Limited Clinical Utility of a Genetic Risk Score for the Prediction of Fracture Risk in Elderly Subjects

Eriksson, Joel; Evans, Daniel S.; Nielson, Carrie M.; Shen, Jian; Srikanth, Priya; Hochberg, Marc; McWeeney, Shannon; Cawthon, Peggy M.; Wilmot, Beth; Zmuda, Joseph; Tranah, Greg; Mirel, Daniel B.; Challa, Sashi; Mooney, Michael; Crenshaw, Andrew; Karlsson, Magnus; Mellstrom, Dan; Vandenput, Liesbeth; Orwoll, Eric; Ohlsson, Claes

Limited Clinical Utility of a Genetic Risk Score for the Prediction of Fracture Risk in Elderly Subjects

Mark

Eriksson, Joel ; Evans, Daniel S. ; Nielson, Carrie M. ; Shen, Jian ; Srikanth, Priya ; Hochberg, Marc ; McWeeney, Shannon ; Cawthon, Peggy M. ; Wilmot, Beth and Zmuda, Joseph , et al. (2015) In Journal of Bone and Mineral Research 30(1). p.184-194

Abstract: It is important to identify the patients at highest risk of fractures. A recent large-scale meta-analysis identified 63 autosomal single-nucleotide polymorphisms (SNPs) associated with bone mineral density (BMD), of which 16 were also associated with fracture risk. Based on these findings, two genetic risk scores (GRS63 and GRS16) were developed. Our aim was to determine the clinical usefulness of these GRSs for the prediction of BMD, BMD change, and fracture risk in elderly subjects. We studied two male (Osteoporotic Fractures in Men Study [MrOS] US, MrOS Sweden) and one female (Study of Osteoporotic Fractures [SOF]) large prospective cohorts of older subjects, looking at BMD, BMD change, and radiographically and/or medically confirmed... (More); It is important to identify the patients at highest risk of fractures. A recent large-scale meta-analysis identified 63 autosomal single-nucleotide polymorphisms (SNPs) associated with bone mineral density (BMD), of which 16 were also associated with fracture risk. Based on these findings, two genetic risk scores (GRS63 and GRS16) were developed. Our aim was to determine the clinical usefulness of these GRSs for the prediction of BMD, BMD change, and fracture risk in elderly subjects. We studied two male (Osteoporotic Fractures in Men Study [MrOS] US, MrOS Sweden) and one female (Study of Osteoporotic Fractures [SOF]) large prospective cohorts of older subjects, looking at BMD, BMD change, and radiographically and/or medically confirmed incident fractures (8067 subjects, 2185 incident nonvertebral or vertebral fractures). GRS63 was associated with BMD (3% of the variation explained) but not with BMD change. Both GRS63 and GRS16 were associated with fractures. After BMD adjustment, the effect sizes for these associations were substantially reduced. Similar results were found using an unweighted GRS63 and an unweighted GRS16 compared with those found using the corresponding weighted risk scores. Only minor improvements in C-statistics (AUC) for fractures were found when the GRSs were added to a base model (age, weight, and height), and no significant improvements in C-statistics were found when they were added to a model further adjusted for BMD. Net reclassification improvements with the addition of the GRSs to a base model were modest and substantially attenuated in BMD-adjusted models. GRS63 is associated with BMD, but not BMD change, suggesting that the genetic determinants of BMD differ from those of BMD change. When BMD is known, the clinical utility of the two GRSs for fracture prediction is limited in elderly subjects. (c) 2014 American Society for Bone and Mineral Research. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/5085205

author

Eriksson, Joel ; Evans, Daniel S. ; Nielson, Carrie M. ; Shen, Jian ; Srikanth, Priya ; Hochberg, Marc ; McWeeney, Shannon ; Cawthon, Peggy M. ; Wilmot, Beth and Zmuda, Joseph , et al. (More)

