Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care

An accurate diagnosis is an integral component of patient care for children with rare genetic disease. Recent advances in sequencing, in particular whole‐exome sequencing (WES), are identifying the genetic basis of disease for 25–40% of patients. The diagnostic rate is probably influenced by when in...

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Autores principales: Sawyer, S.L., Hartley, T., Dyment, D.A., Beaulieu, C.L., Schwartzentruber, J., Smith, A., Bedford, H.M., Bernard, G., Bernier, F.P., Brais, B., Bulman, D.E., Warman Chardon, J., Chitayat, D., Deladoëy, J., Fernandez, B.A., Frosk, P., Geraghty, M.T., Gerull, B., Gibson, W., Gow, R.M., Graham, G.E., Green, J.S., Heon, E., Horvath, G., Innes, A.M., Jabado, N., Kim, R.H., Koenekoop, R.K., Khan, A., Lehmann, O.J., Mendoza‐Londono, R., Michaud, J.L., Nikkel, S.M., Penney, L.S., Polychronakos, C., Richer, J., Rouleau, G.A., Samuels, M.E., Siu, V.M., Suchowersky, O., Tarnopolsky, M.A., Yoon, G., Zahir, F.R., Majewski, J., Boycott, K.M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2015
Materias:
Reviews
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5053223/
https://www.ncbi.nlm.nih.gov/pubmed/26283276
http://dx.doi.org/10.1111/cge.12654
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author Sawyer, S.L.
Hartley, T.
Dyment, D.A.
Beaulieu, C.L.
Schwartzentruber, J.
Smith, A.
Bedford, H.M.
Bernard, G.
Bernier, F.P.
Brais, B.
Bulman, D.E.
Warman Chardon, J.
Chitayat, D.
Deladoëy, J.
Fernandez, B.A.
Frosk, P.
Geraghty, M.T.
Gerull, B.
Gibson, W.
Gow, R.M.
Graham, G.E.
Green, J.S.
Heon, E.
Horvath, G.
Innes, A.M.
Jabado, N.
Kim, R.H.
Koenekoop, R.K.
Khan, A.
Lehmann, O.J.
Mendoza‐Londono, R.
Michaud, J.L.
Nikkel, S.M.
Penney, L.S.
Polychronakos, C.
Richer, J.
Rouleau, G.A.
Samuels, M.E.
Siu, V.M.
Suchowersky, O.
Tarnopolsky, M.A.
Yoon, G.
Zahir, F.R.
Majewski, J.
Boycott, K.M.
author_facet Sawyer, S.L.
Hartley, T.
Dyment, D.A.
Beaulieu, C.L.
Schwartzentruber, J.
Smith, A.
Bedford, H.M.
Bernard, G.
Bernier, F.P.
Brais, B.
Bulman, D.E.
Warman Chardon, J.
Chitayat, D.
Deladoëy, J.
Fernandez, B.A.
Frosk, P.
Geraghty, M.T.
Gerull, B.
Gibson, W.
Gow, R.M.
Graham, G.E.
Green, J.S.
Heon, E.
Horvath, G.
Innes, A.M.
Jabado, N.
Kim, R.H.
Koenekoop, R.K.
Khan, A.
Lehmann, O.J.
Mendoza‐Londono, R.
Michaud, J.L.
Nikkel, S.M.
Penney, L.S.
Polychronakos, C.
Richer, J.
Rouleau, G.A.
Samuels, M.E.
Siu, V.M.
Suchowersky, O.
Tarnopolsky, M.A.
Yoon, G.
Zahir, F.R.
Majewski, J.
Boycott, K.M.
author_sort Sawyer, S.L.
collection PubMed
description An accurate diagnosis is an integral component of patient care for children with rare genetic disease. Recent advances in sequencing, in particular whole‐exome sequencing (WES), are identifying the genetic basis of disease for 25–40% of patients. The diagnostic rate is probably influenced by when in the diagnostic process WES is used. The Finding Of Rare Disease GEnes (FORGE) Canada project was a nation‐wide effort to identify mutations for childhood‐onset disorders using WES. Most children enrolled in the FORGE project were toward the end of the diagnostic odyssey. The two primary outcomes of FORGE were novel gene discovery and the identification of mutations in genes known to cause disease. In the latter instance, WES identified mutations in known disease genes for 105 of 362 families studied (29%), thereby informing the impact of WES in the setting of the diagnostic odyssey. Our analysis of this dataset showed that these known disease genes were not identified prior to WES enrollment for two key reasons: genetic heterogeneity associated with a clinical diagnosis and atypical presentation of known, clinically recognized diseases. What is becoming increasingly clear is that WES will be paradigm altering for patients and families with rare genetic diseases.
