The impact of whole-genome sequencing on the primary care and outcomes of healthy adult patients: A pilot randomized trial

MedSeq Project

doi:10.7326/M17-0188

The impact of whole-genome sequencing on the primary care and outcomes of healthy adult patients: A pilot randomized trial

MedSeq Project

Pediatrics

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

129 Scopus citations

Abstract

Background: Whole-genome sequencing (WGS) in asymptomatic adults might prevent disease but increase health care use without clinical value. Objective: To describe the effect on clinical care and outcomes of adding WGS to standardized family history assessment in primary care. Design: Pilot randomized trial. (ClinicalTrials.gov: NCT 01736566) Setting: Academic primary care practices. Participants: 9 primary care physicians (PCPs) and 100 generally healthy patients recruited at ages 40 to 65 years. Intervention: Patients were randomly assigned to receive a family history report alone (FH group) or in combination with an interpreted WGS report (FH + WGS group), which included monogenic disease risk (MDR) results (associated with Mendelian disorders), carrier variants, pharmacogenomic associations, and polygenic risk estimates for cardiometabolic traits. Each patient met with his or her PCP to discuss the report. Measurements: Clinical outcomes and health care use through 6 months were obtained from medical records and audiorecorded discussions between PCPs and patients. Patients' health behavior changes were surveyed 6 months after receiving results. A panel of clinician-geneticists rated the appropriateness of how PCPs managed MDR results. Results: Mean age was 55 years; 58% of patients were female. Eleven FH + WGS patients (22% [95% CI, 12% to 36%]) had new MDR results. Only 2 (4% [CI, 0.01% to 15%]) had evidence of the phenotypes predicted by an MDR result (fundus albipunctatus due to RDH5 and variegate porphyria due to PPOX). Primary care physicians recommended new clinical actions for 16% (CI, 8% to 30%) of FH patients and 34% (CI, 22% to 49%) of FH + WGS patients. Thirty percent (CI, 17% to 45%) and 41% (CI, 27% to 56%) of FH and FH + WGS patients, respectively, reported making a health behavior change after 6 months. Geneticists rated PCP management of 8 MDR results (73% [CI, 39% to 99%]) as appropriate and 2 results (18% [CI, 3% to 52%]) as inappropriate. Limitation: Limited sample size and ancestral and socioeconomic diversity. Conclusion: Adding WGS to primary care reveals new molecular findings of uncertain clinical utility. Nongeneticist providers may be able to manage WGS results appropriately, but WGS may prompt additional clinical actions of unclear value.

Original language	English (US)
Pages (from-to)	159-169
Number of pages	11
Journal	Annals of internal medicine
Volume	167
Issue number	3
DOIs	https://doi.org/10.7326/M17-0188
State	Published - Aug 1 2017

ASJC Scopus subject areas

Internal Medicine

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10.7326/M17-0188

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@article{8dd128a7e33447abba149972b6d14672,

title = "The impact of whole-genome sequencing on the primary care and outcomes of healthy adult patients: A pilot randomized trial",

