Molecular diagnostic experience of whole-exome sequencing in adult patients

Jennifer E. Posey; Jill A. Rosenfeld; Regis A. James; Matthew Bainbridge; Zhiyv Niu; Xia Wang; Shweta Dhar; Wojciech Wiszniewski; Zeynep H.C. Akdemir; Tomasz Gambin; Fan Xia; Richard E. Person; Magdalena Walkiewicz; Chad A. Shaw; V. Reid Sutton; Arthur L. Beaudet; Donna Muzny; Christine M. Eng; Yaping Yang; Richard A. Gibbs; James R. Lupski; Eric Boerwinkle; Sharon E. Plon

doi:10.1038/gim.2015.142

Molecular diagnostic experience of whole-exome sequencing in adult patients

Jennifer E. Posey, Jill A. Rosenfeld, Regis A. James, Matthew Bainbridge, Zhiyv Niu, Xia Wang, Shweta Dhar, Wojciech Wiszniewski, Zeynep H.C. Akdemir, Tomasz Gambin, Fan Xia, Richard E. Person, Magdalena Walkiewicz, Chad A. Shaw, V. Reid Sutton, Arthur L. Beaudet, Donna Muzny, Christine M. Eng, Yaping Yang, Richard A. GibbsJames R. Lupski, Eric Boerwinkle, Sharon E. Plon

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152 Scopus citations

Abstract

Purpose:Whole-exome sequencing (WES) is increasingly used as a diagnostic tool in medicine, but prior reports focus on predominantly pediatric cohorts with neurologic or developmental disorders. We describe the diagnostic yield and characteristics of WES in adults.Methods:We performed a retrospective analysis of consecutive WES reports for adults from a diagnostic laboratory. Phenotype composition was determined using Human Phenotype Ontology terms.Results:Molecular diagnoses were reported for 17.5% (85/486) of adults, which is lower than that for a primarily pediatric population (25.2%; P = 0.0003); the diagnostic rate was higher (23.9%) for those 18-30 years of age compared to patients older than 30 years (10.4%; P = 0.0001). Dual Mendelian diagnoses contributed to 7% of diagnoses, revealing blended phenotypes. Diagnoses were more frequent among individuals with abnormalities of the nervous system, skeletal system, head/neck, and growth. Diagnostic rate was independent of family history information, and de novo mutations contributed to 61.4% of autosomal dominant diagnoses.Conclusion:Early WES experience in adults demonstrates molecular diagnoses in a substantial proportion of patients, informing clinical management, recurrence risk, and recommendations for relatives. A positive family history was not predictive, consistent with molecular diagnoses often revealed by de novo events, informing the Mendelian basis of genetic disease in adults.

Original language	English (US)
Pages (from-to)	678-685
Number of pages	8
Journal	Genetics in Medicine
Volume	18
Issue number	7
DOIs	https://doi.org/10.1038/gim.2015.142
State	Published - Jul 1 2016
Externally published	Yes

Keywords

adult patients
whole-exome sequencing

ASJC Scopus subject areas

Genetics(clinical)

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10.1038/gim.2015.142

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Posey, J. E., Rosenfeld, J. A., James, R. A., Bainbridge, M., Niu, Z., Wang, X., Dhar, S., Wiszniewski, W., Akdemir, Z. H. C., Gambin, T., Xia, F., Person, R. E., Walkiewicz, M., Shaw, C. A., Sutton, V. R., Beaudet, A. L., Muzny, D., Eng, C. M., Yang, Y., ... Plon, S. E. (2016). Molecular diagnostic experience of whole-exome sequencing in adult patients. Genetics in Medicine, 18(7), 678-685. https://doi.org/10.1038/gim.2015.142

Posey, JE, Rosenfeld, JA, James, RA, Bainbridge, M, Niu, Z, Wang, X, Dhar, S, Wiszniewski, W, Akdemir, ZHC, Gambin, T, Xia, F, Person, RE, Walkiewicz, M, Shaw, CA, Sutton, VR, Beaudet, AL, Muzny, D, Eng, CM, Yang, Y, Gibbs, RA, Lupski, JR, Boerwinkle, E & Plon, SE 2016, 'Molecular diagnostic experience of whole-exome sequencing in adult patients', Genetics in Medicine, vol. 18, no. 7, pp. 678-685. https://doi.org/10.1038/gim.2015.142

