Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study

Yan Fang Guo; Li Shu Zhang; Yong Jun Liu; Hong Gang Hu; Jian Li; Qing Tian; Ping Yu; Feng Zhang; Tie Lin Yang; Yan Guo; Xiang Lei Peng; Meng Dai; Wei Chen; Hong Wen Deng

doi:10.1007/s00439-012-1236-5

Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study

Yan Fang Guo
, Li Shu Zhang
, Yong Jun Liu
, Hong Gang Hu
, Jian Li
, Qing Tian
, Ping Yu
, Feng Zhang
, Tie Lin Yang
, Yan Guo
, Xiang Lei Peng
, Meng Dai
, Wei Chen
, Hong Wen Deng

School of Life Science and Technology (SLST)

Southern Medical University
Beijing Jiaotong University
Tulane University
Xi'an Jiaotong University
University of Shanghai for Science and Technology

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

57 Scopus citations

Abstract

Bone and muscle, two major tissue types of musculoskeletal system, have strong genetic determination. Abnormality in bone and/or muscle may cause musculoskeletal diseases such as osteoporosis and sarcopenia. Bone size phenotypes (BSPs), such as hip bone size (HBS), appendicular bone size (ABS), are genetically correlated with body lean mass (mainly muscle mass). However, the specific genes shared by these phenotypes are largely unknown. In this study, we aimed to identify the specific genes with pleiotropic effects on BSPs and appendicular lean mass (ALM). We performed a bivariate genome-wide association study (GWAS) by analyzing ~690,000 SNPs in 1,627 unrelated Han Chinese adults (802 males and 825 females) followed by a replication study in 2,286 unrelated US Caucasians (558 males and 1,728 females). We identified 14 interesting single nucleotide polymorphisms (SNPs) that may contribute to variation of both BSPs and ALM, with p values <10^-6 in discovery stage. Among them, the association of three SNPs (rs2507838, rs7116722, and rs11826261) in/near GLYAT (glycine-N-acyltransferase) gene was replicated in US Caucasians, with p values ranging from 1.89 × 10^-3 to 3.71 × 10^-4 for ALM-ABS, from 5.14 × 10^-3 to 1.11 × 10^-2 for ALM-HBS, respectively. Meta-analyses yielded stronger association signals for rs2507838, rs7116722, and rs11826261, with pooled p values of 1.68 × 10^-8, 7.94 × 10^-8, 6.80 × 10^-8 for ALB-ABS and 1.22 × 10^-4, 9.85 × 10^-5, 3.96 × 10^-4 for ALM-HBS, respectively. Haplotype allele ATA based on these three SNPs was also associated with ALM-HBS and ALM-ABS in both discovery and replication samples. Interestingly, GLYAT was previously found to be essential to glucose metabolism and energy metabolism, suggesting the gene's dual role in both bone development and muscle growth. Our findings, together with the prior biological evidence, suggest the importance of GLYAT gene in co-regulation of bone phenotypes and body lean mass.

Original language	English
Pages (from-to)	189-199
Number of pages	11
Journal	Human Genetics
Volume	132
Issue number	2
DOIs	https://doi.org/10.1007/s00439-012-1236-5
State	Published - Feb 2013

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Guo, Y. F., Zhang, L. S., Liu, Y. J., Hu, H. G., Li, J., Tian, Q., Yu, P., Zhang, F., Yang, T. L., Guo, Y., Peng, X. L., Dai, M., Chen, W., & Deng, H. W. (2013). Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study. Human Genetics, 132(2), 189-199. https://doi.org/10.1007/s00439-012-1236-5

@article{92fc6867c70247c68edf63fb6d3260c2,

title = "Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study",

abstract = "Bone and muscle, two major tissue types of musculoskeletal system, have strong genetic determination. Abnormality in bone and/or muscle may cause musculoskeletal diseases such as osteoporosis and sarcopenia. Bone size phenotypes (BSPs), such as hip bone size (HBS), appendicular bone size (ABS), are genetically correlated with body lean mass (mainly muscle mass). However, the specific genes shared by these phenotypes are largely unknown. In this study, we aimed to identify the specific genes with pleiotropic effects on BSPs and appendicular lean mass (ALM). We performed a bivariate genome-wide association study (GWAS) by analyzing \textasciitilde{}690,000 SNPs in 1,627 unrelated Han Chinese adults (802 males and 825 females) followed by a replication study in 2,286 unrelated US Caucasians (558 males and 1,728 females). We identified 14 interesting single nucleotide polymorphisms (SNPs) that may contribute to variation of both BSPs and ALM, with p values <10-6 in discovery stage. Among them, the association of three SNPs (rs2507838, rs7116722, and rs11826261) in/near GLYAT (glycine-N-acyltransferase) gene was replicated in US Caucasians, with p values ranging from 1.89 × 10-3 to 3.71 × 10-4 for ALM-ABS, from 5.14 × 10-3 to 1.11 × 10-2 for ALM-HBS, respectively. Meta-analyses yielded stronger association signals for rs2507838, rs7116722, and rs11826261, with pooled p values of 1.68 × 10-8, 7.94 × 10-8, 6.80 × 10-8 for ALB-ABS and 1.22 × 10-4, 9.85 × 10-5, 3.96 × 10-4 for ALM-HBS, respectively. Haplotype allele ATA based on these three SNPs was also associated with ALM-HBS and ALM-ABS in both discovery and replication samples. Interestingly, GLYAT was previously found to be essential to glucose metabolism and energy metabolism, suggesting the gene's dual role in both bone development and muscle growth. Our findings, together with the prior biological evidence, suggest the importance of GLYAT gene in co-regulation of bone phenotypes and body lean mass.",

