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B-vitamin status and the MTHFR 677C→T polymorphism as determinants of bone health in older Irish women from the TUDA ageing cohort study

Published online by Cambridge University Press:  24 September 2014

M. M. Clarke
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
M. Ward
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
L. Hoey
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
J. J. Strain
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
A. Molloy
Affiliation:
School of Medicine, Trinity College Dublin 2, Ireland
E. Laird
Affiliation:
School of Medicine, Trinity College Dublin 2, Ireland
M. Healy
Affiliation:
The Department of Clinical Biochemistry, Central Pathology, St James's Hospital, Dublin, Ireland
M. C. Casey
Affiliation:
The Mercers Institute for Research on Ageing, St James's Hospital, Dublin, Ireland
C. Cunningham
Affiliation:
The Mercers Institute for Research on Ageing, St James's Hospital, Dublin, Ireland
M. T. McCann
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
H. McNulty
Affiliation:
Northern Ireland Centre for Food and Health, University of Ulster, Coleraine, BT52 1SA
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Abstract

Type
Abstract
Copyright
Copyright © The Authors 2014 

Osteoporosis, an increasingly common skeletal disorder characterised by reduced bone mineral density (BMD) and an increased risk of fragility fracture, is associated with increased morbidity and mortality( Reference Strom, Borgstrom and Kanis 1 ). In recent years, B-vitamins involved in 1-carbon metabolism (i.e. folate, vitaminsB12, B6 and riboflavin) have been linked with bone health outcomes. Findings, however, have been somewhat discordant among studies( Reference vanWijngaarden, Doets and Szczecinska 2 ). The aim of this investigation was to examine biomarker status of the B-vitamins and the common 677C→T polymorphism in the gene encoding the folate metabolising enzyme methylenetetrahydrofolatereductase (MTHFR), as determinants of low BMD.

Female participants (n1, 904) recruited to the Trinity Ulster Department of Agriculture (TUDA) ageing cohort study, and with BMD measured by dual energy X-ray absorptiometry scans, were investigated. Low BMD was defined as a combination of osteopenia (a T-Score between –1 and –2.5 SD) and osteoporosis (a T-Score of -2.5 SD or less).B-vitamin biomarker analysis was performed at Trinity College Dublin and the University of Ulster.

An increased risk of low BMD was significantly associated with age (β = 0.062, p < 0.001), physical inactivity (β = 0.483, p = 0.004), weight (β = − 0.056, p < 0.001),and parathyroid hormone (β = 0.011, p = 0.004), but not serum 25-hydroxyvitamin D. Women in the lowest tertile of riboflavin status, or the highest tertile of homocysteine, had a significantly increased risk of low BMD, after adjustment for covariates (Table). The MTHFR 677TT genotype was associated with an increased risk of low BMD. This genotype combined with low status of riboflavin was associated with a 1.9 times increased risk of low BMD, compared to those with high vitamin status and the CC/CT genotypes combined (Table).

Analysis by logistic regression, comparing the lowest tertile of vitamin status (or the highest tertile of homocysteine) to the other tertiles combined, used to determine predictors of low BMD (osteopenia and osteoporosis combined) with adjustment for covariates.

These findings suggest that perturbations of 1-carbon metabolism may have adverse effects on bone health, while optimal B-vitamin status may be protective.

Acknowledgement of Funding: Food for Health Research Initiative of the Irish Department of Agriculture and Health Research Board, with co-funding from the Department for Employment and Learning Northern Ireland under its Cross-Border Research and Development Programme: “Strengthening the all-Island Research Base”.

References

1. Strom, O, Borgstrom, F, Kanis, JA et al. (2011) ArchOsteoporos 6, 59155.Google Scholar
2. vanWijngaarden, JP, Doets, EL, Szczecinska, A et al. (2013) JNutrMetab 486186.Google Scholar