Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death

BACKGROUND: Conditions associated with sudden cardiac arrest/death (SCA/D) in youth often have a genetic etiology. While SCA/D is uncommon, a pro-active family screening approach may identify these inherited structural and electrical abnormalities prior to symptomatic events and allow appropriate su...

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Autores principales: Li, Mindy H., Abrudan, Jenica L., Dulik, Matthew C., Sasson, Ariella, Brunton, Joshua, Jayaraman, Vijayakumar, Dugan, Noreen, Haley, Danielle, Rajagopalan, Ramakrishnan, Biswas, Sawona, Sarmady, Mahdi, DeChene, Elizabeth T., Deardorff, Matthew A., Wilkens, Alisha, Noon, Sarah E., Scarano, Maria I., Santani, Avni B., White, Peter S., Pennington, Jeffrey, Conlin, Laura K., Spinner, Nancy B., Krantz, Ian D., Vetter, Victoria L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Primary Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4506570/
https://www.ncbi.nlm.nih.gov/pubmed/26187847
http://dx.doi.org/10.1186/s40246-015-0038-y
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author Li, Mindy H.
Abrudan, Jenica L.
Dulik, Matthew C.
Sasson, Ariella
Brunton, Joshua
Jayaraman, Vijayakumar
Dugan, Noreen
Haley, Danielle
Rajagopalan, Ramakrishnan
Biswas, Sawona
Sarmady, Mahdi
DeChene, Elizabeth T.
Deardorff, Matthew A.
Wilkens, Alisha
Noon, Sarah E.
Scarano, Maria I.
Santani, Avni B.
White, Peter S.
Pennington, Jeffrey
Conlin, Laura K.
Spinner, Nancy B.
Krantz, Ian D.
Vetter, Victoria L.
author_facet Li, Mindy H.
Abrudan, Jenica L.
Dulik, Matthew C.
Sasson, Ariella
Brunton, Joshua
Jayaraman, Vijayakumar
Dugan, Noreen
Haley, Danielle
Rajagopalan, Ramakrishnan
Biswas, Sawona
Sarmady, Mahdi
DeChene, Elizabeth T.
Deardorff, Matthew A.
Wilkens, Alisha
Noon, Sarah E.
Scarano, Maria I.
Santani, Avni B.
White, Peter S.
Pennington, Jeffrey
Conlin, Laura K.
Spinner, Nancy B.
Krantz, Ian D.
Vetter, Victoria L.
author_sort Li, Mindy H.
collection PubMed
description BACKGROUND: Conditions associated with sudden cardiac arrest/death (SCA/D) in youth often have a genetic etiology. While SCA/D is uncommon, a pro-active family screening approach may identify these inherited structural and electrical abnormalities prior to symptomatic events and allow appropriate surveillance and treatment. This study investigated the diagnostic utility of exome sequencing (ES) by evaluating the capture and coverage of genes related to SCA/D. METHODS: Samples from 102 individuals (13 with known molecular etiologies for SCA/D, 30 individuals without known molecular etiologies for SCA/D and 59 with other conditions) were analyzed following exome capture and sequencing at an average read depth of 100X. Reads were mapped to human genome GRCh37 using Novoalign, and post-processing and analysis was done using Picard and GATK. A total of 103 genes (2,190 exons) related to SCA/D were used as a primary filter. An additional 100 random variants within the targeted genes associated with SCA/D were also selected and evaluated for depth of sequencing and coverage. Although the primary objective was to evaluate the adequacy of depth of sequencing and coverage of targeted SCA/D genes and not for primary diagnosis, all patients who had SCA/D (known or unknown molecular etiologies) were evaluated with the project’s variant analysis pipeline to determine if the molecular etiologies could be successfully identified. RESULTS: The majority of exons (97.6 %) were captured and fully covered on average at minimum of 20x sequencing depth. The proportion of unique genomic positions reported within poorly covered exons remained small (4 %). Exonic regions with less coverage reflect the need to enrich these areas to improve coverage. Despite limitations in coverage, we identified 100 % of cases with a prior known molecular etiology for SCA/D, and analysis of an additional 30 individuals with SCA/D but no known molecular etiology revealed a diagnostic answer in 5/30 (17 %). We also demonstrated 95 % of 100 randomly selected reported variants within our targeted genes would have been picked up on ES based on our coverage analysis. CONCLUSIONS: ES is a helpful clinical diagnostic tool for SCA/D given its potential to successfully identify a molecular diagnosis, but clinicians should be aware of limitations of available platforms from technical and diagnostic perspectives. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s40246-015-0038-y) contains supplementary material, which is available to authorized users.