abstract = "Background: Whole-genome sequencing (WGS) in asymptomatic adults might prevent disease but increase health care use without clinical value. Objective: To describe the effect on clinical care and outcomes of adding WGS to standardized family history assessment in primary care. Design: Pilot randomized trial. (ClinicalTrials.gov: NCT 01736566) Setting: Academic primary care practices. Participants: 9 primary care physicians (PCPs) and 100 generally healthy patients recruited at ages 40 to 65 years. Intervention: Patients were randomly assigned to receive a family history report alone (FH group) or in combination with an interpreted WGS report (FH + WGS group), which included monogenic disease risk (MDR) results (associated with Mendelian disorders), carrier variants, pharmacogenomic associations, and polygenic risk estimates for cardiometabolic traits. Each patient met with his or her PCP to discuss the report. Measurements: Clinical outcomes and health care use through 6 months were obtained from medical records and audiorecorded discussions between PCPs and patients. Patients' health behavior changes were surveyed 6 months after receiving results. A panel of clinician-geneticists rated the appropriateness of how PCPs managed MDR results. Results: Mean age was 55 years; 58% of patients were female. Eleven FH + WGS patients (22% [95% CI, 12% to 36%]) had new MDR results. Only 2 (4% [CI, 0.01% to 15%]) had evidence of the phenotypes predicted by an MDR result (fundus albipunctatus due to RDH5 and variegate porphyria due to PPOX). Primary care physicians recommended new clinical actions for 16% (CI, 8% to 30%) of FH patients and 34% (CI, 22% to 49%) of FH + WGS patients. Thirty percent (CI, 17% to 45%) and 41% (CI, 27% to 56%) of FH and FH + WGS patients, respectively, reported making a health behavior change after 6 months. Geneticists rated PCP management of 8 MDR results (73% [CI, 39% to 99%]) as appropriate and 2 results (18% [CI, 3% to 52%]) as inappropriate. Limitation: Limited sample size and ancestral and socioeconomic diversity. Conclusion: Adding WGS to primary care reveals new molecular findings of uncertain clinical utility. Nongeneticist providers may be able to manage WGS results appropriately, but WGS may prompt additional clinical actions of unclear value.",

author = "{MedSeq Project} and Vassy, {Jason L.} and Christensen, {Kurt D.} and Schonman, {Erica F.} and Blout, {Carrie L.} and Robinson, {Jill O.} and Krier, {Joel B.} and Diamond, {Pamela M.} and Matthew Lebo and Kalotina Machini and Azzariti, {Danielle R.} and Dmitry Dukhovny and Bates, {David W.} and MacRae, {Calum A.} and Murray, {Michael F.} and Rehm, {Heidi L.} and McGuire, {Amy L.} and Green, {Robert C.} and Cirino, {Allison L.} and Ho, {Carolyn Y.} and Lane, {William J.} and Lehmann, {Lisa S.} and Morton, {Cynthia C.} and Perry, {Denise L.} and Seidman, {Christine E.} and Sunyaev, {Shamil R.} and Tiffany Nguyen and Eleanor Steffens and Betting, {Wendi Nicole} and Aronson, {Samuel J.} and Ozge Ceyhan-Birsoy and McLaughlin, {Heather M.} and Tsai, {Ellen A.} and Jennifer Blumenthal-Barby and Feuerman, {Lindsay Z.} and Kaitlyn Lee and Slashinski, {Melody J.} and Kelly Davis and Ubel, {Peter A.} and Peter Kraft and Roberts, {J. Scott} and Garber, {Judy E.} and Tina Hambuch and Isaac Kohane and Kong, {Sek Won}",

note = "Funding Information: Financial Support: By grant U01-HG006500 from the National Human Genome Research Institute of the NIH. Dr. Vassy is an employee of the VA Boston Healthcare System and received support from NIH grant KL2-TR001100 and Career Development Award IK2-CX001262 from the VA Clinical Sciences Research and Development Service. Drs. Green and Rehm are also supported by NIH grants U19-HD077671, U01-HG008685, and U41-HG006834 and by funding from the Broad Institute of MIT and Harvard. Dr. Christensen is supported by NIH grant K01-HG009173. Dr. MacRae's work in this area is supported by NIH grant U01-HG007690 and by the Burroughs Wellcome Fund. This work was conducted with support from Harvard Catalyst | The Harvard Clinical and Translational Science Center (National Center for Research Resources and National Center for Advancing Translational Sciences, NIH grant UL1-TR001102) and financial contributions from Harvard University and its affiliated academic health care centers. Publisher Copyright: {\textcopyright} 2017 American College of Physicians.",

year = "2017",

month = aug,

day = "1",

doi = "10.7326/M17-0188",

language = "English (US)",

volume = "167",

pages = "159--169",

journal = "Annals of Internal Medicine",

issn = "0003-4819",

publisher = "American College of Physicians",

number = "3",

}

TY - JOUR

T1 - The impact of whole-genome sequencing on the primary care and outcomes of healthy adult patients

T2 - A pilot randomized trial

AU - MedSeq Project

AU - Vassy, Jason L.

