A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5

Taisuke Ishikawa; Akinori Sato; Cherisse A. Marcou; David J. Tester; Michael J. Ackerman; Lia Crotti; Peter J. Schwartz; Young Keun On; Jeong Euy Park; Kazufumi Nakamura; Masayasu Hiraoka; Kiyoshi Nakazawa; Harumizu Sakurada; Takuro Arimura; Naomasa Makita; Akinori Kimura

doi:10.1161/CIRCEP.111.969972

A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5

Taisuke Ishikawa, Akinori Sato, Cherisse A. Marcou, David J. Tester, Michael J. Ackerman, Lia Crotti, Peter J. Schwartz, Young Keun On, Jeong Euy Park, Kazufumi Nakamura, Masayasu Hiraoka, Kiyoshi Nakazawa, Harumizu Sakurada, Takuro Arimura, Naomasa Makita, Akinori Kimura

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

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Abstract

Background: Mutations in genes including SCN5A encoding the α-subunit of the cardiac sodium channel (hNav1.5) cause Brugada syndrome via altered function of cardiac ion channels, but more than two-thirds of Brugada syndrome remains pathogenetically elusive. T-tubules and sarcoplasmic reticulum are essential in excitation of cardiomyocytes, and sarcolemmal membrane-associated protein (SLMAP) is a protein of unknown function localizing at T-tubules and sarcoplasmic reticulum. Methods and Results: We analyzed 190 unrelated Brugada syndrome patients for mutations in SLMAP. Two missense mutations, Val269Ile and Glu710Ala, were found in heterozygous state in 2 patients but were not found in healthy individuals. Membrane surface expression of hNav1.5 in the transfected cells was affected by the mutations, and silencing of mutant SLMAP by small interfering RNA rescued the surface expression of hNav1.5. Whole-cell patch-clamp recordings of hNav1.5-expressing cells transfected with mutant SLMAP confirmed the reduced hNav1.5 current. Conclusions: The mutations in SLMAP may cause Brugada syndrome via modulating the intracellular trafficking of hNav1.5 channel.

Original language	English
Pages (from-to)	1098-1107
Number of pages	10
Journal	Circulation: Arrhythmia and Electrophysiology
Volume	5
Issue number	6
DOIs	https://doi.org/10.1161/CIRCEP.111.969972
Publication status	Published - Dec 2012

Keywords

Arrhythmia mechanisms
Genes
Ion channels
Sarcoplasmic reticulum

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine
Physiology (medical)

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10.1161/CIRCEP.111.969972

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Ishikawa, T., Sato, A., Marcou, C. A., Tester, D. J., Ackerman, M. J., Crotti, L., Schwartz, P. J., On, Y. K., Park, J. E., Nakamura, K., Hiraoka, M., Nakazawa, K., Sakurada, H., Arimura, T., Makita, N., & Kimura, A. (2012). A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5. Circulation: Arrhythmia and Electrophysiology, 5(6), 1098-1107. https://doi.org/10.1161/CIRCEP.111.969972

Ishikawa, T, Sato, A, Marcou, CA, Tester, DJ, Ackerman, MJ, Crotti, L, Schwartz, PJ, On, YK, Park, JE, Nakamura, K, Hiraoka, M, Nakazawa, K, Sakurada, H, Arimura, T, Makita, N & Kimura, A 2012, 'A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5', Circulation: Arrhythmia and Electrophysiology, vol. 5, no. 6, pp. 1098-1107. https://doi.org/10.1161/CIRCEP.111.969972

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title = "A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5",

abstract = "Background: Mutations in genes including SCN5A encoding the α-subunit of the cardiac sodium channel (hNav1.5) cause Brugada syndrome via altered function of cardiac ion channels, but more than two-thirds of Brugada syndrome remains pathogenetically elusive. T-tubules and sarcoplasmic reticulum are essential in excitation of cardiomyocytes, and sarcolemmal membrane-associated protein (SLMAP) is a protein of unknown function localizing at T-tubules and sarcoplasmic reticulum. Methods and Results: We analyzed 190 unrelated Brugada syndrome patients for mutations in SLMAP. Two missense mutations, Val269Ile and Glu710Ala, were found in heterozygous state in 2 patients but were not found in healthy individuals. Membrane surface expression of hNav1.5 in the transfected cells was affected by the mutations, and silencing of mutant SLMAP by small interfering RNA rescued the surface expression of hNav1.5. Whole-cell patch-clamp recordings of hNav1.5-expressing cells transfected with mutant SLMAP confirmed the reduced hNav1.5 current. Conclusions: The mutations in SLMAP may cause Brugada syndrome via modulating the intracellular trafficking of hNav1.5 channel.",

