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Genome-wide association meta-analysis of cortical bone mineral density unravels allelic heterogeneity at the RANKL locus and potential Pleiotropic effects on bone
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نویسنده
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paternoster l. ,lorentzon m. ,vandenput l. ,karlsson m.k. ,ljunggren o. ,kindmark a. ,mellstrom d. ,kemp j.p. ,jarett c.e. ,holly j.m.p. ,sayers a. ,st. pourcain b. ,timpson n.j. ,deloukas p. ,smith g.d. ,ring s.m. ,evans d.m. ,tobias j.h. ,ohlsson c.
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منبع
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plos genetics - 2010 - دوره : 6 - شماره : 11
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چکیده
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Previous genome-wide association (gwa) studies have identified snps associated with areal bone mineral density (abmd). however,this measure is influenced by several different skeletal parameters,such as periosteal expansion,cortical bone mineral density (bmdc) cortical thickness,trabecular number,and trabecular thickness,which may be under distinct biological and genetic control. we have carried out a gwa and replication study of bmdc,as measured by peripheral quantitative computed tomography (pqct),a more homogenous and valid measure of actual volumetric bone density. after initial gwa meta-analysis of two cohorts (alspac n = 999,aged ~15 years and good n = 935,aged ~19 years),we attempted to replicate the bmdc associations that had p<1×10-5 in an independent sample of alspac children (n = 2803) and in a cohort of elderly men (mros sweden,n = 1052). the rs1021188 snp (near rankl) was associated with bmdc in all cohorts (overall p = 2×10-14,n = 5739). each minor allele was associated with a decrease in bmdc of ~0.14sd. there was also evidence for an interaction between this variant and sex (p = 0.01),with a stronger effect in males than females (at age 15,males -6.77mg/cm3 per c allele,p = 2×10-6; females -2.79 mg/cm3 per c allele,p = 0.004). furthermore,in a preliminary analysis,the rs1021188 minor c allele was associated with higher circulating levels of srankl (p<0.005). we show this variant to be independent from the previously abmd associated snp (rs9594738) and possibly from a third variant in the same rankl region,which demonstrates important allelic heterogeneity at this locus. associations with skeletal parameters reflecting bone dimensions were either not found or were much less pronounced. this finding implicates rankl as a locus containing variation associated with volumetric bone density and provides further insight into the mechanism by which the rank/rankl/opg pathway may be involved in skeletal development. © 2010 paternoster et al.
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آدرس
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medical research council centre for causal analyses in translational epidemiology,university of bristol,bristol,united kingdom,school of social and community medicine,university of bristol,bristol, United Kingdom, center for bone and arthritis research,departments of internal medicine and geriatrics,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, center for bone and arthritis research,departments of internal medicine and geriatrics,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, clinical and molecular osteoporosis research unit,department of clinical sciences,lund university,malmö,sweden,department of orthopaedics,skåne university hospital,malmö, Sweden, department of medical sciences,university hospital,uppsala, Sweden, department of medical sciences,university hospital,uppsala, Sweden, center for bone and arthritis research,departments of internal medicine and geriatrics,sahlgrenska academy,university of gothenburg,gothenburg, Sweden, medical research council centre for causal analyses in translational epidemiology,university of bristol,bristol,united kingdom,school of social and community medicine,university of bristol,bristol, United Kingdom, department of clinical science at north bristol,university of bristol,bristol, United Kingdom, department of clinical science at north bristol,university of bristol,bristol, United Kingdom, department of clinical science at north bristol,university of bristol,bristol, United Kingdom, school of social and community medicine,university of bristol,bristol, United Kingdom, medical research council centre for causal analyses in translational epidemiology,university of bristol,bristol,united kingdom,school of social and community medicine,university of bristol,bristol, United Kingdom, wellcome trust sanger institute,cambridge, United Kingdom, medical research council centre for causal analyses in translational epidemiology,university of bristol,bristol,united kingdom,school of social and community medicine,university of bristol,bristol, United Kingdom, school of social and community medicine,university of bristol,bristol, United Kingdom, medical research council centre for causal analyses in translational epidemiology,university of bristol,bristol,united kingdom,school of social and community medicine,university of bristol,bristol, United Kingdom, department of clinical science at north bristol,university of bristol,bristol, United Kingdom, center for bone and arthritis research,departments of internal medicine and geriatrics,sahlgrenska academy,university of gothenburg,gothenburg, Sweden
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Authors
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