β3-adrenergic receptor gene, body mass index, bone mineral density and fracture risk in elderly men and women: The Dubbo Osteoporosis Epidemiology Study (DOES)

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Abstract

Background: Recent studies have suggested that the Arg allele of β3-adrenergic receptor (ADRB3) gene is associated with body mass index (BMI), which is an important predictor of bone mineral density (BMD) and fracture risk. However, whether the ADRB3 gene polymorphism is associated with fracture risk has not been investigated. The aim of study was to examine the inter-relationships between ADRB3 gene polymorphisms, BMI, BMD and fracture risk in elderly Caucasians. Methods: Genotypes of the ADRB3 gene were determined in 265 men and 446 women aged 60+ in 1989 at entry into the study, whose BMD were measured by DXA (GE Lunar, WI USA) at baseline. During the follow-up period (between 1989 and 2004), fractures were ascertained by reviewing radiography reports and personal interviews. Results: The allelic frequencies of the Trp and the Arg alleles were 0.925 and 0.075 respectively, and the relative frequencies of genotypes Trp/Trp, Trp/Arg and Arg/Arg 0.857, 0.138 and 0.006 respectively. There was no significant association between BMI and ADRB3 genotypes (p = 0.10 in women and p = 0.68 in men). There was also no significant association between ADRB3 genotypes and lumbar spine or femoral neck BMD in either men and women. Furthermore, there were no significant association between ADRB3 genotypes and fracture risk in both women and men, either before or after adjusting for and, BMD and BMI. Conclusion: The present data suggested that in Caucasian population the contribution of ADRB3 genotypes to the prediction of BMI, BMD and fracture risk is limited. © 2006 Wang et al; licensee BioMed Central Ltd.

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Wang, C. Y., Nguyen, N. D., Morrison, N. A., Eisman, J. A., Center, J. R., & Nguyen, T. V. (2006). β3-adrenergic receptor gene, body mass index, bone mineral density and fracture risk in elderly men and women: The Dubbo Osteoporosis Epidemiology Study (DOES). BMC Medical Genetics, 7. https://doi.org/10.1186/1471-2350-7-57

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