Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy

Maartje Noorman; Sara Hakim; Elise Kessler; Judith A. Groeneweg; Moniek G P J Cox; Angeliki Asimaki; Harold V. M.  van Rijen; Leonie Van Stuijvenberg; Halina Chkourko; Marcel A G Van Der Heyden; Marc A. Vos; Nicolaas De Jonge; Jasper J. Van Der Smagt; Dennis Dooijes; Aryan Vink; Roel A. De Weger; Andras Varro; Jacques M T De Bakker; Jeffrey E. Saffitz; Thomas J. Hund; Peter J. Mohler; Mario Delmar; Richard N W Hauer; Toon A B Van Veen

doi:10.1016/j.hrthm.2012.11.018

Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy

Maartje Noorman, Sara Hakim, Elise Kessler, Judith A. Groeneweg, Moniek G P J Cox, Angeliki Asimaki, Harold V. M. van Rijen, Leonie Van Stuijvenberg, Halina Chkourko, Marcel A G Van Der Heyden, Marc A. Vos, Nicolaas De Jonge, Jasper J. Van Der Smagt, Dennis Dooijes, Aryan Vink, Roel A. De Weger, Andras Varro, Jacques M T De Bakker, Jeffrey E. Saffitz, Thomas J. HundPeter J. Mohler, Mario Delmar, Richard N W Hauer, Toon A B Van Veen^*

^*Corresponding author for this work

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

28 Citations (Scopus)

Abstract

BACKGROUND Arrhythmogenic cardiomyopathy (AC) is closely associated with desmosomal mutations in a majority of patients. Arrhythmogenesis in patients with AC is likely related to remodeling of cardiac gap junctions and increased levels of fibrosis. Recently, using experimental models, we also identified sodium channel dysfunction secondary to desmosomal dysfunction.

OBJECTIVE To assess the immunoreactive signal levels of the sodium channel protein Na(V)1.5, as well as connexin43 (Cx43) and plakoglobin (PKG), in myocardial specimens obtained from patients with AC.

METHODS left and right ventricular free wall postmortem material was obtained from 5 patients with AC and 5 controls matched for age and sex. Right ventricular septal biopsies were taken from another 15 patients with AC. All patients fulfilled the 2010 revised Task Force Criteria for the diagnosis of AC. Immunohistochemical analyses were performed using antibodies against Cx43, PKG, Na(V)1.5, plakophilin-2, and N-cadherin.

RESULTS N-cadherin and desmoplakin immunoreactive signals and distribution were normal in patients with AC compared to controls. Plakophilin-2 signals were unaffected unless a plakophilin-2 mutation predicting haploinsufficiency was present. Distribution was unchanged compared to that in controls. Immunoreactive signal levels of PKG, Cx43, and Na(V)1.5 were disturbed in 74%, 70%, and 65% of the patients, respectively.

CONCLUSIONS A reduced immunoreactive signal of PKG, Cx43, and Na(V)1.5 at the intercalated disks can be observed in a large majority of the patients. Decreased levels of Na(V)1.5 might contribute to arrhythmia vulnerability and, in the future, potentially could serve as a new clinically relevant toot for risk assessment strategies.

Original language	English
Pages (from-to)	412-419
Number of pages	8
Journal	Heart Rhythm
Volume	10
Issue number	3
DOIs	https://doi.org/10.1016/j.hrthm.2012.11.018
Publication status	Published - 2013

Keywords

AC
Arrhythmogenic cardiomyopathy
Connexin 43
Na(V)1.5
Desmosome
Plakophilin-2
Plakoglobin
Immunohistochemistry
RIGHT-VENTRICULAR CARDIOMYOPATHY
HETEROGENEOUS EXPRESSION
MEMBRANE EXCITABILITY
HEART-FAILURE
GAP-JUNCTIONS
PLAKOPHILIN-2
CONDUCTION
MUTATIONS
MODEL
MICE

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10.1016/j.hrthm.2012.11.018

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Noorman, M., Hakim, S., Kessler, E., Groeneweg, J. A., Cox, M. G. P. J., Asimaki, A., van Rijen, H. V. M., Van Stuijvenberg, L., Chkourko, H., Van Der Heyden, M. A. G., Vos, M. A., De Jonge, N., Van Der Smagt, J. J., Dooijes, D., Vink, A., De Weger, R. A., Varro, A., De Bakker, J. M. T., Saffitz, J. E., ... Van Veen, T. A. B. (2013). Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy. Heart Rhythm, 10(3), 412-419. https://doi.org/10.1016/j.hrthm.2012.11.018