AU - Christensen, Kurt D.

AU - Schonman, Erica F.

AU - Blout, Carrie L.

AU - Robinson, Jill O.

AU - Krier, Joel B.

AU - Diamond, Pamela M.

AU - Lebo, Matthew

AU - Machini, Kalotina

AU - Azzariti, Danielle R.

AU - Dukhovny, Dmitry

AU - Bates, David W.

AU - MacRae, Calum A.

AU - Murray, Michael F.

AU - Rehm, Heidi L.

AU - McGuire, Amy L.

AU - Green, Robert C.

AU - Cirino, Allison L.

AU - Ho, Carolyn Y.

AU - Lane, William J.

AU - Lehmann, Lisa S.

AU - Morton, Cynthia C.

AU - Perry, Denise L.

AU - Seidman, Christine E.

AU - Sunyaev, Shamil R.

AU - Nguyen, Tiffany

AU - Steffens, Eleanor

AU - Betting, Wendi Nicole

AU - Aronson, Samuel J.

AU - Ceyhan-Birsoy, Ozge

AU - McLaughlin, Heather M.

AU - Tsai, Ellen A.

AU - Blumenthal-Barby, Jennifer

AU - Feuerman, Lindsay Z.

AU - Lee, Kaitlyn

AU - Slashinski, Melody J.

AU - Davis, Kelly

AU - Ubel, Peter A.

AU - Kraft, Peter

AU - Roberts, J. Scott

AU - Garber, Judy E.

AU - Hambuch, Tina

AU - Kohane, Isaac

AU - Kong, Sek Won

N1 - Funding Information: Financial Support: By grant U01-HG006500 from the National Human Genome Research Institute of the NIH. Dr. Vassy is an employee of the VA Boston Healthcare System and received support from NIH grant KL2-TR001100 and Career Development Award IK2-CX001262 from the VA Clinical Sciences Research and Development Service. Drs. Green and Rehm are also supported by NIH grants U19-HD077671, U01-HG008685, and U41-HG006834 and by funding from the Broad Institute of MIT and Harvard. Dr. Christensen is supported by NIH grant K01-HG009173. Dr. MacRae's work in this area is supported by NIH grant U01-HG007690 and by the Burroughs Wellcome Fund. This work was conducted with support from Harvard Catalyst | The Harvard Clinical and Translational Science Center (National Center for Research Resources and National Center for Advancing Translational Sciences, NIH grant UL1-TR001102) and financial contributions from Harvard University and its affiliated academic health care centers. Publisher Copyright: © 2017 American College of Physicians.

