Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data

Charlotte Hartig Andreasen; Lena Refsgaard; Jonas B Nielsen; Ahmad Sajadieh; Bo G Winkel; Jacob Tfelt-Hansen; Stig Haunsø; Anders G Holst; Jesper H Svendsen; Morten S Olesen

doi:10.1016/j.cjca.2012.12.002

Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data

Charlotte Hartig Andreasen, Lena Refsgaard, Jonas B Nielsen, Ahmad Sajadieh, Bo G Winkel, Jacob Tfelt-Hansen, Stig Haunsø, Anders G Holst, Jesper H Svendsen, Morten S Olesen

44 Citations (Scopus)

Abstract

Background: Sudden infant death syndrome (SIDS) is the leading cause of death in the first 6 months after birth in the industrialized world. The genetic contribution to SIDS has been investigated intensively and to date, 14 cardiac channelopathy genes have been associated with SIDS. Newly published data from National Heart, Lung, and Blood Institute Grand Opportunity (NHLBI GO) Exome Sequencing Project (ESP) provided important knowledge on genetic variation in the background population. Our aim was to identify all variants previously associated with SIDS in ESP to improve the discrimination between plausible disease-causing mutations and variants most likely to be false-positive. Methods: The PubMed database was searched to identify SIDS-associated channelopathy variants and the prevalence of these in the ESP population (6500 individuals) were obtained. In silico prediction tools were applied to variants present in ESP and 6 SIDS-associated variants (CAV3 p.C72W, p.T78M; KCNH2 p.R148W, and SCN5A p.S216L, p.V1951L, p.F2004L) were genotyped in our own control population. Results: Nineteen different missense variants previously associated with SIDS were identified in ESP affecting 225 of 6424 alleles. This corresponds to 1:29 individuals in the ESP population being carriers of a SIDS-associated variant. Genotyping of 6SIDS-associated variants in our own controls revealed frequencies comparable with those found in ESP. Conclusions: A very high prevalence of previously SIDS-associated variants was identified in exome data from population studies. Our findings indicate that the suggested disease-causing role of some of these variants is questionable. A cautious interpretation of these variants must be made when found in SIDS victims.

Original language	English
Journal	Canadian Journal of Cardiology
Volume	29
Issue number	9
Pages (from-to)	1104-1109
Number of pages	6
ISSN	0828-282X
DOIs	https://doi.org/10.1016/j.cjca.2012.12.002
Publication status	Published - Sept 2013

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Andreasen, C. H., Refsgaard, L., Nielsen, J. B., Sajadieh, A., Winkel, B. G., Tfelt-Hansen, J., Haunsø, S., Holst, A. G., Svendsen, J. H., & Olesen, M. S. (2013). Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data. Canadian Journal of Cardiology, 29(9), 1104-1109. https://doi.org/10.1016/j.cjca.2012.12.002

Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data. / Andreasen, Charlotte Hartig; Refsgaard, Lena; Nielsen, Jonas B et al.

In: Canadian Journal of Cardiology, Vol. 29, No. 9, 09.2013, p. 1104-1109.

Research output: Contribution to journal › Journal article › Research › peer-review

Andreasen, CH, Refsgaard, L, Nielsen, JB, Sajadieh, A, Winkel, BG, Tfelt-Hansen, J, Haunsø, S, Holst, AG, Svendsen, JH & Olesen, MS 2013, 'Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data', Canadian Journal of Cardiology, vol. 29, no. 9, pp. 1104-1109. https://doi.org/10.1016/j.cjca.2012.12.002

@article{b3bd78f6c0a94b7a8c8a11718e73f995,

title = "Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data",

abstract = "Background: Sudden infant death syndrome (SIDS) is the leading cause of death in the first 6 months after birth in the industrialized world. The genetic contribution to SIDS has been investigated intensively and to date, 14 cardiac channelopathy genes have been associated with SIDS. Newly published data from National Heart, Lung, and Blood Institute Grand Opportunity (NHLBI GO) Exome Sequencing Project (ESP) provided important knowledge on genetic variation in the background population. Our aim was to identify all variants previously associated with SIDS in ESP to improve the discrimination between plausible disease-causing mutations and variants most likely to be false-positive. Methods: The PubMed database was searched to identify SIDS-associated channelopathy variants and the prevalence of these in the ESP population (6500 individuals) were obtained. In silico prediction tools were applied to variants present in ESP and 6 SIDS-associated variants (CAV3 p.C72W, p.T78M; KCNH2 p.R148W, and SCN5A p.S216L, p.V1951L, p.F2004L) were genotyped in our own control population. Results: Nineteen different missense variants previously associated with SIDS were identified in ESP affecting 225 of 6424 alleles. This corresponds to 1:29 individuals in the ESP population being carriers of a SIDS-associated variant. Genotyping of 6SIDS-associated variants in our own controls revealed frequencies comparable with those found in ESP. Conclusions: A very high prevalence of previously SIDS-associated variants was identified in exome data from population studies. Our findings indicate that the suggested disease-causing role of some of these variants is questionable. A cautious interpretation of these variants must be made when found in SIDS victims.",