@article{804e362305404d5786c07fec6f17752f,

title = "Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy",

abstract = "BACKGROUND Arrhythmogenic cardiomyopathy (AC) is closely associated with desmosomal mutations in a majority of patients. Arrhythmogenesis in patients with AC is likely related to remodeling of cardiac gap junctions and increased levels of fibrosis. Recently, using experimental models, we also identified sodium channel dysfunction secondary to desmosomal dysfunction.OBJECTIVE To assess the immunoreactive signal levels of the sodium channel protein Na(V)1.5, as well as connexin43 (Cx43) and plakoglobin (PKG), in myocardial specimens obtained from patients with AC.METHODS left and right ventricular free wall postmortem material was obtained from 5 patients with AC and 5 controls matched for age and sex. Right ventricular septal biopsies were taken from another 15 patients with AC. All patients fulfilled the 2010 revised Task Force Criteria for the diagnosis of AC. Immunohistochemical analyses were performed using antibodies against Cx43, PKG, Na(V)1.5, plakophilin-2, and N-cadherin.RESULTS N-cadherin and desmoplakin immunoreactive signals and distribution were normal in patients with AC compared to controls. Plakophilin-2 signals were unaffected unless a plakophilin-2 mutation predicting haploinsufficiency was present. Distribution was unchanged compared to that in controls. Immunoreactive signal levels of PKG, Cx43, and Na(V)1.5 were disturbed in 74%, 70%, and 65% of the patients, respectively.CONCLUSIONS A reduced immunoreactive signal of PKG, Cx43, and Na(V)1.5 at the intercalated disks can be observed in a large majority of the patients. Decreased levels of Na(V)1.5 might contribute to arrhythmia vulnerability and, in the future, potentially could serve as a new clinically relevant toot for risk assessment strategies.",

keywords = "AC, Arrhythmogenic cardiomyopathy, Connexin 43, Na(V)1.5, Desmosome, Plakophilin-2, Plakoglobin, Immunohistochemistry, RIGHT-VENTRICULAR CARDIOMYOPATHY, HETEROGENEOUS EXPRESSION, MEMBRANE EXCITABILITY, HEART-FAILURE, GAP-JUNCTIONS, PLAKOPHILIN-2, CONDUCTION, MUTATIONS, MODEL, MICE",

author = "Maartje Noorman and Sara Hakim and Elise Kessler and Groeneweg, {Judith A.} and Cox, {Moniek G P J} and Angeliki Asimaki and {van Rijen}, {Harold V. M.} and {Van Stuijvenberg}, Leonie and Halina Chkourko and {Van Der Heyden}, {Marcel A G} and Vos, {Marc A.} and {De Jonge}, Nicolaas and {Van Der Smagt}, {Jasper J.} and Dennis Dooijes and Aryan Vink and {De Weger}, {Roel A.} and Andras Varro and {De Bakker}, {Jacques M T} and Saffitz, {Jeffrey E.} and Hund, {Thomas J.} and Mohler, {Peter J.} and Mario Delmar and Hauer, {Richard N W} and {Van Veen}, {Toon A B}",

year = "2013",

doi = "10.1016/j.hrthm.2012.11.018",

language = "English",

volume = "10",

pages = "412--419",

journal = "Heart Rhythm",

issn = "1547-5271",

publisher = "Elsevier",

number = "3",

}

Noorman, M, Hakim, S, Kessler, E, Groeneweg, JA, Cox, MGPJ, Asimaki, A, van Rijen, HVM, Van Stuijvenberg, L, Chkourko, H, Van Der Heyden, MAG , Vos, MA, De Jonge, N, Van Der Smagt, JJ , Dooijes, D, Vink, A, De Weger, RA, Varro, A, De Bakker, JMT, Saffitz, JE, Hund, TJ, Mohler, PJ, Delmar, M, Hauer, RNW & Van Veen, TAB 2013, 'Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy', Heart Rhythm, vol. 10, no. 3, pp. 412-419. https://doi.org/10.1016/j.hrthm.2012.11.018

TY - JOUR

T1 - Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy

AU - Noorman, Maartje

AU - Hakim, Sara

AU - Kessler, Elise

AU - Groeneweg, Judith A.

AU - Cox, Moniek G P J

AU - Asimaki, Angeliki

AU - van Rijen, Harold V. M.

AU - Van Stuijvenberg, Leonie

AU - Chkourko, Halina

AU - Van Der Heyden, Marcel A G

AU - Vos, Marc A.

AU - De Jonge, Nicolaas

AU - Van Der Smagt, Jasper J.

AU - Dooijes, Dennis

AU - Vink, Aryan

AU - De Weger, Roel A.

AU - Varro, Andras

AU - De Bakker, Jacques M T

AU - Saffitz, Jeffrey E.

AU - Hund, Thomas J.

AU - Mohler, Peter J.

