Clinical diagnosis by whole-genome sequencing of a prenatal sample.

Michael E Talkowski; Zehra Ordulu; Vamsee Pillalamarri; Carol B Benson; Ian Blumenthal; Susan Connolly; Carrie Hanscom; Naveed Hussain; Shahrin Pereira; Jonathan Picker; Jill A Rosenfeld; Lisa G Shaffer; Louise E Wilkins-Haug; James F Gusella; Cynthia C Morton

doi:10.1056/NEJMoa1208594

Clinical diagnosis by whole-genome sequencing of a prenatal sample.

Michael E Talkowski, Zehra Ordulu, Vamsee Pillalamarri, Carol B Benson, Ian Blumenthal, Susan Connolly, Carrie Hanscom, Naveed Hussain, Shahrin Pereira, Jonathan Picker, Jill A Rosenfeld, Lisa G Shaffer, Louise E Wilkins-Haug, James F Gusella, Cynthia C Morton

Research output: Contribution to journal › Article › peer-review

Abstract

Conventional cytogenetic testing offers low-resolution detection of balanced karyotypic abnormalities but cannot provide the precise, gene-level knowledge required to predict outcomes. The use of high-resolution whole-genome deep sequencing is currently impractical for the purpose of routine clinical care. We show here that whole-genome "jumping libraries" can offer an immediately applicable, nucleotide-level complement to conventional genetic diagnostics within a time frame that allows for clinical action. We performed large-insert sequencing of DNA extracted from amniotic-fluid cells with a balanced de novo translocation. The amniotic-fluid sample was from a patient in the third trimester of pregnancy who underwent amniocentesis because of severe polyhydramnios after multiple fetal anomalies had been detected on ultrasonography. Using a 13-day sequence and analysis pipeline, we discovered direct disruption of CHD7, a causal locus in the CHARGE syndrome (coloboma of the eye, heart anomaly, atresia of the choanae, retardation, and genital and ear anomalies). Clinical findings at birth were consistent with the CHARGE syndrome, a diagnosis that could not have been reliably inferred from the cytogenetic breakpoint. This case study illustrates the potential power of customized whole-genome jumping libraries when used to augment prenatal karyotyping.

Original language	English
Journal	The New England Journal of Medicine
Volume	367
Issue number	23
DOIs	https://doi.org/10.1056/NEJMoa1208594
Publication status	Published - 6 Dec 2012

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Talkowski, M. E., Ordulu, Z., Pillalamarri, V., Benson, C. B., Blumenthal, I., Connolly, S., Hanscom, C., Hussain, N., Pereira, S., Picker, J., Rosenfeld, J. A., Shaffer, L. G., Wilkins-Haug, L. E., Gusella, J. F., & Morton, C. C. (2012). Clinical diagnosis by whole-genome sequencing of a prenatal sample. The New England Journal of Medicine, 367(23). https://doi.org/10.1056/NEJMoa1208594

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title = "Clinical diagnosis by whole-genome sequencing of a prenatal sample.",

abstract = "Conventional cytogenetic testing offers low-resolution detection of balanced karyotypic abnormalities but cannot provide the precise, gene-level knowledge required to predict outcomes. The use of high-resolution whole-genome deep sequencing is currently impractical for the purpose of routine clinical care. We show here that whole-genome {"}jumping libraries{"} can offer an immediately applicable, nucleotide-level complement to conventional genetic diagnostics within a time frame that allows for clinical action. We performed large-insert sequencing of DNA extracted from amniotic-fluid cells with a balanced de novo translocation. The amniotic-fluid sample was from a patient in the third trimester of pregnancy who underwent amniocentesis because of severe polyhydramnios after multiple fetal anomalies had been detected on ultrasonography. Using a 13-day sequence and analysis pipeline, we discovered direct disruption of CHD7, a causal locus in the CHARGE syndrome (coloboma of the eye, heart anomaly, atresia of the choanae, retardation, and genital and ear anomalies). Clinical findings at birth were consistent with the CHARGE syndrome, a diagnosis that could not have been reliably inferred from the cytogenetic breakpoint. This case study illustrates the potential power of customized whole-genome jumping libraries when used to augment prenatal karyotyping.",

author = "Talkowski, {Michael E} and Zehra Ordulu and Vamsee Pillalamarri and Benson, {Carol B} and Ian Blumenthal and Susan Connolly and Carrie Hanscom and Naveed Hussain and Shahrin Pereira and Jonathan Picker and Rosenfeld, {Jill A} and Shaffer, {Lisa G} and Wilkins-Haug, {Louise E} and Gusella, {James F} and Morton, {Cynthia C}",

