A Meta-Analysis of Osteoporotic Fracture Risk with Medication Nonadherence

Abstract Objectives Therapy for osteoporosis reduces the risk of fracture in clinical trials; real-world adherence to therapy is suboptimal and may reduce the effectiveness of intervention. The objective was to assess the fracture risk among patients nonadherent versus adherent to therapy for osteop...

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Bibliographic Details
Published in:Value in health 2011-06, Vol.14 (4), p.571-581
Main Authors: Ross, Susan, MD, FRCPC, Samuels, Ebony, PhD, Gairy, Kerry, MSc, Iqbal, Sheikh, MD, MPH, MBA, Badamgarav, Enkhe, MD, MPH, Siris, Ethel, MD
Format: Article
Language:English
Subjects:
adherence
Case-Control Studies
compliance
fracture
Fractures, Bone - drug therapy
Fractures, Bone - epidemiology
Fractures, Bone - etiology
Humans
Internal Medicine
Medication Adherence - statistics & numerical data
meta-analysis
osteoporosis
Osteoporosis - complications
Osteoporosis - drug therapy
Osteoporosis - epidemiology
Osteoporotic Fractures - drug therapy
Osteoporotic Fractures - epidemiology
Osteoporotic Fractures - etiology
Patient Compliance - statistics & numerical data
Prospective Studies
Retrospective Studies
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Summary:Abstract Objectives Therapy for osteoporosis reduces the risk of fracture in clinical trials; real-world adherence to therapy is suboptimal and may reduce the effectiveness of intervention. The objective was to assess the fracture risk among patients nonadherent versus adherent to therapy for osteoporosis. Methods Medline, Embase, and CINAHL were searched for English-language publications of observational studies (January 1998–February 2009). Proceedings from two recent meetings of five relevant conferences were hand searched. Prospective and retrospective observational studies of patients with osteoporosis receiving bisphosphonates, parathyroid hormone, or selective estrogen receptor modulators denosumab were included. Studies were required to consider both fracture risk and adherence (compliance and/or persistence); any definition of adherence/fracture was acceptable. Data were analyzed using pooled comparisons of the odds and hazard ratios of fracture in noncompliance versus compliance and nonpersistence versus persistence. Sensitivity analyses were conducted to determine the effect of clinical heterogeneity on the results. Results Twenty-seven citations were identified, the majority of which were retrospective database analyses considering the effect of adherence to bisphosphonate therapy on fracture at any skeletal site. The absolute frequency of fracture ranged from 6% to 38% with noncompliance and from 5% to 19% with nonpersistence (104–159 weeks). Meta-analysis indicates that fracture risk increases by approximately 30% with noncompliance (odds ratio [95% confidence interval] 1.29 [1.22–1.38]; hazard ratio 1.28 [1.18–1.38]) and by 30% to 40% with nonpersistence (odds ratio 1.40 [1.29–1.52]; hazard ratio 1.32 [1.23–1.42]). Conclusions Poor medication adherence is associated with a significantly increased risk of fracture versus optimal adherence. Improving medication adherence in patients with osteoporosis may lead to a greater reduction in fracture.
ISSN:1098-3015
1524-4733
DOI:10.1016/j.jval.2010.11.010