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Loci for regulation of bone mineral density in men and women identified by genome wide linkage scan: the FAMOS study

Loci for regulation of bone mineral density in men and women identified by genome wide linkage scan: the FAMOS study
Loci for regulation of bone mineral density in men and women identified by genome wide linkage scan: the FAMOS study
Osteoporosis is a common disease with a strong genetic component, characterized by reduced bone mass and an increased risk of fracture. Bone mineral density (BMD) is a highly heritable trait and a key determinant of osteoporotic fracture risk, but the genes responsible are incompletely defined.
Here, we identified quantitative trait loci (QTL) for regulation of BMD by a genome wide scan involving 3691 individuals from 715 families, who were selected because of reduced BMD values at the lumbar spine (LS-BMD) or femoral neck (FN-BMD) in probands. Linkage analysis was conducted in the study group as a whole with correction for age, gender, weight and height. Further analyses were conducted for men and women separately to identify gender-specific QTL and for those under and over the age of 50 years to distinguish QTL for peak bone mass from those that influence bone mass in older people.
No regions of suggestive or significant linkage were identified when data from all subjects were analyzed together. On subgroup analysis, however, we identified a significant QTL for FN-BMD on chromosome 10q21 (LOD score +4.42; men 50 years) and two suggestive QTL for LS-BMD on chromosomes 18p11 (LOD score +2.83; women >50 years) and 20q13 (LOD score +3.20; women 50 years). We identified five other QTL for BMD with LOD scores of greater than +2.20 on chromosomes 3q25, 4q25, 7p14, 16p13 and 16q23. This study provides evidence for gender-specific, site-specific and age-specific QTL, which regulate BMD in humans, and illustrates the importance of conducting subgroup analysis to detect these loci.
943-951
Ralston, Stuart H.
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Galwey, Nick
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Mackay, Ian
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Albagha, Omar M.E.
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Cardon, Lon
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Compston, Juliet E.
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Cooper, Cyrus
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Duncan, Emma
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Keen, Richard
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Langdahl, Bente
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McLellan, Alastair
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O'Riordan, Jeffrey
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Pols, Huibert A.
a0e72ed7-b9f7-4845-86fd-c7ae43e72637
Reid, David M.
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Uitterlinden, Andre G.
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Wass, John
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Bennett, Simon T.
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Ralston, Stuart H.
1edc2a3a-ef8d-459d-a9a2-d7ef14462d2b
Galwey, Nick
81cfb0d4-cb77-4574-b35f-72d23688e3cf
Mackay, Ian
8d00806d-1ced-4dd6-8dd0-7e95a49a1397
Albagha, Omar M.E.
d8173fd9-e739-439f-97b0-06ea7edc6566
Cardon, Lon
d88bd204-6b7c-466b-9969-c03b5f7000be
Compston, Juliet E.
1038f0cb-dd36-49e5-8609-9091266faf67
Cooper, Cyrus
e05f5612-b493-4273-9b71-9e0ce32bdad6
Duncan, Emma
1f72bf7f-10a0-44cd-9060-3fa82f63cbe4
Keen, Richard
8ea73228-e6e4-46f4-a1c5-e461b926185a
Langdahl, Bente
ebedcef0-9a49-4c9f-a9f7-d1e867138ac2
McLellan, Alastair
537e5f1e-e6be-41f1-8487-b6e4519f11dc
O'Riordan, Jeffrey
b21eb49a-0972-48b4-8c2e-9793b08d15e3
Pols, Huibert A.
a0e72ed7-b9f7-4845-86fd-c7ae43e72637
Reid, David M.
2e17f1fd-d47a-4ba2-88db-1b25731224c8
Uitterlinden, Andre G.
845d72ec-de5a-4d53-9678-7469af317b29
Wass, John
2866a97c-9363-4081-860f-27f5cff91a90
Bennett, Simon T.
dd4ba856-23a0-4c48-ba2c-18326dff2a82

Ralston, Stuart H., Galwey, Nick, Mackay, Ian, Albagha, Omar M.E., Cardon, Lon, Compston, Juliet E., Cooper, Cyrus, Duncan, Emma, Keen, Richard, Langdahl, Bente, McLellan, Alastair, O'Riordan, Jeffrey, Pols, Huibert A., Reid, David M., Uitterlinden, Andre G., Wass, John and Bennett, Simon T. (2005) Loci for regulation of bone mineral density in men and women identified by genome wide linkage scan: the FAMOS study. Human Molecular Genetics, 14 (7), 943-951. (doi:10.1093/hmg/ddi088).

Record type: Article

Abstract

Osteoporosis is a common disease with a strong genetic component, characterized by reduced bone mass and an increased risk of fracture. Bone mineral density (BMD) is a highly heritable trait and a key determinant of osteoporotic fracture risk, but the genes responsible are incompletely defined.
Here, we identified quantitative trait loci (QTL) for regulation of BMD by a genome wide scan involving 3691 individuals from 715 families, who were selected because of reduced BMD values at the lumbar spine (LS-BMD) or femoral neck (FN-BMD) in probands. Linkage analysis was conducted in the study group as a whole with correction for age, gender, weight and height. Further analyses were conducted for men and women separately to identify gender-specific QTL and for those under and over the age of 50 years to distinguish QTL for peak bone mass from those that influence bone mass in older people.
No regions of suggestive or significant linkage were identified when data from all subjects were analyzed together. On subgroup analysis, however, we identified a significant QTL for FN-BMD on chromosome 10q21 (LOD score +4.42; men 50 years) and two suggestive QTL for LS-BMD on chromosomes 18p11 (LOD score +2.83; women >50 years) and 20q13 (LOD score +3.20; women 50 years). We identified five other QTL for BMD with LOD scores of greater than +2.20 on chromosomes 3q25, 4q25, 7p14, 16p13 and 16q23. This study provides evidence for gender-specific, site-specific and age-specific QTL, which regulate BMD in humans, and illustrates the importance of conducting subgroup analysis to detect these loci.

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Published date: 2005
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Identifiers

Local EPrints ID: 25924
URI: http://eprints.soton.ac.uk/id/eprint/25924
DOI: doi:10.1093/hmg/ddi088
PURE UUID: dc1401ca-8add-427a-bc92-21e67e2bcca3
ORCID for Cyrus Cooper: ORCID iD orcid.org/0000-0003-3510-0709

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Date deposited: 20 Apr 2006
Last modified: 18 Mar 2024 02:44

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Contributors

Author: Stuart H. Ralston
Author: Nick Galwey
Author: Ian Mackay
Author: Omar M.E. Albagha
Author: Lon Cardon
Author: Juliet E. Compston
Author: Cyrus Cooper ORCID iD
Author: Emma Duncan
Author: Richard Keen
Author: Bente Langdahl
Author: Alastair McLellan
Author: Jeffrey O'Riordan
Author: Huibert A. Pols
Author: David M. Reid
Author: Andre G. Uitterlinden
Author: John Wass
Author: Simon T. Bennett

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