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spelling pubmed-50532232016-10-19 Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care Sawyer, S.L. Hartley, T. Dyment, D.A. Beaulieu, C.L. Schwartzentruber, J. Smith, A. Bedford, H.M. Bernard, G. Bernier, F.P. Brais, B. Bulman, D.E. Warman Chardon, J. Chitayat, D. Deladoëy, J. Fernandez, B.A. Frosk, P. Geraghty, M.T. Gerull, B. Gibson, W. Gow, R.M. Graham, G.E. Green, J.S. Heon, E. Horvath, G. Innes, A.M. Jabado, N. Kim, R.H. Koenekoop, R.K. Khan, A. Lehmann, O.J. Mendoza‐Londono, R. Michaud, J.L. Nikkel, S.M. Penney, L.S. Polychronakos, C. Richer, J. Rouleau, G.A. Samuels, M.E. Siu, V.M. Suchowersky, O. Tarnopolsky, M.A. Yoon, G. Zahir, F.R. Majewski, J. Boycott, K.M. Clin Genet Reviews An accurate diagnosis is an integral component of patient care for children with rare genetic disease. Recent advances in sequencing, in particular whole‐exome sequencing (WES), are identifying the genetic basis of disease for 25–40% of patients. The diagnostic rate is probably influenced by when in the diagnostic process WES is used. The Finding Of Rare Disease GEnes (FORGE) Canada project was a nation‐wide effort to identify mutations for childhood‐onset disorders using WES. Most children enrolled in the FORGE project were toward the end of the diagnostic odyssey. The two primary outcomes of FORGE were novel gene discovery and the identification of mutations in genes known to cause disease. In the latter instance, WES identified mutations in known disease genes for 105 of 362 families studied (29%), thereby informing the impact of WES in the setting of the diagnostic odyssey. Our analysis of this dataset showed that these known disease genes were not identified prior to WES enrollment for two key reasons: genetic heterogeneity associated with a clinical diagnosis and atypical presentation of known, clinically recognized diseases. What is becoming increasingly clear is that WES will be paradigm altering for patients and families with rare genetic diseases. Blackwell Publishing Ltd 2015-09-22 2016-03 /pmc/articles/PMC5053223/ /pubmed/26283276 http://dx.doi.org/10.1111/cge.12654 Text en © 2015 The Authors. Clinical Genetics published by John Wiley & Sons A/S. Published by John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution‐NonCommercial‐NoDerivs (http://creativecommons.org/licenses/by-nc-nd/4.0/) License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non‐commercial and no modifications or adaptations are made.
spellingShingle Reviews
Sawyer, S.L.
Hartley, T.
Dyment, D.A.
Beaulieu, C.L.
Schwartzentruber, J.
Smith, A.
Bedford, H.M.
Bernard, G.
Bernier, F.P.
Brais, B.
Bulman, D.E.
Warman Chardon, J.
Chitayat, D.
Deladoëy, J.
Fernandez, B.A.
Frosk, P.
Geraghty, M.T.
Gerull, B.
Gibson, W.
Gow, R.M.
Graham, G.E.
Green, J.S.
Heon, E.
Horvath, G.
Innes, A.M.
Jabado, N.
Kim, R.H.
Koenekoop, R.K.
Khan, A.
Lehmann, O.J.
Mendoza‐Londono, R.
Michaud, J.L.
Nikkel, S.M.
Penney, L.S.
Polychronakos, C.
Richer, J.
Rouleau, G.A.
Samuels, M.E.
Siu, V.M.
Suchowersky, O.
Tarnopolsky, M.A.
Yoon, G.
Zahir, F.R.
Majewski, J.
Boycott, K.M.
Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title_full Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title_fullStr Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title_full_unstemmed Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title_short Utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
title_sort utility of whole‐exome sequencing for those near the end of the diagnostic odyssey: time to address gaps in care
topic Reviews
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5053223/
https://www.ncbi.nlm.nih.gov/pubmed/26283276
http://dx.doi.org/10.1111/cge.12654
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