The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study

Margrit Urbanek; M. Geoffrey Hayes; Loren L. Armstrong; Jean Morrison; Lynn P. Lowe; Sylvia E. Badon; Doug Scheftner; Anna Pluzhnikov; David Levine; Cathy C. Laurie; Caitlin McHugh; Christine M. Ackerman; Daniel B. Mirel; Kimberly F. Doheny; Cong Guo; Denise M. Scholtens; Alan R. Dyer; Boyd E. Metzger; Timothy E. Reddy; Nancy J. Cox; William L. Lowe

doi:10.1093/hmg/ddt168

The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study

Margrit Urbanek, M. Geoffrey Hayes, Loren L. Armstrong, Jean Morrison, Lynn P. Lowe, Sylvia E. Badon, Doug Scheftner, Anna Pluzhnikov, David Levine, Cathy C. Laurie, Caitlin McHugh, Christine M. Ackerman, Daniel B. Mirel, Kimberly F. Doheny, Cong Guo, Denise M. Scholtens, Alan R. Dyer, Boyd E. Metzger, Timothy E. Reddy, Nancy J. CoxWilliam L. Lowe

School of Medicine

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

26 Scopus citations

Abstract

Newborns characterized as large and small for gestational age are at risk for increased mortality and morbidity during the first year of life as well as for obesity and dysglycemia as children and adults. The intrauterine environment and fetal genes contribute to the fetal size at birth. To define the genetic architecture underlying the newborn size, we performed a genome-wide association study (GWAS) in 4281 newborns in four ethnic groups from the Hyperglycemia and Adverse Pregnancy Outcome Study. We tested for association with newborn anthropometric traits (birth length, headcircumference, birth weight, percent fatmassandsumof skinfolds)andnewborn metabolic traits (cord glucose and C-peptide) under three models. Model 1 adjusted for field center, ancestry, neonatal gender, gestational age at delivery, parity, maternal age at oral glucose tolerance test (OGTT); Model 2 adjusted for Model 1 covariates, maternal body mass index (BMI) at OGTT, maternal height at OGTT, maternal mean arterial pressure at OGTT, maternal smoking and drinking; Model 3 adjusted for Model 2 covariates, maternal glucose and C-peptide atOGTT. Strong evidence for associationwasobserved with measures of newborn adiposity (sum of skinfolds model 3 Z-score 7.356, P = 1.90 × 10^-13, and to a lesser degree fat mass and birth weight) and a region on Chr3q25.31 mapping between CCNL and LEKR1. These findings were replicated in an independent cohort of 2296 newborns. This region has previously been shown to be associated with birth weight in Europeans. The current study suggests that association of this locus with birth weight is secondary to an effect on fat as opposed to lean body mass.

Original language	English (US)
Article number	ddt168
Pages (from-to)	3583-3596
Number of pages	14
Journal	Human molecular genetics
Volume	22
Issue number	17
DOIs	https://doi.org/10.1093/hmg/ddt168
State	Published - Sep 2013

ASJC Scopus subject areas

Molecular Biology
Genetics
Genetics(clinical)

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10.1093/hmg/ddt168

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Urbanek, M., Hayes, M. G., Armstrong, L. L., Morrison, J., Lowe, L. P., Badon, S. E., Scheftner, D., Pluzhnikov, A., Levine, D., Laurie, C. C., McHugh, C., Ackerman, C. M., Mirel, D. B., Doheny, K. F., Guo, C., Scholtens, D. M., Dyer, A. R., Metzger, B. E., Reddy, T. E., ... Lowe, W. L. (2013). The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study. Human molecular genetics, 22(17), 3583-3596. Article ddt168. https://doi.org/10.1093/hmg/ddt168

Urbanek, M, Hayes, MG, Armstrong, LL, Morrison, J, Lowe, LP, Badon, SE, Scheftner, D, Pluzhnikov, A, Levine, D, Laurie, CC, McHugh, C, Ackerman, CM, Mirel, DB, Doheny, KF, Guo, C, Scholtens, DM, Dyer, AR, Metzger, BE, Reddy, TE, Cox, NJ & Lowe, WL 2013, 'The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study', Human molecular genetics, vol. 22, no. 17, ddt168, pp. 3583-3596. https://doi.org/10.1093/hmg/ddt168