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spelling pubmed-45065702015-07-19 Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death Li, Mindy H. Abrudan, Jenica L. Dulik, Matthew C. Sasson, Ariella Brunton, Joshua Jayaraman, Vijayakumar Dugan, Noreen Haley, Danielle Rajagopalan, Ramakrishnan Biswas, Sawona Sarmady, Mahdi DeChene, Elizabeth T. Deardorff, Matthew A. Wilkens, Alisha Noon, Sarah E. Scarano, Maria I. Santani, Avni B. White, Peter S. Pennington, Jeffrey Conlin, Laura K. Spinner, Nancy B. Krantz, Ian D. Vetter, Victoria L. Hum Genomics Primary Research BACKGROUND: Conditions associated with sudden cardiac arrest/death (SCA/D) in youth often have a genetic etiology. While SCA/D is uncommon, a pro-active family screening approach may identify these inherited structural and electrical abnormalities prior to symptomatic events and allow appropriate surveillance and treatment. This study investigated the diagnostic utility of exome sequencing (ES) by evaluating the capture and coverage of genes related to SCA/D. METHODS: Samples from 102 individuals (13 with known molecular etiologies for SCA/D, 30 individuals without known molecular etiologies for SCA/D and 59 with other conditions) were analyzed following exome capture and sequencing at an average read depth of 100X. Reads were mapped to human genome GRCh37 using Novoalign, and post-processing and analysis was done using Picard and GATK. A total of 103 genes (2,190 exons) related to SCA/D were used as a primary filter. An additional 100 random variants within the targeted genes associated with SCA/D were also selected and evaluated for depth of sequencing and coverage. Although the primary objective was to evaluate the adequacy of depth of sequencing and coverage of targeted SCA/D genes and not for primary diagnosis, all patients who had SCA/D (known or unknown molecular etiologies) were evaluated with the project’s variant analysis pipeline to determine if the molecular etiologies could be successfully identified. RESULTS: The majority of exons (97.6 %) were captured and fully covered on average at minimum of 20x sequencing depth. The proportion of unique genomic positions reported within poorly covered exons remained small (4 %). Exonic regions with less coverage reflect the need to enrich these areas to improve coverage. Despite limitations in coverage, we identified 100 % of cases with a prior known molecular etiology for SCA/D, and analysis of an additional 30 individuals with SCA/D but no known molecular etiology revealed a diagnostic answer in 5/30 (17 %). We also demonstrated 95 % of 100 randomly selected reported variants within our targeted genes would have been picked up on ES based on our coverage analysis. CONCLUSIONS: ES is a helpful clinical diagnostic tool for SCA/D given its potential to successfully identify a molecular diagnosis, but clinicians should be aware of limitations of available platforms from technical and diagnostic perspectives. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s40246-015-0038-y) contains supplementary material, which is available to authorized users. BioMed Central 2015-07-19 /pmc/articles/PMC4506570/ /pubmed/26187847 http://dx.doi.org/10.1186/s40246-015-0038-y Text en © Li et al. 2015 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly credited. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Primary Research
Li, Mindy H.
Abrudan, Jenica L.
Dulik, Matthew C.
Sasson, Ariella
Brunton, Joshua
Jayaraman, Vijayakumar
Dugan, Noreen
Haley, Danielle
Rajagopalan, Ramakrishnan
Biswas, Sawona
Sarmady, Mahdi
DeChene, Elizabeth T.
Deardorff, Matthew A.
Wilkens, Alisha
Noon, Sarah E.
Scarano, Maria I.
Santani, Avni B.
White, Peter S.
Pennington, Jeffrey
Conlin, Laura K.
Spinner, Nancy B.
Krantz, Ian D.
Vetter, Victoria L.
Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title_full Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title_fullStr Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title_full_unstemmed Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title_short Utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
title_sort utility and limitations of exome sequencing as a genetic diagnostic tool for conditions associated with pediatric sudden cardiac arrest/sudden cardiac death
topic Primary Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4506570/
https://www.ncbi.nlm.nih.gov/pubmed/26187847
http://dx.doi.org/10.1186/s40246-015-0038-y
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