author = "Andreasen, {Charlotte Hartig} and Lena Refsgaard and Nielsen, {Jonas B} and Ahmad Sajadieh and Winkel, {Bo G} and Jacob Tfelt-Hansen and Stig Hauns{\o} and Holst, {Anders G} and Svendsen, {Jesper H} and Olesen, {Morten S}",

year = "2013",

month = sep,

doi = "10.1016/j.cjca.2012.12.002",

language = "English",

volume = "29",

pages = "1104--1109",

journal = "Canadian Journal of Cardiology",

issn = "0828-282X",

publisher = "Elsevier",

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T1 - Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data

AU - Andreasen, Charlotte Hartig

AU - Refsgaard, Lena

AU - Nielsen, Jonas B

AU - Sajadieh, Ahmad

AU - Winkel, Bo G

AU - Tfelt-Hansen, Jacob

AU - Haunsø, Stig

AU - Holst, Anders G

AU - Svendsen, Jesper H

AU - Olesen, Morten S

PY - 2013/9

Y1 - 2013/9

N2 - Background: Sudden infant death syndrome (SIDS) is the leading cause of death in the first 6 months after birth in the industrialized world. The genetic contribution to SIDS has been investigated intensively and to date, 14 cardiac channelopathy genes have been associated with SIDS. Newly published data from National Heart, Lung, and Blood Institute Grand Opportunity (NHLBI GO) Exome Sequencing Project (ESP) provided important knowledge on genetic variation in the background population. Our aim was to identify all variants previously associated with SIDS in ESP to improve the discrimination between plausible disease-causing mutations and variants most likely to be false-positive. Methods: The PubMed database was searched to identify SIDS-associated channelopathy variants and the prevalence of these in the ESP population (6500 individuals) were obtained. In silico prediction tools were applied to variants present in ESP and 6 SIDS-associated variants (CAV3 p.C72W, p.T78M; KCNH2 p.R148W, and SCN5A p.S216L, p.V1951L, p.F2004L) were genotyped in our own control population. Results: Nineteen different missense variants previously associated with SIDS were identified in ESP affecting 225 of 6424 alleles. This corresponds to 1:29 individuals in the ESP population being carriers of a SIDS-associated variant. Genotyping of 6SIDS-associated variants in our own controls revealed frequencies comparable with those found in ESP. Conclusions: A very high prevalence of previously SIDS-associated variants was identified in exome data from population studies. Our findings indicate that the suggested disease-causing role of some of these variants is questionable. A cautious interpretation of these variants must be made when found in SIDS victims.

AB - Background: Sudden infant death syndrome (SIDS) is the leading cause of death in the first 6 months after birth in the industrialized world. The genetic contribution to SIDS has been investigated intensively and to date, 14 cardiac channelopathy genes have been associated with SIDS. Newly published data from National Heart, Lung, and Blood Institute Grand Opportunity (NHLBI GO) Exome Sequencing Project (ESP) provided important knowledge on genetic variation in the background population. Our aim was to identify all variants previously associated with SIDS in ESP to improve the discrimination between plausible disease-causing mutations and variants most likely to be false-positive. Methods: The PubMed database was searched to identify SIDS-associated channelopathy variants and the prevalence of these in the ESP population (6500 individuals) were obtained. In silico prediction tools were applied to variants present in ESP and 6 SIDS-associated variants (CAV3 p.C72W, p.T78M; KCNH2 p.R148W, and SCN5A p.S216L, p.V1951L, p.F2004L) were genotyped in our own control population. Results: Nineteen different missense variants previously associated with SIDS were identified in ESP affecting 225 of 6424 alleles. This corresponds to 1:29 individuals in the ESP population being carriers of a SIDS-associated variant. Genotyping of 6SIDS-associated variants in our own controls revealed frequencies comparable with those found in ESP. Conclusions: A very high prevalence of previously SIDS-associated variants was identified in exome data from population studies. Our findings indicate that the suggested disease-causing role of some of these variants is questionable. A cautious interpretation of these variants must be made when found in SIDS victims.

U2 - 10.1016/j.cjca.2012.12.002

DO - 10.1016/j.cjca.2012.12.002

M3 - Journal article

C2 - 23465283

SN - 0828-282X

VL - 29

SP - 1104

EP - 1109

JO - Canadian Journal of Cardiology

JF - Canadian Journal of Cardiology

IS - 9

ER -

Mutations in Genes Encoding Cardiac Ion Channels Previously Associated With Sudden Infant Death Syndrome (SIDS) Are Present With High Frequency in New Exome Data

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