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title = "The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study",

abstract = "Newborns characterized as large and small for gestational age are at risk for increased mortality and morbidity during the first year of life as well as for obesity and dysglycemia as children and adults. The intrauterine environment and fetal genes contribute to the fetal size at birth. To define the genetic architecture underlying the newborn size, we performed a genome-wide association study (GWAS) in 4281 newborns in four ethnic groups from the Hyperglycemia and Adverse Pregnancy Outcome Study. We tested for association with newborn anthropometric traits (birth length, headcircumference, birth weight, percent fatmassandsumof skinfolds)andnewborn metabolic traits (cord glucose and C-peptide) under three models. Model 1 adjusted for field center, ancestry, neonatal gender, gestational age at delivery, parity, maternal age at oral glucose tolerance test (OGTT); Model 2 adjusted for Model 1 covariates, maternal body mass index (BMI) at OGTT, maternal height at OGTT, maternal mean arterial pressure at OGTT, maternal smoking and drinking; Model 3 adjusted for Model 2 covariates, maternal glucose and C-peptide atOGTT. Strong evidence for associationwasobserved with measures of newborn adiposity (sum of skinfolds model 3 Z-score 7.356, P = 1.90 × 10-13, and to a lesser degree fat mass and birth weight) and a region on Chr3q25.31 mapping between CCNL and LEKR1. These findings were replicated in an independent cohort of 2296 newborns. This region has previously been shown to be associated with birth weight in Europeans. The current study suggests that association of this locus with birth weight is secondary to an effect on fat as opposed to lean body mass.",

author = "Margrit Urbanek and Hayes, {M. Geoffrey} and Armstrong, {Loren L.} and Jean Morrison and Lowe, {Lynn P.} and Badon, {Sylvia E.} and Doug Scheftner and Anna Pluzhnikov and David Levine and Laurie, {Cathy C.} and Caitlin McHugh and Ackerman, {Christine M.} and Mirel, {Daniel B.} and Doheny, {Kimberly F.} and Cong Guo and Scholtens, {Denise M.} and Dyer, {Alan R.} and Metzger, {Boyd E.} and Reddy, {Timothy E.} and Cox, {Nancy J.} and Lowe, {William L.}",

note = "Funding Information: We are indebted to the participants, investigators and research staff of the HAPO study at each of the following centers: Newcastle and Brisbane, Australia; Bridgetown, Barbados; Toronto, Canada; Hong Kong, Hong Kong; Bangkok, Thailand; Belfast and Manchester, UK; Bellflower, CA, Chicago, IL, Cleveland, OH and Providence, RI, USA. This work was supported by US National Institutes of Health (NIH) grants (HD34242, HD34243, HG004415 and CA141688) and by the American Diabetes Association. Genotype cleaning and general study coordination were provided by the GENEVA Co-ordinating Center (U01HG004446). Genotyping was performed at the Broad Institute of MIT and Harvard, with funding support from the NIH GEI (U01HG04424), and Johns Hopkins University Center for Inherited Disease Research, with support from the NIH GEI (U01HG004438) and the NIH contract {\textquoteleft}High throughput genotyping for studying the genetic contributions to human disease{\textquoteright} (HHSN268200782096C).",

year = "2013",

month = sep,

doi = "10.1093/hmg/ddt168",

language = "English (US)",

volume = "22",

pages = "3583--3596",

journal = "Human molecular genetics",

issn = "0964-6906",

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T1 - The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study

AU - Urbanek, Margrit

AU - Hayes, M. Geoffrey

AU - Armstrong, Loren L.

AU - Morrison, Jean

AU - Lowe, Lynn P.

AU - Badon, Sylvia E.

AU - Scheftner, Doug

AU - Pluzhnikov, Anna

AU - Levine, David

AU - Laurie, Cathy C.

AU - McHugh, Caitlin

AU - Ackerman, Christine M.

AU - Mirel, Daniel B.

AU - Doheny, Kimberly F.

AU - Guo, Cong

AU - Scholtens, Denise M.

AU - Dyer, Alan R.

AU - Metzger, Boyd E.

AU - Reddy, Timothy E.

AU - Cox, Nancy J.

