information: Dr Shoemaker has received sponsored research funding from Roche Pharmaceuticals to Vanderbilt University Medical Center . All other author have no conflicts of interest to disclose. Publisher Copyright: © 2023

PY - 2023/8

Y1 - 2023/8

N2 - Background: Truncating variants in filamin C (FLNC) can cause arrhythmogenic cardiomyopathy (ACM) through haploinsufficiency. Noncanonical splice-altering variants may contribute to this phenotype. Objective: The purpose of this study was to investigate the clinical and functional consequences of a recurrent FLNC intronic variant of uncertain significance (VUS), c.970-4A>G. Methods: Clinical data in 9 variant heterozygotes from 4 kindreds were obtained from 5 tertiary health care centers. We used in silico predictors and functional studies with peripheral blood and patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs). Isolated RNA was studied by reverse transcription polymerase chain reaction. iPSC-CMs were further characterized at baseline and after nonsense-mediated decay (NMD) inhibition, using quantitative polymerase chain reaction (qPCR), RNA-sequencing, and cellular electrophysiology. American College of Medical Genetics and Genomics (ACMG) criteria were used to adjudicate variant pathogenicity. Results: Variant heterozygotes displayed a spectrum of disease phenotypes, spanning from mild ventricular dysfunction with palpitations to severe ventricular arrhythmias requiring device shocks or progressive cardiomyopathy requiring heart transplantation. Consistent with in silico predictors, the c.970-4A>G FLNC variant activated a cryptic splice acceptor site, introducing a 3-bp insertion containing a premature termination codon. NMD inhibition upregulated aberrantly spliced transcripts by qPCR and RNA-sequencing. Patch clamp studies revealed irregular spontaneous action potentials, increased action potential duration, and increased sodium late current in proband-derived iPSC-CMs. These findings fulfilled multiple ACMG criteria for pathogenicity. Conclusion: Clinical, in silico, and functional evidence support the prediction that the intronic c.970-4A>G VUS disrupts splicing and drives ACM, enabling reclassification from VUS to pathogenic.

AB - Background: Truncating variants in filamin C (FLNC) can cause arrhythmogenic cardiomyopathy (ACM) through haploinsufficiency. Noncanonical splice-altering variants may contribute to this phenotype. Objective: The purpose of this study was to investigate the clinical and functional consequences of a recurrent FLNC intronic variant of uncertain significance (VUS), c.970-4A>G. Methods: Clinical data in 9 variant heterozygotes from 4 kindreds were obtained from 5 tertiary health care centers. We used in silico predictors and functional studies with peripheral blood and patient-specific induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs). Isolated RNA was studied by reverse transcription polymerase chain reaction. iPSC-CMs were further characterized at baseline and after nonsense-mediated decay (NMD) inhibition, using quantitative polymerase chain reaction (qPCR), RNA-sequencing, and cellular electrophysiology. American College of Medical Genetics and Genomics (ACMG) criteria were used to adjudicate variant pathogenicity. Results: Variant heterozygotes displayed a spectrum of disease phenotypes, spanning from mild ventricular dysfunction with palpitations to severe ventricular arrhythmias requiring device shocks or progressive cardiomyopathy requiring heart transplantation. Consistent with in silico predictors, the c.970-4A>G FLNC variant activated a cryptic splice acceptor site, introducing a 3-bp insertion containing a premature termination codon. NMD inhibition upregulated aberrantly spliced transcripts by qPCR and RNA-sequencing. Patch clamp studies revealed irregular spontaneous action potentials, increased action potential duration, and increased sodium late current in proband-derived iPSC-CMs. These findings fulfilled multiple ACMG criteria for pathogenicity. Conclusion: Clinical, in silico, and functional evidence support the prediction that the intronic c.970-4A>G VUS disrupts splicing and drives ACM, enabling reclassification from VUS to pathogenic.

KW - Arrhythmia

KW - Arrhythmogenic cardiomyopathy

KW - Functional genetics

KW - Nonsense-mediated decay

KW - Splicing

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U2 - https://doi.org/10.1016/j.hrthm.2023.05.006

DO - https://doi.org/10.1016/j.hrthm.2023.05.006

M3 - Article

C2 - 37164047

SN - 1547-5271

VL - 20

SP - 1158

EP - 1166

JO - Heart Rhythm

JF - Heart Rhythm

IS - 8

ER -

Multicenter clinical and functional evidence reclassifies a recurrent noncanonical filamin C splice-altering variant

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Keywords

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