Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics

Jamie R. Robinson; Robert J. Carroll; Lisa Bastarache; Qingxia Chen; James Pirruccello; Zongyang Mou; Wei Qi Wei; John Connolly; Frank Mentch; Paul K. Crane; Scott J. Hebbring; David R. Crosslin; Adam S. Gordon; Elisabeth A. Rosenthal; Ian B. Stanaway; M. Geoffrey Hayes; Wei Wei; Lynn Petukhova; Bahram Namjou-Khales; Ge Zhang; Mayya S. Safarova; Nephi A. Walton; Christopher Still; Erwin P. Bottinger; Ruth J.F. Loos; Shawn N. Murphy; Gretchen P. Jackson; Naji Abumrad; Iftikhar J. Kullo; Gail P. Jarvik; Eric B. Larson; Chunhua Weng; Dan Roden; Amit V. Khera; Joshua C. Denny

doi:10.1002/oby.23561

Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics

Jamie R. Robinson, Robert J. Carroll, Lisa Bastarache, Qingxia Chen, James Pirruccello, Zongyang Mou, Wei Qi Wei, John Connolly, Frank Mentch, Paul K. Crane, Scott J. Hebbring, David R. Crosslin, Adam S. Gordon, Elisabeth A. Rosenthal, Ian B. Stanaway, M. Geoffrey Hayes, Wei Wei, Lynn Petukhova, Bahram Namjou-Khales, Ge ZhangMayya S. Safarova, Nephi A. Walton, Christopher Still, Erwin P. Bottinger, Ruth J.F. Loos, Shawn N. Murphy, Gretchen P. Jackson, Naji Abumrad, Iftikhar J. Kullo, Gail P. Jarvik, Eric B. Larson, Chunhua Weng, Dan Roden, Amit V. Khera, Joshua C. Denny

Cardiovascular Medicine

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

Abstract

Objective: High BMI is associated with many comorbidities and mortality. This study aimed to elucidate the overall clinical risk of obesity using a genome- and phenome-wide approach. Methods: This study performed a phenome-wide association study of BMI using a clinical cohort of 736,726 adults. This was followed by genetic association studies using two separate cohorts: one consisting of 65,174 adults in the Electronic Medical Records and Genomics (eMERGE) Network and another with 405,432 participants in the UK Biobank. Results: Class 3 obesity was associated with 433 phenotypes, representing 59.3% of all billing codes in individuals with severe obesity. A genome-wide polygenic risk score for BMI, accounting for 7.5% of variance in BMI, was associated with 296 clinical diseases, including strong associations with type 2 diabetes, sleep apnea, hypertension, and chronic liver disease. In all three cohorts, 199 phenotypes were associated with class 3 obesity and polygenic risk for obesity, including novel associations such as increased risk of renal failure, venous insufficiency, and gastroesophageal reflux. Conclusions: This combined genomic and phenomic systematic approach demonstrated that obesity has a strong genetic predisposition and is associated with a considerable burden of disease across all disease classes.

Original language	English (US)
Pages (from-to)	2477-2488
Number of pages	12
Journal	Obesity
Volume	30
Issue number	12
DOIs	https://doi.org/10.1002/oby.23561
State	Published - Dec 2022

ASJC Scopus subject areas

Medicine (miscellaneous)
Endocrinology, Diabetes and Metabolism
Endocrinology
Nutrition and Dietetics

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10.1002/oby.23561

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Robinson, J. R., Carroll, R. J., Bastarache, L., Chen, Q., Pirruccello, J., Mou, Z., Wei, W. Q., Connolly, J., Mentch, F., Crane, P. K., Hebbring, S. J., Crosslin, D. R., Gordon, A. S., Rosenthal, E. A., Stanaway, I. B., Hayes, M. G., Wei, W., Petukhova, L., Namjou-Khales, B., ... Denny, J. C. (2022). Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics. Obesity, 30(12), 2477-2488. https://doi.org/10.1002/oby.23561

Robinson, JR, Carroll, RJ, Bastarache, L, Chen, Q, Pirruccello, J, Mou, Z, Wei, WQ, Connolly, J, Mentch, F, Crane, PK, Hebbring, SJ, Crosslin, DR, Gordon, AS, Rosenthal, EA, Stanaway, IB, Hayes, MG, Wei, W, Petukhova, L, Namjou-Khales, B, Zhang, G, Safarova, MS, Walton, NA, Still, C, Bottinger, EP, Loos, RJF, Murphy, SN, Jackson, GP, Abumrad, N, Kullo, IJ, Jarvik, GP, Larson, EB, Weng, C, Roden, D, Khera, AV & Denny, JC 2022, 'Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics', Obesity, vol. 30, no. 12, pp. 2477-2488. https://doi.org/10.1002/oby.23561