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doi = "10.1056/NEJMoa1208594",

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Talkowski, ME, Ordulu, Z, Pillalamarri, V, Benson, CB, Blumenthal, I, Connolly, S, Hanscom, C, Hussain, N, Pereira, S, Picker, J, Rosenfeld, JA, Shaffer, LG, Wilkins-Haug, LE, Gusella, JF & Morton, CC 2012, 'Clinical diagnosis by whole-genome sequencing of a prenatal sample.', The New England Journal of Medicine, vol. 367, no. 23. https://doi.org/10.1056/NEJMoa1208594

TY - JOUR

T1 - Clinical diagnosis by whole-genome sequencing of a prenatal sample.

AU - Talkowski, Michael E

AU - Ordulu, Zehra

AU - Pillalamarri, Vamsee

AU - Benson, Carol B

AU - Blumenthal, Ian

AU - Connolly, Susan

AU - Hanscom, Carrie

AU - Hussain, Naveed

AU - Pereira, Shahrin

AU - Picker, Jonathan

AU - Rosenfeld, Jill A

AU - Shaffer, Lisa G

AU - Wilkins-Haug, Louise E

AU - Gusella, James F

AU - Morton, Cynthia C

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PY - 2012/12/6

Y1 - 2012/12/6

N2 - Conventional cytogenetic testing offers low-resolution detection of balanced karyotypic abnormalities but cannot provide the precise, gene-level knowledge required to predict outcomes. The use of high-resolution whole-genome deep sequencing is currently impractical for the purpose of routine clinical care. We show here that whole-genome "jumping libraries" can offer an immediately applicable, nucleotide-level complement to conventional genetic diagnostics within a time frame that allows for clinical action. We performed large-insert sequencing of DNA extracted from amniotic-fluid cells with a balanced de novo translocation. The amniotic-fluid sample was from a patient in the third trimester of pregnancy who underwent amniocentesis because of severe polyhydramnios after multiple fetal anomalies had been detected on ultrasonography. Using a 13-day sequence and analysis pipeline, we discovered direct disruption of CHD7, a causal locus in the CHARGE syndrome (coloboma of the eye, heart anomaly, atresia of the choanae, retardation, and genital and ear anomalies). Clinical findings at birth were consistent with the CHARGE syndrome, a diagnosis that could not have been reliably inferred from the cytogenetic breakpoint. This case study illustrates the potential power of customized whole-genome jumping libraries when used to augment prenatal karyotyping.

AB - Conventional cytogenetic testing offers low-resolution detection of balanced karyotypic abnormalities but cannot provide the precise, gene-level knowledge required to predict outcomes. The use of high-resolution whole-genome deep sequencing is currently impractical for the purpose of routine clinical care. We show here that whole-genome "jumping libraries" can offer an immediately applicable, nucleotide-level complement to conventional genetic diagnostics within a time frame that allows for clinical action. We performed large-insert sequencing of DNA extracted from amniotic-fluid cells with a balanced de novo translocation. The amniotic-fluid sample was from a patient in the third trimester of pregnancy who underwent amniocentesis because of severe polyhydramnios after multiple fetal anomalies had been detected on ultrasonography. Using a 13-day sequence and analysis pipeline, we discovered direct disruption of CHD7, a causal locus in the CHARGE syndrome (coloboma of the eye, heart anomaly, atresia of the choanae, retardation, and genital and ear anomalies). Clinical findings at birth were consistent with the CHARGE syndrome, a diagnosis that could not have been reliably inferred from the cytogenetic breakpoint. This case study illustrates the potential power of customized whole-genome jumping libraries when used to augment prenatal karyotyping.

U2 - 10.1056/NEJMoa1208594

DO - 10.1056/NEJMoa1208594

M3 - Article

C2 - 23215558

VL - 367

JO - The New England Journal of Medicine

JF - The New England Journal of Medicine

SN - 1533-4406

IS - 23

ER -

Clinical diagnosis by whole-genome sequencing of a prenatal sample.

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