Pharmacogenomic Effects of β-Blocker Use on Femoral Neck Bone Mineral Density

Author:

Nevola Kathleen T1,Nagarajan Archana12,Hinton Alexandra C2ORCID,Trajanoska Katerina34,Formosa Melissa M56,Xuereb-Anastasi Angela56,van der Velde Nathalie7ORCID,Stricker Bruno H4,Rivadeneira Fernando34,Fuggle Nicholas R8,Westbury Leo D9,Dennison Elaine M810,Cooper Cyrus8911,Kiel Douglas P1213ORCID,Motyl Katherine J14,Lary Christine W2ORCID

Affiliation:

1. Graduate School of Biomedical Sciences, Tufts University, Boston, MA, 02111, USA

2. Center for Outcomes Research and Evaluation, Maine Medical Center Research Institute, Portland, ME 04101, USA

3. Department of Internal Medicine, Erasmus MC, University Medical Center, Rotterdam 3015 GD, the Netherlands

4. Department of Epidemiology, Erasmus MC, University Medical Center, Rotterdam 3015 GD, the Netherlands

5. Department of Applied Biomedical Science, Faculty of Health Sciences, University of Malta, Msida MSD 2080, Malta

6. Centre for Molecular Medicine and Biobanking, MSD 2080, Malta

7. Department of Internal Medicine, Geriatrics, Amsterdam Public Health Research Institute, Amsterdam University Medical Center, Amsterdam, 1105 AZ, the Netherlands

8. MRC Lifecourse Epidemiology Unit, University of Southampton, Southampton, SO16 6YD, UK

9. NIHR Southampton Biomedical Research Centre, University of Southampton and University Hospital Southampton NHS Foundation Trust, Southampton, UK

10. Victoria University of Wellington, Wellington, New Zealand

11. NIHR Oxford Biomedical Research Centre, University of Oxford, Oxford, UK

12. Department of Medicine, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA 02215, USA

13. Hinda and Arthur Marcus Institute for Aging Research Hebrew SeniorLife, Boston, MA 02131, USA

14. Center for Molecular Medicine, Maine Medical Center Research Institute, Maine Medical Center, Scarborough, ME 04074, USA

Abstract

Abstract Context Recent studies have shown that β-blocker (BB) users have a decreased risk of fracture and higher bone mineral density (BMD) compared to nonusers, likely due to the suppression of adrenergic signaling in osteoblasts, leading to increased BMD. There is also variability in the effect size of BB use on BMD in humans, which may be due to pharmacogenomic effects. Objective To investigate potential single-nucleotide variations (SNVs) associated with the effect of BB use on femoral neck BMD, we performed a cross-sectional analysis using clinical data, dual-energy x-ray absorptiometry, and genetic data from the Framingham Heart Study’s (FHS) Offspring Cohort. We then sought to validate our top 4 genetic findings using data from the Rotterdam Study, the BPROOF Study, the Malta Osteoporosis Fracture Study (MOFS), and the Hertfordshire Cohort Study. Methods We used sex-stratified linear mixed models to determine SNVs that had a significant interaction effect with BB use on femoral neck (FN) BMD across 11 gene regions. We also evaluated the association of our top SNVs from the FHS with microRNA (miRNA) expression in blood and identified potential miRNA-mediated mechanisms by which these SNVs may affect FN BMD. Results One variation (rs11124190 in HDAC4) was validated in females using data from the Rotterdam Study, while another (rs12414657 in ADRB1) was validated in females using data from the MOFS. We performed an exploratory meta-analysis of all 5 studies for these variations, which further validated our findings. Conclusion This analysis provides a starting point for investigating the pharmacogenomic effects of BB use on BMD measures.

Funder

National Institutes of Health

Framingham Contract Number

The Netherlands Organization for Health Research and Development

Ministry of Economic Affairs, Agriculture and Innovation

Medical Research Council University Unit Partnership

Publisher

The Endocrine Society

Subject

Endocrinology, Diabetes and Metabolism

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