Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel

Jennifer L. Smith; David J. Tester; Allison R. Hall; Don E. Burgess; Chun Chun Hsu; Samy Claude Elayi; Corey L. Anderson; Craig T. January; Jonathan Z. Luo; Dustin N. Hartzel; Uyenlinh L. Mirshahi; Michael F. Murray; Tooraj Mirshahi; Michael J. Ackerman; Brian P. Delisle

doi:10.1161/CIRCEP.117.005859

Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel

Jennifer L. Smith, David J. Tester, Allison R. Hall, Don E. Burgess, Chun Chun Hsu, Samy Claude Elayi, Corey L. Anderson, Craig T. January, Jonathan Z. Luo, Dustin N. Hartzel, Uyenlinh L. Mirshahi, Michael F. Murray, Tooraj Mirshahi, Michael J. Ackerman, Brian P. Delisle

Cardiovascular Medicine

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

1 Scopus citations

Abstract

BACKGROUND: Heterologous functional validation studies of putative long-QT syndrome subtype 2-associated variants clarify their pathological potential and identify disease mechanism(s) for most variants studied. The purpose of this study is to clarify the pathological potential for rare nonsynonymous KCNH2 variants seemingly associated with sudden infant death syndrome. METHODS: Genetic testing of 292 sudden infant death syndrome cases identified 9 KCNH2 variants: E90K, R181Q, A190T, G294V, R791W, P967L, R1005W, R1047L, and Q1068R. Previous studies show R181Q-, P967L-, and R1047L-Kv11.1 channels function similar to wild-type Kv11.1 channels, whereas Q1068R-Kv11.1 channels accelerate inactivation gating. We studied the biochemical and biophysical properties for E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels expressed in human embryonic kidney 293 cells; examined the electronic health records of patients who were genotype positive for the sudden infant death syndrome-linked KCNH2 variants; and simulated their functional impact using computational models of the human ventricular action potential. RESULTS: Western blot and voltage-clamping analyses of cells expressing E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels demonstrated these variants express and generate peak Kv11.1 current levels similar to cells expressing wild-type-Kv11.1 channels, but R791W- and R1005W-Kv11.1 channels accelerated deactivation and activation gating, respectively. Electronic health records of patients with the sudden infant death syndrome-linked KCNH2 variants showed that the patients had median heart rate-corrected QT intervals <480 ms and none had been diagnosed with long-QT syndrome or experienced cardiac arrest. Simulating the impact of dysfunctional gating variants predicted that they have little impact on ventricular action potential duration. CONCLUSIONS: We conclude that these rare Kv11.1 missense variants are not long-QT syndrome subtype 2-causative variants and therefore do not represent the pathogenic substrate for sudden infant death syndrome in the variant-positive infants.

Original language	English (US)
Pages (from-to)	e005859
Journal	Circulation. Arrhythmia and electrophysiology
Volume	11
Issue number	5
DOIs	https://doi.org/10.1161/CIRCEP.117.005859
State	Published - May 1 2018

Keywords

death, sudden
genetic testing
human genetics
ion channels
long QT syndrome
potassium channels
sudden infant death

ASJC Scopus subject areas

Cardiology and Cardiovascular Medicine
Physiology (medical)

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10.1161/CIRCEP.117.005859

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Smith, J. L., Tester, D. J., Hall, A. R., Burgess, D. E., Hsu, C. C., Elayi, S. C., Anderson, C. L., January, C. T., Luo, J. Z., Hartzel, D. N., Mirshahi, U. L., Murray, M. F., Mirshahi, T., Ackerman, M. J., & Delisle, B. P. (2018). Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel. Circulation. Arrhythmia and electrophysiology, 11(5), e005859. https://doi.org/10.1161/CIRCEP.117.005859

