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Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence

Whole-genome sequencing harbors unprecedented potential for characterization of individual and family genetic variation. Here, we develop a novel synthetic human reference sequence that is ethnically concordant and use it for the analysis of genomes from a nuclear family with history of familial thr...

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Autores principales: Dewey, Frederick E., Chen, Rong, Cordero, Sergio P., Ormond, Kelly E., Caleshu, Colleen, Karczewski, Konrad J., Whirl-Carrillo, Michelle, Wheeler, Matthew T., Dudley, Joel T., Byrnes, Jake K., Cornejo, Omar E., Knowles, Joshua W., Woon, Mark, Sangkuhl, Katrin, Gong, Li, Thorn, Caroline F., Hebert, Joan M., Capriotti, Emidio, David, Sean P., Pavlovic, Aleksandra, West, Anne, Thakuria, Joseph V., Ball, Madeleine P., Zaranek, Alexander W., Rehm, Heidi L., Church, George M., West, John S., Bustamante, Carlos D., Snyder, Michael, Altman, Russ B., Klein, Teri E., Butte, Atul J., Ashley, Euan A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3174201/
https://www.ncbi.nlm.nih.gov/pubmed/21935354
http://dx.doi.org/10.1371/journal.pgen.1002280
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author Dewey, Frederick E.
Chen, Rong
Cordero, Sergio P.
Ormond, Kelly E.
Caleshu, Colleen
Karczewski, Konrad J.
Whirl-Carrillo, Michelle
Wheeler, Matthew T.
Dudley, Joel T.
Byrnes, Jake K.
Cornejo, Omar E.
Knowles, Joshua W.
Woon, Mark
Sangkuhl, Katrin
Gong, Li
Thorn, Caroline F.
Hebert, Joan M.
Capriotti, Emidio
David, Sean P.
Pavlovic, Aleksandra
West, Anne
Thakuria, Joseph V.
Ball, Madeleine P.
Zaranek, Alexander W.
Rehm, Heidi L.
Church, George M.
West, John S.
Bustamante, Carlos D.
Snyder, Michael
Altman, Russ B.
Klein, Teri E.
Butte, Atul J.
Ashley, Euan A.
author_facet Dewey, Frederick E.
Chen, Rong
Cordero, Sergio P.
Ormond, Kelly E.
Caleshu, Colleen
Karczewski, Konrad J.
Whirl-Carrillo, Michelle
Wheeler, Matthew T.
Dudley, Joel T.
Byrnes, Jake K.
Cornejo, Omar E.
Knowles, Joshua W.
Woon, Mark
Sangkuhl, Katrin
Gong, Li
Thorn, Caroline F.
Hebert, Joan M.
Capriotti, Emidio
David, Sean P.
Pavlovic, Aleksandra
West, Anne
Thakuria, Joseph V.
Ball, Madeleine P.
Zaranek, Alexander W.
Rehm, Heidi L.
Church, George M.
West, John S.
Bustamante, Carlos D.
Snyder, Michael
Altman, Russ B.
Klein, Teri E.
Butte, Atul J.
Ashley, Euan A.
author_sort Dewey, Frederick E.
collection PubMed
description Whole-genome sequencing harbors unprecedented potential for characterization of individual and family genetic variation. Here, we develop a novel synthetic human reference sequence that is ethnically concordant and use it for the analysis of genomes from a nuclear family with history of familial thrombophilia. We demonstrate that the use of the major allele reference sequence results in improved genotype accuracy for disease-associated variant loci. We infer recombination sites to the lowest median resolution demonstrated to date (<1,000 base pairs). We use family inheritance state analysis to control sequencing error and inform family-wide haplotype phasing, allowing quantification of genome-wide compound heterozygosity. We develop a sequence-based methodology for Human Leukocyte Antigen typing that contributes to disease risk prediction. Finally, we advance methods for analysis of disease and pharmacogenomic risk across the coding and non-coding genome that incorporate phased variant data. We show these methods are capable of identifying multigenic risk for inherited thrombophilia and informing the appropriate pharmacological therapy. These ethnicity-specific, family-based approaches to interpretation of genetic variation are emblematic of the next generation of genetic risk assessment using whole-genome sequencing.
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spelling pubmed-31742012011-09-20 Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence Dewey, Frederick E. Chen, Rong Cordero, Sergio P. Ormond, Kelly E. Caleshu, Colleen Karczewski, Konrad J. Whirl-Carrillo, Michelle Wheeler, Matthew T. Dudley, Joel T. Byrnes, Jake K. Cornejo, Omar E. Knowles, Joshua W. Woon, Mark Sangkuhl, Katrin Gong, Li Thorn, Caroline F. Hebert, Joan M. Capriotti, Emidio David, Sean P. Pavlovic, Aleksandra West, Anne Thakuria, Joseph V. Ball, Madeleine P. Zaranek, Alexander W. Rehm, Heidi L. Church, George M. West, John S. Bustamante, Carlos D. Snyder, Michael Altman, Russ B. Klein, Teri E. Butte, Atul J. Ashley, Euan A. PLoS Genet Research Article Whole-genome sequencing harbors unprecedented potential for characterization of individual and family genetic variation. Here, we develop a novel synthetic human reference sequence that is ethnically concordant and use it for the analysis of genomes from a nuclear family with history of familial thrombophilia. We demonstrate that the use of the major allele reference sequence results in improved genotype accuracy for disease-associated variant loci. We infer recombination sites to the lowest median resolution demonstrated to date (<1,000 base pairs). We use family inheritance state analysis to control sequencing error and inform family-wide haplotype phasing, allowing quantification of genome-wide compound heterozygosity. We develop a sequence-based methodology for Human Leukocyte Antigen typing that contributes to disease risk prediction. Finally, we advance methods for analysis of disease and pharmacogenomic risk across the coding and non-coding genome that incorporate phased variant data. We show these methods are capable of identifying multigenic risk for inherited thrombophilia and informing the appropriate pharmacological therapy. These ethnicity-specific, family-based approaches to interpretation of genetic variation are emblematic of the next generation of genetic risk assessment using whole-genome sequencing. Public Library of Science 2011-09-15 /pmc/articles/PMC3174201/ /pubmed/21935354 http://dx.doi.org/10.1371/journal.pgen.1002280 Text en Dewey et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Dewey, Frederick E.
Chen, Rong
Cordero, Sergio P.
Ormond, Kelly E.
Caleshu, Colleen
Karczewski, Konrad J.
Whirl-Carrillo, Michelle
Wheeler, Matthew T.
Dudley, Joel T.
Byrnes, Jake K.
Cornejo, Omar E.
Knowles, Joshua W.
Woon, Mark
Sangkuhl, Katrin
Gong, Li
Thorn, Caroline F.
Hebert, Joan M.
Capriotti, Emidio
David, Sean P.
Pavlovic, Aleksandra
West, Anne
Thakuria, Joseph V.
Ball, Madeleine P.
Zaranek, Alexander W.
Rehm, Heidi L.
Church, George M.
West, John S.
Bustamante, Carlos D.
Snyder, Michael
Altman, Russ B.
Klein, Teri E.
Butte, Atul J.
Ashley, Euan A.
Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title_full Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title_fullStr Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title_full_unstemmed Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title_short Phased Whole-Genome Genetic Risk in a Family Quartet Using a Major Allele Reference Sequence
title_sort phased whole-genome genetic risk in a family quartet using a major allele reference sequence
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3174201/
https://www.ncbi.nlm.nih.gov/pubmed/21935354
http://dx.doi.org/10.1371/journal.pgen.1002280
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