keywords = "Arrhythmia mechanisms, Genes, Ion channels, Sarcoplasmic reticulum",

author = "Taisuke Ishikawa and Akinori Sato and Marcou, {Cherisse A.} and Tester, {David J.} and Ackerman, {Michael J.} and Lia Crotti and Schwartz, {Peter J.} and On, {Young Keun} and Park, {Jeong Euy} and Kazufumi Nakamura and Masayasu Hiraoka and Kiyoshi Nakazawa and Harumizu Sakurada and Takuro Arimura and Naomasa Makita and Akinori Kimura",

year = "2012",

month = dec,

doi = "10.1161/CIRCEP.111.969972",

language = "English",

volume = "5",

pages = "1098--1107",

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T1 - A novel disease gene for Brugada syndrome

T2 - Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5

AU - Ishikawa, Taisuke

AU - Sato, Akinori

AU - Marcou, Cherisse A.

AU - Tester, David J.

AU - Ackerman, Michael J.

AU - Crotti, Lia

AU - Schwartz, Peter J.

AU - On, Young Keun

AU - Park, Jeong Euy

AU - Nakamura, Kazufumi

AU - Hiraoka, Masayasu

AU - Nakazawa, Kiyoshi

AU - Sakurada, Harumizu

AU - Arimura, Takuro

AU - Makita, Naomasa

AU - Kimura, Akinori

PY - 2012/12

Y1 - 2012/12

N2 - Background: Mutations in genes including SCN5A encoding the α-subunit of the cardiac sodium channel (hNav1.5) cause Brugada syndrome via altered function of cardiac ion channels, but more than two-thirds of Brugada syndrome remains pathogenetically elusive. T-tubules and sarcoplasmic reticulum are essential in excitation of cardiomyocytes, and sarcolemmal membrane-associated protein (SLMAP) is a protein of unknown function localizing at T-tubules and sarcoplasmic reticulum. Methods and Results: We analyzed 190 unrelated Brugada syndrome patients for mutations in SLMAP. Two missense mutations, Val269Ile and Glu710Ala, were found in heterozygous state in 2 patients but were not found in healthy individuals. Membrane surface expression of hNav1.5 in the transfected cells was affected by the mutations, and silencing of mutant SLMAP by small interfering RNA rescued the surface expression of hNav1.5. Whole-cell patch-clamp recordings of hNav1.5-expressing cells transfected with mutant SLMAP confirmed the reduced hNav1.5 current. Conclusions: The mutations in SLMAP may cause Brugada syndrome via modulating the intracellular trafficking of hNav1.5 channel.

AB - Background: Mutations in genes including SCN5A encoding the α-subunit of the cardiac sodium channel (hNav1.5) cause Brugada syndrome via altered function of cardiac ion channels, but more than two-thirds of Brugada syndrome remains pathogenetically elusive. T-tubules and sarcoplasmic reticulum are essential in excitation of cardiomyocytes, and sarcolemmal membrane-associated protein (SLMAP) is a protein of unknown function localizing at T-tubules and sarcoplasmic reticulum. Methods and Results: We analyzed 190 unrelated Brugada syndrome patients for mutations in SLMAP. Two missense mutations, Val269Ile and Glu710Ala, were found in heterozygous state in 2 patients but were not found in healthy individuals. Membrane surface expression of hNav1.5 in the transfected cells was affected by the mutations, and silencing of mutant SLMAP by small interfering RNA rescued the surface expression of hNav1.5. Whole-cell patch-clamp recordings of hNav1.5-expressing cells transfected with mutant SLMAP confirmed the reduced hNav1.5 current. Conclusions: The mutations in SLMAP may cause Brugada syndrome via modulating the intracellular trafficking of hNav1.5 channel.

KW - Arrhythmia mechanisms

KW - Genes

KW - Ion channels

KW - Sarcoplasmic reticulum

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A novel disease gene for Brugada syndrome: Sarcolemmal membrane-associated protein gene mutations impair intracellular trafficking of hNav1.5

Abstract

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