Smith, JL, Tester, DJ, Hall, AR, Burgess, DE, Hsu, CC, Elayi, SC, Anderson, CL, January, CT, Luo, JZ, Hartzel, DN, Mirshahi, UL, Murray, MF, Mirshahi, T, Ackerman, MJ & Delisle, BP 2018, 'Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel', Circulation. Arrhythmia and electrophysiology, vol. 11, no. 5, pp. e005859. https://doi.org/10.1161/CIRCEP.117.005859

@article{4e45acd6ec264096b3a326eaa30019e8,

title = "Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel",

abstract = "BACKGROUND: Heterologous functional validation studies of putative long-QT syndrome subtype 2-associated variants clarify their pathological potential and identify disease mechanism(s) for most variants studied. The purpose of this study is to clarify the pathological potential for rare nonsynonymous KCNH2 variants seemingly associated with sudden infant death syndrome. METHODS: Genetic testing of 292 sudden infant death syndrome cases identified 9 KCNH2 variants: E90K, R181Q, A190T, G294V, R791W, P967L, R1005W, R1047L, and Q1068R. Previous studies show R181Q-, P967L-, and R1047L-Kv11.1 channels function similar to wild-type Kv11.1 channels, whereas Q1068R-Kv11.1 channels accelerate inactivation gating. We studied the biochemical and biophysical properties for E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels expressed in human embryonic kidney 293 cells; examined the electronic health records of patients who were genotype positive for the sudden infant death syndrome-linked KCNH2 variants; and simulated their functional impact using computational models of the human ventricular action potential. RESULTS: Western blot and voltage-clamping analyses of cells expressing E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels demonstrated these variants express and generate peak Kv11.1 current levels similar to cells expressing wild-type-Kv11.1 channels, but R791W- and R1005W-Kv11.1 channels accelerated deactivation and activation gating, respectively. Electronic health records of patients with the sudden infant death syndrome-linked KCNH2 variants showed that the patients had median heart rate-corrected QT intervals <480 ms and none had been diagnosed with long-QT syndrome or experienced cardiac arrest. Simulating the impact of dysfunctional gating variants predicted that they have little impact on ventricular action potential duration. CONCLUSIONS: We conclude that these rare Kv11.1 missense variants are not long-QT syndrome subtype 2-causative variants and therefore do not represent the pathogenic substrate for sudden infant death syndrome in the variant-positive infants.",

keywords = "death, sudden, genetic testing, human genetics, ion channels, long QT syndrome, potassium channels, sudden infant death",

author = "Smith, {Jennifer L.} and Tester, {David J.} and Hall, {Allison R.} and Burgess, {Don E.} and Hsu, {Chun Chun} and Elayi, {Samy Claude} and Anderson, {Corey L.} and January, {Craig T.} and Luo, {Jonathan Z.} and Hartzel, {Dustin N.} and Mirshahi, {Uyenlinh L.} and Murray, {Michael F.} and Tooraj Mirshahi and Ackerman, {Michael J.} and Delisle, {Brian P.}",

note = "Publisher Copyright: {\textcopyright} 2018 American Heart Association, Inc.",

year = "2018",

month = may,

day = "1",

doi = "10.1161/CIRCEP.117.005859",

language = "English (US)",

volume = "11",

pages = "e005859",

journal = "Circulation. Arrhythmia and electrophysiology",

issn = "1941-3149",

publisher = "Lippincott Williams and Wilkins",

number = "5",

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TY - JOUR

T1 - Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel

AU - Smith, Jennifer L.

AU - Tester, David J.

AU - Hall, Allison R.

AU - Burgess, Don E.

AU - Hsu, Chun Chun

AU - Elayi, Samy Claude

AU - Anderson, Corey L.

AU - January, Craig T.

AU - Luo, Jonathan Z.

AU - Hartzel, Dustin N.

AU - Mirshahi, Uyenlinh L.

AU - Murray, Michael F.

AU - Mirshahi, Tooraj

AU - Ackerman, Michael J.

AU - Delisle, Brian P.