author = "Guo, \{Yan Fang\} and Zhang, \{Li Shu\} and Liu, \{Yong Jun\} and Hu, \{Hong Gang\} and Jian Li and Qing Tian and Ping Yu and Feng Zhang and Yang, \{Tie Lin\} and Yan Guo and Peng, \{Xiang Lei\} and Meng Dai and Wei Chen and Deng, \{Hong Wen\}",

year = "2013",

month = feb,

doi = "10.1007/s00439-012-1236-5",

language = "英语",

volume = "132",

pages = "189--199",

journal = "Human Genetics",

issn = "0340-6717",

publisher = "Springer Science and Business Media Deutschland GmbH",

number = "2",

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TY - JOUR

T1 - Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study

AU - Guo, Yan Fang

AU - Zhang, Li Shu

AU - Liu, Yong Jun

AU - Hu, Hong Gang

AU - Li, Jian

AU - Tian, Qing

AU - Yu, Ping

AU - Zhang, Feng

AU - Yang, Tie Lin

AU - Guo, Yan

AU - Peng, Xiang Lei

AU - Dai, Meng

AU - Chen, Wei

AU - Deng, Hong Wen

PY - 2013/2

Y1 - 2013/2

N2 - Bone and muscle, two major tissue types of musculoskeletal system, have strong genetic determination. Abnormality in bone and/or muscle may cause musculoskeletal diseases such as osteoporosis and sarcopenia. Bone size phenotypes (BSPs), such as hip bone size (HBS), appendicular bone size (ABS), are genetically correlated with body lean mass (mainly muscle mass). However, the specific genes shared by these phenotypes are largely unknown. In this study, we aimed to identify the specific genes with pleiotropic effects on BSPs and appendicular lean mass (ALM). We performed a bivariate genome-wide association study (GWAS) by analyzing ~690,000 SNPs in 1,627 unrelated Han Chinese adults (802 males and 825 females) followed by a replication study in 2,286 unrelated US Caucasians (558 males and 1,728 females). We identified 14 interesting single nucleotide polymorphisms (SNPs) that may contribute to variation of both BSPs and ALM, with p values <10-6 in discovery stage. Among them, the association of three SNPs (rs2507838, rs7116722, and rs11826261) in/near GLYAT (glycine-N-acyltransferase) gene was replicated in US Caucasians, with p values ranging from 1.89 × 10-3 to 3.71 × 10-4 for ALM-ABS, from 5.14 × 10-3 to 1.11 × 10-2 for ALM-HBS, respectively. Meta-analyses yielded stronger association signals for rs2507838, rs7116722, and rs11826261, with pooled p values of 1.68 × 10-8, 7.94 × 10-8, 6.80 × 10-8 for ALB-ABS and 1.22 × 10-4, 9.85 × 10-5, 3.96 × 10-4 for ALM-HBS, respectively. Haplotype allele ATA based on these three SNPs was also associated with ALM-HBS and ALM-ABS in both discovery and replication samples. Interestingly, GLYAT was previously found to be essential to glucose metabolism and energy metabolism, suggesting the gene's dual role in both bone development and muscle growth. Our findings, together with the prior biological evidence, suggest the importance of GLYAT gene in co-regulation of bone phenotypes and body lean mass.

AB - Bone and muscle, two major tissue types of musculoskeletal system, have strong genetic determination. Abnormality in bone and/or muscle may cause musculoskeletal diseases such as osteoporosis and sarcopenia. Bone size phenotypes (BSPs), such as hip bone size (HBS), appendicular bone size (ABS), are genetically correlated with body lean mass (mainly muscle mass). However, the specific genes shared by these phenotypes are largely unknown. In this study, we aimed to identify the specific genes with pleiotropic effects on BSPs and appendicular lean mass (ALM). We performed a bivariate genome-wide association study (GWAS) by analyzing ~690,000 SNPs in 1,627 unrelated Han Chinese adults (802 males and 825 females) followed by a replication study in 2,286 unrelated US Caucasians (558 males and 1,728 females). We identified 14 interesting single nucleotide polymorphisms (SNPs) that may contribute to variation of both BSPs and ALM, with p values <10-6 in discovery stage. Among them, the association of three SNPs (rs2507838, rs7116722, and rs11826261) in/near GLYAT (glycine-N-acyltransferase) gene was replicated in US Caucasians, with p values ranging from 1.89 × 10-3 to 3.71 × 10-4 for ALM-ABS, from 5.14 × 10-3 to 1.11 × 10-2 for ALM-HBS, respectively. Meta-analyses yielded stronger association signals for rs2507838, rs7116722, and rs11826261, with pooled p values of 1.68 × 10-8, 7.94 × 10-8, 6.80 × 10-8 for ALB-ABS and 1.22 × 10-4, 9.85 × 10-5, 3.96 × 10-4 for ALM-HBS, respectively. Haplotype allele ATA based on these three SNPs was also associated with ALM-HBS and ALM-ABS in both discovery and replication samples. Interestingly, GLYAT was previously found to be essential to glucose metabolism and energy metabolism, suggesting the gene's dual role in both bone development and muscle growth. Our findings, together with the prior biological evidence, suggest the importance of GLYAT gene in co-regulation of bone phenotypes and body lean mass.

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DO - 10.1007/s00439-012-1236-5

M3 - 文章

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AN - SCOPUS:84874766536

SN - 0340-6717

VL - 132

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EP - 199

JO - Human Genetics

JF - Human Genetics

IS - 2

ER -

Suggestion of GLYAT gene underlying variation of bone size and body lean mass as revealed by a bivariate genome-wide association study

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