Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.

The aims of the study were to establish the prevalence of high bone mass (HBM) in a cohort of Spanish postmenopausal women (BARCOS) and to assess the contribution of LRP5 and DKK1 mutations and of common bone mineral density (BMD) variants to a HBM phenotype. Furthermore, we describe the expression...

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Main Authors: Patricia Sarrión, Leonardo Mellibovsky, Roser Urreizti, Sergi Civit, Neus Cols, Natàlia García-Giralt, Guy Yoskovitz, Alvaro Aranguren, Jorge Malouf, Silvana Di Gregorio, Luís Del Río, Roberto Güerri, Xavier Nogués, Adolfo Díez-Pérez, Daniel Grinberg, Susana Balcells
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24736728/pdf/?tool=EBI
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spelling doaj-c695d365529f4709b72c757a857e76af2021-03-04T09:33:05ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0194e9460710.1371/journal.pone.0094607Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.Patricia SarriónLeonardo MellibovskyRoser UrreiztiSergi CivitNeus ColsNatàlia García-GiraltGuy YoskovitzAlvaro ArangurenJorge MaloufSilvana Di GregorioLuís Del RíoRoberto GüerriXavier NoguésXavier NoguésAdolfo Díez-PérezDaniel GrinbergSusana BalcellsThe aims of the study were to establish the prevalence of high bone mass (HBM) in a cohort of Spanish postmenopausal women (BARCOS) and to assess the contribution of LRP5 and DKK1 mutations and of common bone mineral density (BMD) variants to a HBM phenotype. Furthermore, we describe the expression of several osteoblast-specific and Wnt-pathway genes in primary osteoblasts from two HBM cases. A 0.6% of individuals (10/1600) displayed Z-scores in the HBM range (sum Z-score >4). While no mutation in the relevant exons of LRP5 was detected, a rare missense change in DKK1 was found (p.Y74F), which cosegregated with the phenotype in a small pedigree. Fifty-five BMD SNPs from Estrada et al. [NatGenet 44:491-501,2012] were genotyped in the HBM cases to obtain risk scores for each individual. In this small group of samples, Z-scores were found inversely related to risk scores, suggestive of a polygenic etiology. There was a single exception, which may be explained by a rare penetrant genetic variant, counterbalancing the additive effect of the risk alleles. The expression analysis in primary osteoblasts from two HBM cases and five controls suggested that IL6R, DLX3, TWIST1 and PPARG are negatively related to Z-score. One HBM case presented with high levels of RUNX2, while the other displayed very low SOX6. In conclusion, we provide evidence of lack of LRP5 mutations and of a putative HBM-causing mutation in DKK1. Additionally, we present SNP genotyping and expression results that suggest additive effects of several genes for HBM.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24736728/pdf/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Patricia Sarrión
Leonardo Mellibovsky
Roser Urreizti
Sergi Civit
Neus Cols
Natàlia García-Giralt
Guy Yoskovitz
Alvaro Aranguren
Jorge Malouf
Silvana Di Gregorio
Luís Del Río
Roberto Güerri
Xavier Nogués
Xavier Nogués
Adolfo Díez-Pérez
Daniel Grinberg
Susana Balcells
spellingShingle Patricia Sarrión
Leonardo Mellibovsky
Roser Urreizti
Sergi Civit
Neus Cols
Natàlia García-Giralt
Guy Yoskovitz
Alvaro Aranguren
Jorge Malouf
Silvana Di Gregorio
Luís Del Río
Roberto Güerri
Xavier Nogués
Xavier Nogués
Adolfo Díez-Pérez
Daniel Grinberg
Susana Balcells
Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
PLoS ONE
author_facet Patricia Sarrión
Leonardo Mellibovsky
Roser Urreizti
Sergi Civit
Neus Cols
Natàlia García-Giralt
Guy Yoskovitz
Alvaro Aranguren
Jorge Malouf
Silvana Di Gregorio
Luís Del Río
Roberto Güerri
Xavier Nogués
Xavier Nogués
Adolfo Díez-Pérez
Daniel Grinberg
Susana Balcells
author_sort Patricia Sarrión
title Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
title_short Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
title_full Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
title_fullStr Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
title_full_unstemmed Genetic analysis of high bone mass cases from the BARCOS cohort of Spanish postmenopausal women.
title_sort genetic analysis of high bone mass cases from the barcos cohort of spanish postmenopausal women.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description The aims of the study were to establish the prevalence of high bone mass (HBM) in a cohort of Spanish postmenopausal women (BARCOS) and to assess the contribution of LRP5 and DKK1 mutations and of common bone mineral density (BMD) variants to a HBM phenotype. Furthermore, we describe the expression of several osteoblast-specific and Wnt-pathway genes in primary osteoblasts from two HBM cases. A 0.6% of individuals (10/1600) displayed Z-scores in the HBM range (sum Z-score >4). While no mutation in the relevant exons of LRP5 was detected, a rare missense change in DKK1 was found (p.Y74F), which cosegregated with the phenotype in a small pedigree. Fifty-five BMD SNPs from Estrada et al. [NatGenet 44:491-501,2012] were genotyped in the HBM cases to obtain risk scores for each individual. In this small group of samples, Z-scores were found inversely related to risk scores, suggestive of a polygenic etiology. There was a single exception, which may be explained by a rare penetrant genetic variant, counterbalancing the additive effect of the risk alleles. The expression analysis in primary osteoblasts from two HBM cases and five controls suggested that IL6R, DLX3, TWIST1 and PPARG are negatively related to Z-score. One HBM case presented with high levels of RUNX2, while the other displayed very low SOX6. In conclusion, we provide evidence of lack of LRP5 mutations and of a putative HBM-causing mutation in DKK1. Additionally, we present SNP genotyping and expression results that suggest additive effects of several genes for HBM.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/24736728/pdf/?tool=EBI
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