Increased diagnostic and new genes identification outcome using research reanalysis of singleton exome sequencing

In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established human-disease genes. The diagnostic yield of cES in intellectual disability and/or multiple congenital anomalies (ID/MCA) is currently about 30%. Though...

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Published in	European journal of human genetics : EJHG Vol. 27; no. 10; pp. 1519 - 1531
Main Authors	Bruel, Ange-Line, Nambot, Sophie, Quéré, Virginie, Vitobello, Antonio, Thevenon, Julien, Assoum, Mirna, Moutton, Sébastien, Houcinat, Nada, Lehalle, Daphné, Jean-Marçais, Nolwenn, Chevarin, Martin, Jouan, Thibaud, Poë, Charlotte, Callier, Patrick, Tisserand, Emilie, Philippe, Christophe, Them, Frédéric Tran Mau, Duffourd, Yannis, Faivre, Laurence, Thauvin-Robinet, Christel
Format	Journal Article
Language	English
Published	Cham Springer International Publishing 01.10.2019 Nature Publishing Group
Subjects	45/23 631/208/514/1948 631/208/514/2254 Adolescent Bioinformatics Biomedical and Life Sciences Biomedicine Child Child, Preschool Computational Biology - methods Congenital defects Cytogenetics Disease Female Gene Expression Genetic Association Studies Genetic Predisposition to Disease Genetics Genomics Genomics - methods Human Genetics Human health and pathology Humans Intellectual disabilities Life Sciences Male Molecular Diagnostic Techniques Phenotypes Polymorphism, Single Nucleotide Rare diseases Sequence Analysis, DNA Whole Exome Sequencing - methods Whole genome sequencing Genetics Clinical Exome Sequencing (cES) Congenitals anomalies DNA Sequencing Next Generation Sequencing
Online Access	Get full text
ISSN	1018-4813 1476-5438 1476-5438
DOI	10.1038/s41431-019-0442-1

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Abstract	In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established human-disease genes. The diagnostic yield of cES in intellectual disability and/or multiple congenital anomalies (ID/MCA) is currently about 30%. Though the results may seem acceptable for rare diseases, they mean that 70% of affected individuals remain genetically undiagnosed. Further analysis extended to all mutated genes in a research environment is a valuable strategy for improving diagnostic yields. This study presents the results of systematic research reanalysis of negative cES in a cohort of 313 individuals with ID/MCA. We identified 17 new genes not related to human disease, implicated 22 non-OMIM disease-causing genes recently or previously rarely related to disease, and described 1 new phenotype associated with a known gene. Twenty-six candidate genes were identified and are waiting for future recurrence. Overall, we diagnose 15% of the individuals with initial negative cES, increasing the diagnostic yield from 30% to more than 40% (or 46% if strong candidate genes are considered). This study demonstrates the power of such extended research reanalysis to increase scientific knowledge of rare diseases. These novel findings can then be applied in the field of diagnostics.
AbstractList	In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established human-disease genes. The diagnostic yield of cES in intellectual disability and/or multiple congenital anomalies (ID/MCA) is currently about 30%. Though the results may seem acceptable for rare diseases, they mean that 70% of affected individuals remain genetically undiagnosed. Further analysis extended to all mutated genes in a research environment is a valuable strategy for improving diagnostic yields. This study presents the results of systematic research reanalysis of negative cES in a cohort of 313 individuals with ID/MCA. We identified 17 new genes not related to human disease, implicated 22 non-OMIM disease-causing genes recently or previously rarely related to disease, and described 1 new phenotype associated with a known gene. Twenty-six candidate genes were identified and are waiting for future recurrence. Overall, we diagnose 15% of the individuals with initial negative cES, increasing the diagnostic yield from 30% to more than 40% (or 46% if strong candidate genes are considered). This study demonstrates the power of such extended research reanalysis to increase scientific knowledge of rare diseases. These novel findings can then be applied in the field of diagnostics. In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established human-disease genes. The diagnostic yield of cES in intellectual disability and/or multiple congenital anomalies (ID/MCA) is currently about 30%. Though the results may seem acceptable for rare diseases, they mean that 70% of affected individuals remain genetically undiagnosed. Further analysis extended to all mutated genes in a research environment is a valuable strategy for improving diagnostic yields. This study presents the results of systematic research reanalysis of negative cES in a cohort of 313 individuals with ID/MCA. We identified 17 new genes not related to human disease, implicated 22 non-OMIM disease-causing genes recently or previously rarely related to disease, and described 1 new phenotype associated with a known gene. Twenty-six candidate genes were identified and are waiting for future recurrence. Overall, we diagnose 15% of the individuals with initial negative cES, increasing the diagnostic yield from 30% to more than 40% (or 46% if strong candidate genes are considered). This study demonstrates the power of such extended research reanalysis to increase scientific knowledge of rare diseases. These novel findings can then be applied in the field of diagnostics.In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established human-disease genes. The diagnostic yield of cES in intellectual disability and/or multiple congenital anomalies (ID/MCA) is currently about 30%. Though the results may seem acceptable for rare diseases, they mean that 70% of affected individuals remain genetically undiagnosed. Further analysis extended to all mutated genes in a research environment is a valuable strategy for improving diagnostic yields. This study presents the results of systematic research reanalysis of negative cES in a cohort of 313 individuals with ID/MCA. We identified 17 new genes not related to human disease, implicated 22 non-OMIM disease-causing genes recently or previously rarely related to disease, and described 1 new phenotype associated with a known gene. Twenty-six candidate genes were identified and are waiting for future recurrence. Overall, we diagnose 15% of the individuals with initial negative cES, increasing the diagnostic yield from 30% to more than 40% (or 46% if strong candidate genes are considered). This study demonstrates the power of such extended research reanalysis to increase scientific knowledge of rare diseases. These novel findings can then be applied in the field of diagnostics.
Author	Nambot, Sophie Jean-Marçais, Nolwenn Lehalle, Daphné Moutton, Sébastien Philippe, Christophe Jouan, Thibaud Assoum, Mirna Quéré, Virginie Houcinat, Nada Vitobello, Antonio Chevarin, Martin Poë, Charlotte Faivre, Laurence Duffourd, Yannis Thevenon, Julien Thauvin-Robinet, Christel Callier, Patrick Them, Frédéric Tran Mau Tisserand, Emilie Bruel, Ange-Line
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Copyright	The Author(s), under exclusive licence to European Society of Human Genetics 2019 Copyright Nature Publishing Group Oct 2019 Distributed under a Creative Commons Attribution 4.0 International License
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Snippet	In clinical exome sequencing (cES), the American College of Medical Genetics and Genomics recommends limiting variant interpretation to established...
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SubjectTerms	45/23 631/208/514/1948 631/208/514/2254 Adolescent Bioinformatics Biomedical and Life Sciences Biomedicine Child Child, Preschool Computational Biology - methods Congenital defects Cytogenetics Disease Female Gene Expression Genetic Association Studies Genetic Predisposition to Disease Genetics Genomics Genomics - methods Human Genetics Human health and pathology Humans Intellectual disabilities Life Sciences Male Molecular Diagnostic Techniques Phenotypes Polymorphism, Single Nucleotide Rare diseases Sequence Analysis, DNA Whole Exome Sequencing - methods Whole genome sequencing
Title	Increased diagnostic and new genes identification outcome using research reanalysis of singleton exome sequencing
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