GeneSet Information

Tier II GS129106 • bone mineral density 1 (Bomd1 Published QTL Chr 7)

DESCRIPTION:

QTL associated with bone mineral density 1. The confidence interval is Chr7:92864897-93179294 bp,+strand

LABEL:

QTL-Bomd1-Mouse-Chr 7

SCORE TYPE:

Binary

DATE ADDED:

2012-04-02

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Klein RF, Mitchell SR, Phillips TJ, Belknap JK, Orwoll ES

TITLE:

Quantitative trait loci affecting peak bone mineral density in mice.

JOURNAL:

Journal of bone and mineral research : the official journal of the American Society for Bone and Mineral Research Nov 1998, Vol 13, pp. 1648-56

ABSTRACT:

Peak bone mass is a major determinant of risk of osteoporotic fracture. Family and twin studies have found a strong genetic component to the determination of bone mineral density (BMD). However, BMD is a complex trait whose expression is confounded by environmental influences and polygenic inheritance. The number, locations, and effects of the individual genes contributing to natural variation in this trait are all unknown. Experimental animal models provide a means to circumvent complicating environmental factors, and the development of dense genetic maps based on molecular markers now provides opportunities to resolve quantitative genetic variation into individual regions of the genome influencing a given trait (quantitative trait loci, QTL). To begin to identify the heritable determinants of BMD, we have examined genetically distinct laboratory mouse strains raised under strict environmental control. Mouse whole-body bone mineral content by dual-energy X-ray absorptiometry (DXA) correlated strongly with skeletal calcium content by ashing, and peak whole-body BMD by DXA in female mice occurred at approximately 80-90 days of age. We therefore determined mean body weight and peak whole body BMD values in 12-week-old female mice from a panel of 24 recombinant inbred (RI) BXD strains, derived from a cross between C57BL/6 and DBA/2 progenitors. The distribution of body weight and BMD values among the strains clearly indicated the presence of strong genetic influences on both of these traits, with an estimated narrow sense heritability of 60% and 35%, respectively. The patterns of differences in body weight and peak whole body BMD in the BXD strains were then integrated with a large database of genetic markers previously defined in the RI BXD strains to generate chromosome map sites for QTL. After correction for redundancy among the significant correlations, QTL analysis of the BXD RI strain series provisionally identified 10 chromosomal sites linked to peak bone mass development in the female. Several of the identified sites map near genes encoding hormones, structural proteins, and cell surface receptors that are intricately involved in skeletal homeostasis. Four QTL for body weight were also identified. One of these loci was also strongly linked to inherited variation in BMD. This finding suggests that body weight and peak BMD may be influenced by linked genes or perhaps by common genes with pleiotropic effects. Our phenotyping in the RI BXD strains has allowed us to map a number of specific genetic loci strongly related to the acquisition of peak BMD. Confirmation of these findings will likely result in the understanding of which genes control skeletal health. PUBMED: 9797472
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Annotation Information

No sequence read archive data associated with this GeneSet.


Genetic Variation (D014644)
Homeostasis (D006706)
Laboratories (D007753)
Osteoporotic Fractures (D058866)
Animals (D000818)
Bone Density (D015519)
Chromosomes (D002875)
Calcium (D002118)
Comprehension (D032882)
Quantitative Trait Loci (D040641)
Genetic Markers (D005819)
Models, Animal (D023421)
Proteins (D011506)
Genetic Loci (D056426)
Multifactorial Inheritance (D020412)
Bone and Bones (D001842)
Hormones (D006728)
Absorptiometry, Photon (D015502)
Body Weight (D001835)
Receptors, Cell Surface (D011956)
Twin Study (D018486)
Confidence Intervals (D016001)
cell surface (GO:0009986)
chromosome (GO:0005694)

Gene List • 2 Genes

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