Literature DB >> 21907839

Cortical bone health shows significant linkage to chromosomes 2p, 3p, and 17q in 10-year-old children.

Dana L Duren1, John Blangero, Richard J Sherwood, Maja Seselj, Thomas Dyer, Shelley A Cole, Miryoung Lee, Audrey C Choh, Wm Cameron Chumlea, Roger M Siervogel, Stefan A Czerwinski, Bradford Towne.   

Abstract

Genes play an important role in lifelong skeletal health. Genes that influence bone building during childhood have the potential to affect bone health not only throughout childhood but also into adulthood. Given that peak bone mass is a significant predictor of adult fracture risk, it is imperative that the genetic underpinnings of the normal pediatric skeleton are uncovered. In a sample of 600 10-year-old children from 144 families in the Fels Longitudinal Study, we examined radiographic cortical bone measures of the second metacarpal. Morphometic measurements included bone width, medial and lateral cortical thicknesses, and the calculated cortical index representing the amount of cortex relative to bone width. We then conducted genome-wide linkage analysis on these traits in 440 genotyped individuals using the SOLAR analytic platform. Significant quantitative trait loci (QTL) were identified for bone traits on three separate chromosomes. A QTL for medial cortical thickness was localized to chromosome 2p25.2. A QTL for lateral cortical thickness was localized to chromosomal region 3p26.1-3p25.3. Finally, a QTL detected for cortical index was localized to the 17q21.2 chromosomal region. Each region contains plausible candidate genes for pediatric skeletal health, some of which confirm findings from studies of adulthood bone, and for others represent novel candidate genes for skeletal health.
Copyright © 2011 Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21907839      PMCID: PMC3221785          DOI: 10.1016/j.bone.2011.08.024

Source DB:  PubMed          Journal:  Bone        ISSN: 1873-2763            Impact factor:   4.398


  60 in total

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  6 in total

1.  Bone growth in juvenile rhesus monkeys is influenced by 5HTTLPR polymorphisms and interactions between 5HTTLPR polymorphisms and fluoxetine.

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2.  The influence of age at menarche on cross-sectional geometry of bone in young adulthood.

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5.  Low-dose combined oral contraceptive use is associated with lower bone mineral content variation in adolescents over a 1-year period.

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6.  Genetic factors influencing bone mineral content in a black South African population.

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