Genetic determinants of bone mass in adult women:​ a reevaluation of the twin model and the potential importance of gene interaction on heritability estimates

Slemenda, Charles W.<sup>1,2</sup>; Christian, Joe C.<sup>3</sup>; Williams, Christopher J.<sup>3</sup>; Norton, James A.<sup>4</sup>; Johnston, Jr, C. Conrad<sup>1</sup>

Affiliations

¹Department of Medicine, Indiana University School of Medicine, Indianapolis

²Regenstrief Institute for Health Care, Indiana University School of Medicine, Indianapolis

³Department of Medical Genetics, Indiana University School of Medicine, Indianapolis

⁴Department of Psychiatry, Indiana University School of Medicine, Indianapolis

Abstract

We estimated genetic effects on bone density in pre- and postmenopausal twins and critically considered the assumptions of the twin model. Bone mass in the radius, lumbar spine, and hip, anthropometric measurements, usual calcium and caffeine intake, tobacco and alcohol use, number of pregnancies and live births, menstrual history, usual physical activity, and medical history were measured in a volunteer sample of 171 twin pairs [124 monozygotic (MZ) and 47 dizygotic (DZ)], aged 25–80, free of diseases known to affect bone mass or mineral metabolism. At all skeletal sites, MZ intraclass correlations exceeded DZ correlations for both pre- and postmenopausal women, yielding highly significant estimates of heritability for bone mass. Adjustments for height, age, and environmental characteristics did not reduce the heritability estimates. However, many of these estimates were unrealistically high, suggesting some violation(s) of the assumptions of the twin model. Thus, the familial resemblance in bone mass is due primarily to genetic effects at all skeletal sites and at all ages, although the importance of genetic effects is diminished with aging, as evidenced by increasing within-MZ pair variability in older women. Because of failures in the assumptions of the twin model, however, particularly the greater MZ environmental similarity and the probability of gene interaction, heritability estimates are probably too high and require cautious interpretation.

Links

DOI: 10.1002/jbmr.5650060606

PubMed: 1887818

WoS: A1991GN78700005

History

Received: 1990-04-28

Revised: 1990-11-29

Accepted: 1990-12-26

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Cited By (23)

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2020	Liu H, Zhao H, Lin H, Li Z, Xue H, Zhang Y, Lu J. Relationship of COL9A1 and SOX9 genes with genetic susceptibility of postmenopausal osteoporosis. Calcif Tiss Int. March 2020;106(3):248-255.
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