AU - Delmar, Mario

AU - Hauer, Richard N W

AU - Van Veen, Toon A B

PY - 2013

Y1 - 2013

N2 - BACKGROUND Arrhythmogenic cardiomyopathy (AC) is closely associated with desmosomal mutations in a majority of patients. Arrhythmogenesis in patients with AC is likely related to remodeling of cardiac gap junctions and increased levels of fibrosis. Recently, using experimental models, we also identified sodium channel dysfunction secondary to desmosomal dysfunction.OBJECTIVE To assess the immunoreactive signal levels of the sodium channel protein Na(V)1.5, as well as connexin43 (Cx43) and plakoglobin (PKG), in myocardial specimens obtained from patients with AC.METHODS left and right ventricular free wall postmortem material was obtained from 5 patients with AC and 5 controls matched for age and sex. Right ventricular septal biopsies were taken from another 15 patients with AC. All patients fulfilled the 2010 revised Task Force Criteria for the diagnosis of AC. Immunohistochemical analyses were performed using antibodies against Cx43, PKG, Na(V)1.5, plakophilin-2, and N-cadherin.RESULTS N-cadherin and desmoplakin immunoreactive signals and distribution were normal in patients with AC compared to controls. Plakophilin-2 signals were unaffected unless a plakophilin-2 mutation predicting haploinsufficiency was present. Distribution was unchanged compared to that in controls. Immunoreactive signal levels of PKG, Cx43, and Na(V)1.5 were disturbed in 74%, 70%, and 65% of the patients, respectively.CONCLUSIONS A reduced immunoreactive signal of PKG, Cx43, and Na(V)1.5 at the intercalated disks can be observed in a large majority of the patients. Decreased levels of Na(V)1.5 might contribute to arrhythmia vulnerability and, in the future, potentially could serve as a new clinically relevant toot for risk assessment strategies.

AB - BACKGROUND Arrhythmogenic cardiomyopathy (AC) is closely associated with desmosomal mutations in a majority of patients. Arrhythmogenesis in patients with AC is likely related to remodeling of cardiac gap junctions and increased levels of fibrosis. Recently, using experimental models, we also identified sodium channel dysfunction secondary to desmosomal dysfunction.OBJECTIVE To assess the immunoreactive signal levels of the sodium channel protein Na(V)1.5, as well as connexin43 (Cx43) and plakoglobin (PKG), in myocardial specimens obtained from patients with AC.METHODS left and right ventricular free wall postmortem material was obtained from 5 patients with AC and 5 controls matched for age and sex. Right ventricular septal biopsies were taken from another 15 patients with AC. All patients fulfilled the 2010 revised Task Force Criteria for the diagnosis of AC. Immunohistochemical analyses were performed using antibodies against Cx43, PKG, Na(V)1.5, plakophilin-2, and N-cadherin.RESULTS N-cadherin and desmoplakin immunoreactive signals and distribution were normal in patients with AC compared to controls. Plakophilin-2 signals were unaffected unless a plakophilin-2 mutation predicting haploinsufficiency was present. Distribution was unchanged compared to that in controls. Immunoreactive signal levels of PKG, Cx43, and Na(V)1.5 were disturbed in 74%, 70%, and 65% of the patients, respectively.CONCLUSIONS A reduced immunoreactive signal of PKG, Cx43, and Na(V)1.5 at the intercalated disks can be observed in a large majority of the patients. Decreased levels of Na(V)1.5 might contribute to arrhythmia vulnerability and, in the future, potentially could serve as a new clinically relevant toot for risk assessment strategies.

KW - AC

KW - Arrhythmogenic cardiomyopathy

KW - Connexin 43

KW - Na(V)1.5

KW - Desmosome

KW - Plakophilin-2

KW - Plakoglobin

KW - Immunohistochemistry

KW - RIGHT-VENTRICULAR CARDIOMYOPATHY

KW - HETEROGENEOUS EXPRESSION

KW - MEMBRANE EXCITABILITY

KW - HEART-FAILURE

KW - GAP-JUNCTIONS

KW - PLAKOPHILIN-2

KW - CONDUCTION

KW - MUTATIONS

KW - MODEL

KW - MICE

UR - http://www.scopus.com/inward/record.url?scp=84875364545&partnerID=8YFLogxK

U2 - 10.1016/j.hrthm.2012.11.018

DO - 10.1016/j.hrthm.2012.11.018

M3 - Article

C2 - 23178689

SN - 1547-5271

VL - 10

SP - 412

EP - 419

JO - Heart Rhythm

JF - Heart Rhythm

IS - 3

ER -

Remodeling of the cardiac sodium channel, connexin43, and plakoglobin at the intercalated disk in patients with arrhythmogenic cardiomyopathy

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