@article{96390d8bb2a44a0ca22edd782425b8a1,

title = "Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics",

abstract = "Objective: High BMI is associated with many comorbidities and mortality. This study aimed to elucidate the overall clinical risk of obesity using a genome- and phenome-wide approach. Methods: This study performed a phenome-wide association study of BMI using a clinical cohort of 736,726 adults. This was followed by genetic association studies using two separate cohorts: one consisting of 65,174 adults in the Electronic Medical Records and Genomics (eMERGE) Network and another with 405,432 participants in the UK Biobank. Results: Class 3 obesity was associated with 433 phenotypes, representing 59.3% of all billing codes in individuals with severe obesity. A genome-wide polygenic risk score for BMI, accounting for 7.5% of variance in BMI, was associated with 296 clinical diseases, including strong associations with type 2 diabetes, sleep apnea, hypertension, and chronic liver disease. In all three cohorts, 199 phenotypes were associated with class 3 obesity and polygenic risk for obesity, including novel associations such as increased risk of renal failure, venous insufficiency, and gastroesophageal reflux. Conclusions: This combined genomic and phenomic systematic approach demonstrated that obesity has a strong genetic predisposition and is associated with a considerable burden of disease across all disease classes.",

author = "Robinson, {Jamie R.} and Carroll, {Robert J.} and Lisa Bastarache and Qingxia Chen and James Pirruccello and Zongyang Mou and Wei, {Wei Qi} and John Connolly and Frank Mentch and Crane, {Paul K.} and Hebbring, {Scott J.} and Crosslin, {David R.} and Gordon, {Adam S.} and Rosenthal, {Elisabeth A.} and Stanaway, {Ian B.} and Hayes, {M. Geoffrey} and Wei Wei and Lynn Petukhova and Bahram Namjou-Khales and Ge Zhang and Safarova, {Mayya S.} and Walton, {Nephi A.} and Christopher Still and Bottinger, {Erwin P.} and Loos, {Ruth J.F.} and Murphy, {Shawn N.} and Jackson, {Gretchen P.} and Naji Abumrad and Kullo, {Iftikhar J.} and Jarvik, {Gail P.} and Larson, {Eric B.} and Chunhua Weng and Dan Roden and Khera, {Amit V.} and Denny, {Joshua C.}",

note = "Publisher Copyright: {\textcopyright} 2022 The Obesity Society. This article has been contributed to by U.S. Government employees and their work is in the public domain in the USA.",

year = "2022",

month = dec,

doi = "10.1002/oby.23561",

language = "English (US)",

volume = "30",

pages = "2477--2488",

journal = "Obesity",

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TY - JOUR

T1 - Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics

AU - Robinson, Jamie R.

AU - Carroll, Robert J.

AU - Bastarache, Lisa

AU - Chen, Qingxia

AU - Pirruccello, James

AU - Mou, Zongyang

AU - Wei, Wei Qi

AU - Connolly, John

AU - Mentch, Frank

AU - Crane, Paul K.

AU - Hebbring, Scott J.

AU - Crosslin, David R.

AU - Gordon, Adam S.

AU - Rosenthal, Elisabeth A.

AU - Stanaway, Ian B.

AU - Hayes, M. Geoffrey

AU - Wei, Wei

AU - Petukhova, Lynn

AU - Namjou-Khales, Bahram

AU - Zhang, Ge

AU - Safarova, Mayya S.

AU - Walton, Nephi A.

AU - Still, Christopher

AU - Bottinger, Erwin P.

AU - Loos, Ruth J.F.

AU - Murphy, Shawn N.

AU - Jackson, Gretchen P.

AU - Abumrad, Naji

AU - Kullo, Iftikhar J.

AU - Jarvik, Gail P.

AU - Larson, Eric B.

AU - Weng, Chunhua

AU - Roden, Dan

AU - Khera, Amit V.

AU - Denny, Joshua C.

PY - 2022/12

Y1 - 2022/12

N2 - Objective: High BMI is associated with many comorbidities and mortality. This study aimed to elucidate the overall clinical risk of obesity using a genome- and phenome-wide approach. Methods: This study performed a phenome-wide association study of BMI using a clinical cohort of 736,726 adults. This was followed by genetic association studies using two separate cohorts: one consisting of 65,174 adults in the Electronic Medical Records and Genomics (eMERGE) Network and another with 405,432 participants in the UK Biobank. Results: Class 3 obesity was associated with 433 phenotypes, representing 59.3% of all billing codes in individuals with severe obesity. A genome-wide polygenic risk score for BMI, accounting for 7.5% of variance in BMI, was associated with 296 clinical diseases, including strong associations with type 2 diabetes, sleep apnea, hypertension, and chronic liver disease. In all three cohorts, 199 phenotypes were associated with class 3 obesity and polygenic risk for obesity, including novel associations such as increased risk of renal failure, venous insufficiency, and gastroesophageal reflux. Conclusions: This combined genomic and phenomic systematic approach demonstrated that obesity has a strong genetic predisposition and is associated with a considerable burden of disease across all disease classes.

AB - Objective: High BMI is associated with many comorbidities and mortality. This study aimed to elucidate the overall clinical risk of obesity using a genome- and phenome-wide approach. Methods: This study performed a phenome-wide association study of BMI using a clinical cohort of 736,726 adults. This was followed by genetic association studies using two separate cohorts: one consisting of 65,174 adults in the Electronic Medical Records and Genomics (eMERGE) Network and another with 405,432 participants in the UK Biobank. Results: Class 3 obesity was associated with 433 phenotypes, representing 59.3% of all billing codes in individuals with severe obesity. A genome-wide polygenic risk score for BMI, accounting for 7.5% of variance in BMI, was associated with 296 clinical diseases, including strong associations with type 2 diabetes, sleep apnea, hypertension, and chronic liver disease. In all three cohorts, 199 phenotypes were associated with class 3 obesity and polygenic risk for obesity, including novel associations such as increased risk of renal failure, venous insufficiency, and gastroesophageal reflux. Conclusions: This combined genomic and phenomic systematic approach demonstrated that obesity has a strong genetic predisposition and is associated with a considerable burden of disease across all disease classes.

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JO - Obesity

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ER -

Quantifying the phenome-wide disease burden of obesity using electronic health records and genomics

Abstract

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