PY - 2018/5/1

Y1 - 2018/5/1

N2 - BACKGROUND: Heterologous functional validation studies of putative long-QT syndrome subtype 2-associated variants clarify their pathological potential and identify disease mechanism(s) for most variants studied. The purpose of this study is to clarify the pathological potential for rare nonsynonymous KCNH2 variants seemingly associated with sudden infant death syndrome. METHODS: Genetic testing of 292 sudden infant death syndrome cases identified 9 KCNH2 variants: E90K, R181Q, A190T, G294V, R791W, P967L, R1005W, R1047L, and Q1068R. Previous studies show R181Q-, P967L-, and R1047L-Kv11.1 channels function similar to wild-type Kv11.1 channels, whereas Q1068R-Kv11.1 channels accelerate inactivation gating. We studied the biochemical and biophysical properties for E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels expressed in human embryonic kidney 293 cells; examined the electronic health records of patients who were genotype positive for the sudden infant death syndrome-linked KCNH2 variants; and simulated their functional impact using computational models of the human ventricular action potential. RESULTS: Western blot and voltage-clamping analyses of cells expressing E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels demonstrated these variants express and generate peak Kv11.1 current levels similar to cells expressing wild-type-Kv11.1 channels, but R791W- and R1005W-Kv11.1 channels accelerated deactivation and activation gating, respectively. Electronic health records of patients with the sudden infant death syndrome-linked KCNH2 variants showed that the patients had median heart rate-corrected QT intervals <480 ms and none had been diagnosed with long-QT syndrome or experienced cardiac arrest. Simulating the impact of dysfunctional gating variants predicted that they have little impact on ventricular action potential duration. CONCLUSIONS: We conclude that these rare Kv11.1 missense variants are not long-QT syndrome subtype 2-causative variants and therefore do not represent the pathogenic substrate for sudden infant death syndrome in the variant-positive infants.

AB - BACKGROUND: Heterologous functional validation studies of putative long-QT syndrome subtype 2-associated variants clarify their pathological potential and identify disease mechanism(s) for most variants studied. The purpose of this study is to clarify the pathological potential for rare nonsynonymous KCNH2 variants seemingly associated with sudden infant death syndrome. METHODS: Genetic testing of 292 sudden infant death syndrome cases identified 9 KCNH2 variants: E90K, R181Q, A190T, G294V, R791W, P967L, R1005W, R1047L, and Q1068R. Previous studies show R181Q-, P967L-, and R1047L-Kv11.1 channels function similar to wild-type Kv11.1 channels, whereas Q1068R-Kv11.1 channels accelerate inactivation gating. We studied the biochemical and biophysical properties for E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels expressed in human embryonic kidney 293 cells; examined the electronic health records of patients who were genotype positive for the sudden infant death syndrome-linked KCNH2 variants; and simulated their functional impact using computational models of the human ventricular action potential. RESULTS: Western blot and voltage-clamping analyses of cells expressing E90K-, G294V-, R791W-, and R1005W-Kv11.1 channels demonstrated these variants express and generate peak Kv11.1 current levels similar to cells expressing wild-type-Kv11.1 channels, but R791W- and R1005W-Kv11.1 channels accelerated deactivation and activation gating, respectively. Electronic health records of patients with the sudden infant death syndrome-linked KCNH2 variants showed that the patients had median heart rate-corrected QT intervals <480 ms and none had been diagnosed with long-QT syndrome or experienced cardiac arrest. Simulating the impact of dysfunctional gating variants predicted that they have little impact on ventricular action potential duration. CONCLUSIONS: We conclude that these rare Kv11.1 missense variants are not long-QT syndrome subtype 2-causative variants and therefore do not represent the pathogenic substrate for sudden infant death syndrome in the variant-positive infants.

KW - death, sudden

KW - genetic testing

KW - human genetics

KW - ion channels

KW - long QT syndrome

KW - potassium channels

KW - sudden infant death

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Functional Invalidation of Putative Sudden Infant Death Syndrome-Associated Variants in the KCNH2-Encoded Kv11.1 Channel

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