AU - Lowe, William L.

N1 - Funding Information: We are indebted to the participants, investigators and research staff of the HAPO study at each of the following centers: Newcastle and Brisbane, Australia; Bridgetown, Barbados; Toronto, Canada; Hong Kong, Hong Kong; Bangkok, Thailand; Belfast and Manchester, UK; Bellflower, CA, Chicago, IL, Cleveland, OH and Providence, RI, USA. This work was supported by US National Institutes of Health (NIH) grants (HD34242, HD34243, HG004415 and CA141688) and by the American Diabetes Association. Genotype cleaning and general study coordination were provided by the GENEVA Co-ordinating Center (U01HG004446). Genotyping was performed at the Broad Institute of MIT and Harvard, with funding support from the NIH GEI (U01HG04424), and Johns Hopkins University Center for Inherited Disease Research, with support from the NIH GEI (U01HG004438) and the NIH contract ‘High throughput genotyping for studying the genetic contributions to human disease’ (HHSN268200782096C).

PY - 2013/9

Y1 - 2013/9

N2 - Newborns characterized as large and small for gestational age are at risk for increased mortality and morbidity during the first year of life as well as for obesity and dysglycemia as children and adults. The intrauterine environment and fetal genes contribute to the fetal size at birth. To define the genetic architecture underlying the newborn size, we performed a genome-wide association study (GWAS) in 4281 newborns in four ethnic groups from the Hyperglycemia and Adverse Pregnancy Outcome Study. We tested for association with newborn anthropometric traits (birth length, headcircumference, birth weight, percent fatmassandsumof skinfolds)andnewborn metabolic traits (cord glucose and C-peptide) under three models. Model 1 adjusted for field center, ancestry, neonatal gender, gestational age at delivery, parity, maternal age at oral glucose tolerance test (OGTT); Model 2 adjusted for Model 1 covariates, maternal body mass index (BMI) at OGTT, maternal height at OGTT, maternal mean arterial pressure at OGTT, maternal smoking and drinking; Model 3 adjusted for Model 2 covariates, maternal glucose and C-peptide atOGTT. Strong evidence for associationwasobserved with measures of newborn adiposity (sum of skinfolds model 3 Z-score 7.356, P = 1.90 × 10-13, and to a lesser degree fat mass and birth weight) and a region on Chr3q25.31 mapping between CCNL and LEKR1. These findings were replicated in an independent cohort of 2296 newborns. This region has previously been shown to be associated with birth weight in Europeans. The current study suggests that association of this locus with birth weight is secondary to an effect on fat as opposed to lean body mass.

AB - Newborns characterized as large and small for gestational age are at risk for increased mortality and morbidity during the first year of life as well as for obesity and dysglycemia as children and adults. The intrauterine environment and fetal genes contribute to the fetal size at birth. To define the genetic architecture underlying the newborn size, we performed a genome-wide association study (GWAS) in 4281 newborns in four ethnic groups from the Hyperglycemia and Adverse Pregnancy Outcome Study. We tested for association with newborn anthropometric traits (birth length, headcircumference, birth weight, percent fatmassandsumof skinfolds)andnewborn metabolic traits (cord glucose and C-peptide) under three models. Model 1 adjusted for field center, ancestry, neonatal gender, gestational age at delivery, parity, maternal age at oral glucose tolerance test (OGTT); Model 2 adjusted for Model 1 covariates, maternal body mass index (BMI) at OGTT, maternal height at OGTT, maternal mean arterial pressure at OGTT, maternal smoking and drinking; Model 3 adjusted for Model 2 covariates, maternal glucose and C-peptide atOGTT. Strong evidence for associationwasobserved with measures of newborn adiposity (sum of skinfolds model 3 Z-score 7.356, P = 1.90 × 10-13, and to a lesser degree fat mass and birth weight) and a region on Chr3q25.31 mapping between CCNL and LEKR1. These findings were replicated in an independent cohort of 2296 newborns. This region has previously been shown to be associated with birth weight in Europeans. The current study suggests that association of this locus with birth weight is secondary to an effect on fat as opposed to lean body mass.

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The chromosome 3q25 genomic region is associated with measures of adiposity in newborns in a multi-ethnic genome-wide association study

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