Association of CDX1 binding site of periostin gene with bone mineral density and vertebral fracture risk

S-M Xiao; Y Gao; C-L Cheung; C H Bow; K-S Lau; P C Sham; K C B Tan; A W C Kung

doi:10.1007/s00198-011-1861-1

Association of CDX1 binding site of periostin gene with bone mineral density and vertebral fracture risk

Osteoporos Int. 2012 Jul;23(7):1877-87. doi: 10.1007/s00198-011-1861-1. Epub 2012 Jan 4.

Authors

S-M Xiao¹, Y Gao, C-L Cheung, C H Bow, K-S Lau, P C Sham, K C B Tan, A W C Kung

Affiliation

¹ Department of Medicine, Faculty of Medicine, The University of Hong Kong, Hong Kong, China. xiaosm@hku.hk

Abstract

Summary: Periostin (POSTN) as a regulator of osteoblast differentiation and bone formation may affect susceptibility to osteoporosis. This study suggests POSTN as a candidate gene for bone mineral density (BMD) variation and vertebral fracture risk, which could better our understanding about the genetic pathogenesis of osteoporosis and will be useful in clinic in the future.

Introduction: The genetic determination of osteoporosis is complex and ill-defined. Periostin (POSTN), an extracellular matrix secreted by osteoblasts and a regulator of osteoblast differentiation and bone formation, may affect susceptibility to osteoporosis.

Methods: We adopted a tag-single nucleotide polymorphism (SNP) based association method followed by imputation-based verification and identification of a causal variant. The association was investigated in 1,572 subjects with extreme-BMD and replicated in an independent population of 2,509 subjects. BMD was measured by dual X-ray absorptiometry. Vertebral fractures were identified by assessing vertebral height from X-rays of the thoracolumbar spine. Association analyses were performed with PLINK toolset and imputation analyses with MACH software. The top imputation finding was subsequently validated by genotyping. Interactions between POSTN and another BMD-related candidate gene sclerostin (SOST) were analyzed using MDR program and validated by logistical regression analyses. The putative transcription factor binding with target sequence was confirmed by electrophoretic mobility shift assay (EMSA).

Results: Several SNPs of POSTN were associated with BMD or vertebral fractures. The most significant polymorphism was rs9547970, located at the -2,327 bp upstream (P = 6.8 × 10(-4)) of POSTN. Carriers of the minor allele G per copy of rs9547970 had 1.33 higher risk of vertebral fracture (P = 0.007). An interactive effect between POSTN and SOST upon BMD variation was suggested (P < 0.01). A specific binding of CDX1 to the sequence of POSTN with the major allele A of rs9547970 but not the variant G allele was confirmed by EMSA.

Conclusions: Our results suggest POSTN as a candidate gene for BMD variation and vertebral fracture risk.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Binding Sites / genetics
Bone Density / genetics*
Cell Adhesion Molecules / genetics*
Cell Adhesion Molecules / metabolism
Female
Genetic Predisposition to Disease
Genotype
Homeodomain Proteins / metabolism*
Humans
Male
Middle Aged
Osteoporotic Fractures / genetics*
Osteoporotic Fractures / physiopathology
Polymorphism, Single Nucleotide
Protein Binding / genetics
Spinal Fractures / genetics*
Spinal Fractures / physiopathology

Substances

CDX1 protein, human
Cell Adhesion Molecules
Homeodomain Proteins
POSTN protein, human