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title = "Molecular diagnostic experience of whole-exome sequencing in adult patients",

abstract = "Purpose:Whole-exome sequencing (WES) is increasingly used as a diagnostic tool in medicine, but prior reports focus on predominantly pediatric cohorts with neurologic or developmental disorders. We describe the diagnostic yield and characteristics of WES in adults.Methods:We performed a retrospective analysis of consecutive WES reports for adults from a diagnostic laboratory. Phenotype composition was determined using Human Phenotype Ontology terms.Results:Molecular diagnoses were reported for 17.5% (85/486) of adults, which is lower than that for a primarily pediatric population (25.2%; P = 0.0003); the diagnostic rate was higher (23.9%) for those 18-30 years of age compared to patients older than 30 years (10.4%; P = 0.0001). Dual Mendelian diagnoses contributed to 7% of diagnoses, revealing blended phenotypes. Diagnoses were more frequent among individuals with abnormalities of the nervous system, skeletal system, head/neck, and growth. Diagnostic rate was independent of family history information, and de novo mutations contributed to 61.4% of autosomal dominant diagnoses.Conclusion:Early WES experience in adults demonstrates molecular diagnoses in a substantial proportion of patients, informing clinical management, recurrence risk, and recommendations for relatives. A positive family history was not predictive, consistent with molecular diagnoses often revealed by de novo events, informing the Mendelian basis of genetic disease in adults.",

keywords = "adult patients, whole-exome sequencing",

author = "Posey, {Jennifer E.} and Rosenfeld, {Jill A.} and James, {Regis A.} and Matthew Bainbridge and Zhiyv Niu and Xia Wang and Shweta Dhar and Wojciech Wiszniewski and Akdemir, {Zeynep H.C.} and Tomasz Gambin and Fan Xia and Person, {Richard E.} and Magdalena Walkiewicz and Shaw, {Chad A.} and Sutton, {V. Reid} and Beaudet, {Arthur L.} and Donna Muzny and Eng, {Christine M.} and Yaping Yang and Gibbs, {Richard A.} and Lupski, {James R.} and Eric Boerwinkle and Plon, {Sharon E.}",

note = "Funding Information: J.E.P. was supported by the Medical Genetics Research Fellowship Program NIH/NIGMS NIH T32 GM07526. W.W. was supported by the Career Development Award K23NS078056 from the National Institute of Neurological Disorders and Stroke (NINDS). This work was funded in part by grants U01 HG006485 (S.E.P.) from the National Human Genome Research Institute (NHGRI) and National Cancer Institute (NCI), U54 HG006542 (J.R.L.) from the NHGRI and National Heart, Lung, and Blood Institute (NHLBI), U54-HG003273 (R.A.G.) from the NHGRI, and R01 NS058529 (J.R.L.) from the NINDS. NHGRI, NCI, and NINDS had no role in the design and conduct of the study; the collection, management, analysis, and interpretation of the data; the preparation, review, or approval of the manuscript; or the decision to submit the manuscript for publication. Publisher Copyright: {\textcopyright} American College of Medical Genetics and Genomics.",

year = "2016",

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doi = "10.1038/gim.2015.142",

language = "English (US)",

volume = "18",

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T1 - Molecular diagnostic experience of whole-exome sequencing in adult patients

AU - Posey, Jennifer E.

AU - Rosenfeld, Jill A.

AU - James, Regis A.

AU - Bainbridge, Matthew

AU - Niu, Zhiyv

AU - Wang, Xia

AU - Dhar, Shweta

AU - Wiszniewski, Wojciech

AU - Akdemir, Zeynep H.C.

AU - Gambin, Tomasz

AU - Xia, Fan

AU - Person, Richard E.