PY - 2017/8/1

Y1 - 2017/8/1

N2 - Background: Whole-genome sequencing (WGS) in asymptomatic adults might prevent disease but increase health care use without clinical value. Objective: To describe the effect on clinical care and outcomes of adding WGS to standardized family history assessment in primary care. Design: Pilot randomized trial. (ClinicalTrials.gov: NCT 01736566) Setting: Academic primary care practices. Participants: 9 primary care physicians (PCPs) and 100 generally healthy patients recruited at ages 40 to 65 years. Intervention: Patients were randomly assigned to receive a family history report alone (FH group) or in combination with an interpreted WGS report (FH + WGS group), which included monogenic disease risk (MDR) results (associated with Mendelian disorders), carrier variants, pharmacogenomic associations, and polygenic risk estimates for cardiometabolic traits. Each patient met with his or her PCP to discuss the report. Measurements: Clinical outcomes and health care use through 6 months were obtained from medical records and audiorecorded discussions between PCPs and patients. Patients' health behavior changes were surveyed 6 months after receiving results. A panel of clinician-geneticists rated the appropriateness of how PCPs managed MDR results. Results: Mean age was 55 years; 58% of patients were female. Eleven FH + WGS patients (22% [95% CI, 12% to 36%]) had new MDR results. Only 2 (4% [CI, 0.01% to 15%]) had evidence of the phenotypes predicted by an MDR result (fundus albipunctatus due to RDH5 and variegate porphyria due to PPOX). Primary care physicians recommended new clinical actions for 16% (CI, 8% to 30%) of FH patients and 34% (CI, 22% to 49%) of FH + WGS patients. Thirty percent (CI, 17% to 45%) and 41% (CI, 27% to 56%) of FH and FH + WGS patients, respectively, reported making a health behavior change after 6 months. Geneticists rated PCP management of 8 MDR results (73% [CI, 39% to 99%]) as appropriate and 2 results (18% [CI, 3% to 52%]) as inappropriate. Limitation: Limited sample size and ancestral and socioeconomic diversity. Conclusion: Adding WGS to primary care reveals new molecular findings of uncertain clinical utility. Nongeneticist providers may be able to manage WGS results appropriately, but WGS may prompt additional clinical actions of unclear value.

AB - Background: Whole-genome sequencing (WGS) in asymptomatic adults might prevent disease but increase health care use without clinical value. Objective: To describe the effect on clinical care and outcomes of adding WGS to standardized family history assessment in primary care. Design: Pilot randomized trial. (ClinicalTrials.gov: NCT 01736566) Setting: Academic primary care practices. Participants: 9 primary care physicians (PCPs) and 100 generally healthy patients recruited at ages 40 to 65 years. Intervention: Patients were randomly assigned to receive a family history report alone (FH group) or in combination with an interpreted WGS report (FH + WGS group), which included monogenic disease risk (MDR) results (associated with Mendelian disorders), carrier variants, pharmacogenomic associations, and polygenic risk estimates for cardiometabolic traits. Each patient met with his or her PCP to discuss the report. Measurements: Clinical outcomes and health care use through 6 months were obtained from medical records and audiorecorded discussions between PCPs and patients. Patients' health behavior changes were surveyed 6 months after receiving results. A panel of clinician-geneticists rated the appropriateness of how PCPs managed MDR results. Results: Mean age was 55 years; 58% of patients were female. Eleven FH + WGS patients (22% [95% CI, 12% to 36%]) had new MDR results. Only 2 (4% [CI, 0.01% to 15%]) had evidence of the phenotypes predicted by an MDR result (fundus albipunctatus due to RDH5 and variegate porphyria due to PPOX). Primary care physicians recommended new clinical actions for 16% (CI, 8% to 30%) of FH patients and 34% (CI, 22% to 49%) of FH + WGS patients. Thirty percent (CI, 17% to 45%) and 41% (CI, 27% to 56%) of FH and FH + WGS patients, respectively, reported making a health behavior change after 6 months. Geneticists rated PCP management of 8 MDR results (73% [CI, 39% to 99%]) as appropriate and 2 results (18% [CI, 3% to 52%]) as inappropriate. Limitation: Limited sample size and ancestral and socioeconomic diversity. Conclusion: Adding WGS to primary care reveals new molecular findings of uncertain clinical utility. Nongeneticist providers may be able to manage WGS results appropriately, but WGS may prompt additional clinical actions of unclear value.

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UR - http://www.scopus.com/inward/citedby.url?scp=85026656059&partnerID=8YFLogxK

U2 - 10.7326/M17-0188

DO - 10.7326/M17-0188

M3 - Article

C2 - 28654958

AN - SCOPUS:85026656059

SN - 0003-4819

VL - 167

SP - 159

EP - 169

JO - Annals of Internal Medicine

JF - Annals of Internal Medicine

IS - 3

ER -

The impact of whole-genome sequencing on the primary care and outcomes of healthy adult patients: A pilot randomized trial

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