Practical guidance for the management of aromatase inhibitor-associated bone loss

doi:10.1093/annonc/mdn164

Annals of Oncology Advance Access originally published online on April 29, 2008
Annals of Oncology 2008 19(8):1407-1416; doi:10.1093/annonc/mdn164

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© The Author 2008. Published by Oxford University Press on behalf of the European Society for Medical Oncology. All rights reserved. For permissions, please email: journals.permissions@oxfordjournals.org

breast cancer

Practical guidance for the management of aromatase inhibitor-associated bone loss

P. Hadji¹^,*, J. -J. Body², M. S. Aapro³, A. Brufsky⁴, R. E. Coleman⁵, T. Guise⁶, A. Lipton⁷ and M. Tubiana-Hulin⁸

¹ Department of Gynecology, Philipps-University of Marburg, Marburg, Germany
² CHU Brugmann and Institute J. Bordet, Université Libre de Bruxelles, Brussels, Belgium
³ Institut Multidisciplinaire d'Oncologie Clinique de Genolier, Genolier, Switzerland
⁴ Division of Hematology and Oncology, University of Pittsburgh Cancer Institute, Pittsburgh, Pennsylvania, USA
⁵ Cancer Research Centre, Weston Park Hospital, University of Sheffield, Sheffield, UK
⁶ Department of Medicine, Division of Endocrinology, University of Virginia, Charlottesville, Virginia, USA
⁷ Milton S. Hershey Medical Center, Pennsylvania State University, Hershey, Pennsylvania, USA
⁸ Centre René Huguenin, St Cloud, France

^* Correspondence to: Dr P. Hadji, Philipps-University of Marburg, Baldingerstrasse 35033 Marburg, Germany. Tel: +49-6421-28-66486; Fax: +49-6421-28-67070; E-mail: hadji{at}med.uni-marburg.de

Background: Recent studies indicate that women with breast cancerare at increased risk of fracture compared with their age-matchedpeers. Current treatment guidelines are inadequate for avertingfractures in osteopenic women, especially those receiving aromataseinhibitor (AI) therapy. Therefore, we sought to identify clinicallyrelevant risk factors for fracture that can be used to assessoverall fracture risk and to provide practical guidance forpreventing and treating bone loss in women with breast cancerreceiving AI therapy.

Methods: Systematic review of pertinent information from publishedliterature and meeting abstracts through December 2007 was carriedout to identify factors contributing to fracture risk in womenwith breast cancer. An evidence-based medicine approach wasused to select risk factors that can be used to determine whento initiate bisphosphonate treatment of aromatase inhibitor-associatedbone loss (AIBL).

Results: Fracture risk factors were chosen from large, well-designed,controlled, population-based trials in postmenopausal women.Evidence from multiple prospective clinical trials in womenwith breast cancer was used to validate AI therapy as a fracturerisk factor. Overall, eight fracture risk factors were validatedin women with breast cancer: AI therapy, T-score <–1.5,age >65 years, low body mass index (BMI <20 kg/m²), familyhistory of hip fracture, personal history of fragility fractureafter age 50, oral corticosteroid use >6 months, and smoking.Treatment recommendations were derived from randomized clinicaltrials.

Conclusions: The authors recommend the following for preventingand treating AIBL in women with breast cancer. All patientsinitiating AI therapy should receive calcium and vitamin D supplements.Any patient initiating or receiving AI therapy with a T-score $≥$ –2.0 and no additional risk factors should be monitoredevery 1–2 years for change in risk status and bone mineraldensity (BMD). Any patient initiating or receiving AI therapywith a T-score <–2.0 should receive bisphosphonatetherapy. Any patient initiating or receiving AI therapy withany two of the following risk factors—T-score <–1.5,age >65 years, low BMI (<20 kg/m²), family history ofhip fracture, personal history of fragility fracture after age50, oral corticosteroid use >6 months, and smoking—shouldreceive bisphosphonate therapy. BMD should be monitored every2 years, and treatment should continue for at least 2 yearsand possibly for as long as AI therapy is continued. To date,the overwhelming majority of clinical evidence supports zoledronicacid 4 mg every 6 months to prevent bone loss in women at highrisk. Although there is a trend towards fewer fractures withzoledronic acid, studies completed to date have not been designedto capture significant differences in fracture rate, and longerfollow-up is needed.

Key words: Fractune risk, zoledronic acid, biophoephonates, treatment recommendations, postmenopausal

Received for publication February 4, 2008. Revision received March 17, 2008. Accepted for publication March 18, 2008.

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