AU - Walkiewicz, Magdalena

AU - Shaw, Chad A.

AU - Sutton, V. Reid

AU - Beaudet, Arthur L.

AU - Muzny, Donna

AU - Eng, Christine M.

AU - Yang, Yaping

AU - Gibbs, Richard A.

AU - Lupski, James R.

AU - Boerwinkle, Eric

AU - Plon, Sharon E.

N1 - Funding Information: J.E.P. was supported by the Medical Genetics Research Fellowship Program NIH/NIGMS NIH T32 GM07526. W.W. was supported by the Career Development Award K23NS078056 from the National Institute of Neurological Disorders and Stroke (NINDS). This work was funded in part by grants U01 HG006485 (S.E.P.) from the National Human Genome Research Institute (NHGRI) and National Cancer Institute (NCI), U54 HG006542 (J.R.L.) from the NHGRI and National Heart, Lung, and Blood Institute (NHLBI), U54-HG003273 (R.A.G.) from the NHGRI, and R01 NS058529 (J.R.L.) from the NINDS. NHGRI, NCI, and NINDS had no role in the design and conduct of the study; the collection, management, analysis, and interpretation of the data; the preparation, review, or approval of the manuscript; or the decision to submit the manuscript for publication. Publisher Copyright: © American College of Medical Genetics and Genomics.

PY - 2016/7/1

Y1 - 2016/7/1

N2 - Purpose:Whole-exome sequencing (WES) is increasingly used as a diagnostic tool in medicine, but prior reports focus on predominantly pediatric cohorts with neurologic or developmental disorders. We describe the diagnostic yield and characteristics of WES in adults.Methods:We performed a retrospective analysis of consecutive WES reports for adults from a diagnostic laboratory. Phenotype composition was determined using Human Phenotype Ontology terms.Results:Molecular diagnoses were reported for 17.5% (85/486) of adults, which is lower than that for a primarily pediatric population (25.2%; P = 0.0003); the diagnostic rate was higher (23.9%) for those 18-30 years of age compared to patients older than 30 years (10.4%; P = 0.0001). Dual Mendelian diagnoses contributed to 7% of diagnoses, revealing blended phenotypes. Diagnoses were more frequent among individuals with abnormalities of the nervous system, skeletal system, head/neck, and growth. Diagnostic rate was independent of family history information, and de novo mutations contributed to 61.4% of autosomal dominant diagnoses.Conclusion:Early WES experience in adults demonstrates molecular diagnoses in a substantial proportion of patients, informing clinical management, recurrence risk, and recommendations for relatives. A positive family history was not predictive, consistent with molecular diagnoses often revealed by de novo events, informing the Mendelian basis of genetic disease in adults.

AB - Purpose:Whole-exome sequencing (WES) is increasingly used as a diagnostic tool in medicine, but prior reports focus on predominantly pediatric cohorts with neurologic or developmental disorders. We describe the diagnostic yield and characteristics of WES in adults.Methods:We performed a retrospective analysis of consecutive WES reports for adults from a diagnostic laboratory. Phenotype composition was determined using Human Phenotype Ontology terms.Results:Molecular diagnoses were reported for 17.5% (85/486) of adults, which is lower than that for a primarily pediatric population (25.2%; P = 0.0003); the diagnostic rate was higher (23.9%) for those 18-30 years of age compared to patients older than 30 years (10.4%; P = 0.0001). Dual Mendelian diagnoses contributed to 7% of diagnoses, revealing blended phenotypes. Diagnoses were more frequent among individuals with abnormalities of the nervous system, skeletal system, head/neck, and growth. Diagnostic rate was independent of family history information, and de novo mutations contributed to 61.4% of autosomal dominant diagnoses.Conclusion:Early WES experience in adults demonstrates molecular diagnoses in a substantial proportion of patients, informing clinical management, recurrence risk, and recommendations for relatives. A positive family history was not predictive, consistent with molecular diagnoses often revealed by de novo events, informing the Mendelian basis of genetic disease in adults.

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Molecular diagnostic experience of whole-exome sequencing in adult patients

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