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Meta-analysis of genome-wide scans for total body BMD in children and adults reveals allelic heterogeneity and age-specific effects at the WNT16 locus
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نویسنده
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medina-gomez c. ,kemp j.p. ,estrada k. ,eriksson j. ,liu j. ,reppe s. ,evans d.m. ,heppe d.h.m. ,vandenput l. ,herrera l. ,ring s.m. ,kruithof c.j. ,timpson n.j. ,zillikens m.c. ,olstad o.k. ,zheng h.-f. ,richards j.b. ,st. pourcain b. ,hofman a. ,jaddoe v.w.v. ,smith g.d. ,lorentzon m. ,gautvik k.m. ,uitterlinden a.g. ,brommage r. ,ohlsson c. ,tobias j.h. ,rivadeneira f.
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منبع
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plos genetics - 2012 - دوره : 8 - شماره : 7
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چکیده
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To identify genetic loci influencing bone accrual,we performed a genome-wide association scan for total-body bone mineral density (tb-bmd) variation in 2,660 children of different ethnicities. we discovered variants in 7q31.31 associated with bmd measurements,with the lowest p = 4.1×10-11 observed for rs917727 with minor allele frequency of 0.37. we sought replication for all snps located ±500 kb from rs917727 in 11,052 additional individuals from five independent studies including children and adults,together with de novo genotyping of rs3801387 (in perfect linkage disequilibrium (ld) with rs917727) in 1,014 mothers of children from the discovery cohort. the top signal mapping in the surroundings of wnt16 was replicated across studies with a meta-analysis p = 2.6×10-31 and an effect size explaining between 0.6%-1.8% of tb-bmd variance. conditional analyses on this signal revealed a secondary signal for total body bmd (p = 1.42×10-10) for rs4609139 and mapping to c7orf58. we also examined the genomic region for association with skull bmd to test if the associations were independent of skeletal loading. we identified two signals influencing skull bmd variation,including rs917727 (p = 1.9×10-16) and rs7801723 (p = 8.9×10-28),also mapping to c7orf58 (r2 = 0.50 with rs4609139). wnt16 knockout (ko) mice with reduced total body bmd and gene expression profiles in human bone biopsies support a role of c7orf58 and wnt16 on the bmd phenotypes observed at the human population level. in summary,we detected two independent signals influencing total body and skull bmd variation in children and adults,thus demonstrating the presence of allelic heterogeneity at the wnt16 locus. one of the skull bmd signals mapping to c7orf58 is mostly driven by children,suggesting temporal determination on peak bone mass acquisition. our life-course approach postulates that these genetic effects influencing peak bone mass accrual may impact the risk of osteoporosis later in life. © 2012 medina-gomez et al.
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آدرس
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department of internal medicine,erasmus university medical center,rotterdam,netherlands,the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands, mrc caite centre,school of social and community medicine,university of bristol,bristol,united kingdom,avon longitudinal study of parents and children (alspac),school of social and community medicine,university of bristol,bristol, United Kingdom, department of internal medicine,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands, center for bone and arthritis research,institute of medicine,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, lexicon pharmaceuticals,the woodlands,tx, United States, department of medical biochemistry,oslo university hospital,ullevaal,oslo, Norway, mrc caite centre,school of social and community medicine,university of bristol,bristol,united kingdom,avon longitudinal study of parents and children (alspac),school of social and community medicine,university of bristol,bristol, United Kingdom, the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,department of pediatrics,erasmus university medical center,rotterdam, Netherlands, center for bone and arthritis research,institute of medicine,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, department of internal medicine,erasmus university medical center,rotterdam, Netherlands, avon longitudinal study of parents and children (alspac),school of social and community medicine,university of bristol,bristol, United Kingdom, the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam, Netherlands, mrc caite centre,school of social and community medicine,university of bristol,bristol,united kingdom,avon longitudinal study of parents and children (alspac),school of social and community medicine,university of bristol,bristol, United Kingdom, department of internal medicine,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands, department of medical biochemistry,oslo university hospital,ullevaal,oslo, Norway, department of medicine,human genetics,mcgill university,montreal,qc,canada,department of epidemiology and biostatistics,lady davis institute for medical research,jewish general hospital,montreal,qc, Canada, department of medicine,human genetics,mcgill university,montreal,qc,canada,department of epidemiology and biostatistics,lady davis institute for medical research,jewish general hospital,montreal,qc,canada,twin research and genetic epidemiology,king's college london,london, United Kingdom, mrc caite centre,school of social and community medicine,university of bristol,bristol, United Kingdom, the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands, the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,department of pediatrics,erasmus university medical center,rotterdam, Netherlands, mrc caite centre,school of social and community medicine,university of bristol,bristol,united kingdom,avon longitudinal study of parents and children (alspac),school of social and community medicine,university of bristol,bristol, United Kingdom, center for bone and arthritis research,institute of medicine,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, department of medical biochemistry,oslo university hospital,ullevaal,oslo,norway,department of medical biochemistry,oslo deacon hospital,oslo, Norway, department of internal medicine,erasmus university medical center,rotterdam,netherlands,the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands, lexicon pharmaceuticals,the woodlands,tx, United States, center for bone and arthritis research,institute of medicine,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, school of clinical sciences,university of bristol,bristol, United Kingdom, department of internal medicine,erasmus university medical center,rotterdam,netherlands,the generation r study group,erasmus university medical center,rotterdam,netherlands,department of epidemiology,erasmus university medical center,rotterdam,netherlands,netherlands genomics initiative (ngi)-sponsored netherlands consortium for healthy aging (ncha),rotterdam, Netherlands
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Authors
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