Eriksson, Joel ; Evans, Daniel S. ; Nielson, Carrie M. ; Shen, Jian ; Srikanth, Priya ; Hochberg, Marc ; McWeeney, Shannon ; Cawthon, Peggy M. ; Wilmot, Beth ; Zmuda, Joseph ; Tranah, Greg ; Mirel, Daniel B. ; Challa, Sashi ; Mooney, Michael ; Crenshaw, Andrew ; Karlsson, Magnus ^LU ; Mellstrom, Dan ; Vandenput, Liesbeth ; Orwoll, Eric and Ohlsson, Claes (Less)

organization

publishing date

2015

type

Contribution to journal

publication status

published

subject

Orthopedics

keywords

GENERAL POPULATION STUDIES, HUMAN ASSOCIATION STUDIES, FRACTURE RISK, ASSESSMENT, OSTEOPOROSIS, DXA

in

Journal of Bone and Mineral Research

volume

30

issue

1

pages

184 - 194

publisher

Wiley-Blackwell

external identifiers

wos:000346914600020
scopus:84919918723
pmid:25043339

ISSN

1523-4681

DOI

10.1002/jbmr.2314

language

English

LU publication?

yes

id

b88ec6cd-de18-4c5d-ab35-c4811e3cd3cc (old id 5085205)

date added to LUP

2016-04-01 10:10:27

date last changed

2022-01-25 20:31:19

@article{b88ec6cd-de18-4c5d-ab35-c4811e3cd3cc,
  abstract     = {{It is important to identify the patients at highest risk of fractures. A recent large-scale meta-analysis identified 63 autosomal single-nucleotide polymorphisms (SNPs) associated with bone mineral density (BMD), of which 16 were also associated with fracture risk. Based on these findings, two genetic risk scores (GRS63 and GRS16) were developed. Our aim was to determine the clinical usefulness of these GRSs for the prediction of BMD, BMD change, and fracture risk in elderly subjects. We studied two male (Osteoporotic Fractures in Men Study [MrOS] US, MrOS Sweden) and one female (Study of Osteoporotic Fractures [SOF]) large prospective cohorts of older subjects, looking at BMD, BMD change, and radiographically and/or medically confirmed incident fractures (8067 subjects, 2185 incident nonvertebral or vertebral fractures). GRS63 was associated with BMD (3% of the variation explained) but not with BMD change. Both GRS63 and GRS16 were associated with fractures. After BMD adjustment, the effect sizes for these associations were substantially reduced. Similar results were found using an unweighted GRS63 and an unweighted GRS16 compared with those found using the corresponding weighted risk scores. Only minor improvements in C-statistics (AUC) for fractures were found when the GRSs were added to a base model (age, weight, and height), and no significant improvements in C-statistics were found when they were added to a model further adjusted for BMD. Net reclassification improvements with the addition of the GRSs to a base model were modest and substantially attenuated in BMD-adjusted models. GRS63 is associated with BMD, but not BMD change, suggesting that the genetic determinants of BMD differ from those of BMD change. When BMD is known, the clinical utility of the two GRSs for fracture prediction is limited in elderly subjects. (c) 2014 American Society for Bone and Mineral Research.}},
  author       = {{Eriksson, Joel and Evans, Daniel S. and Nielson, Carrie M. and Shen, Jian and Srikanth, Priya and Hochberg, Marc and McWeeney, Shannon and Cawthon, Peggy M. and Wilmot, Beth and Zmuda, Joseph and Tranah, Greg and Mirel, Daniel B. and Challa, Sashi and Mooney, Michael and Crenshaw, Andrew and Karlsson, Magnus and Mellstrom, Dan and Vandenput, Liesbeth and Orwoll, Eric and Ohlsson, Claes}},
  issn         = {{1523-4681}},
  keywords     = {{GENERAL POPULATION STUDIES; HUMAN ASSOCIATION STUDIES; FRACTURE RISK; ASSESSMENT; OSTEOPOROSIS; DXA}},
  language     = {{eng}},
  number       = {{1}},
  pages        = {{184--194}},
  publisher    = {{Wiley-Blackwell}},
  series       = {{Journal of Bone and Mineral Research}},
  title        = {{Limited Clinical Utility of a Genetic Risk Score for the Prediction of Fracture Risk in Elderly Subjects}},
  url          = {{http://dx.doi.org/10.1002/jbmr.2314}},
  doi          = {{10.1002/jbmr.2314}},
  volume       = {{30}},
  year         = {{2015}},
}

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Limited Clinical Utility of a Genetic Risk Score for the Prediction of Fracture Risk in Elderly Subjects