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. 2023 Nov;34(11):1961-1973.
doi: 10.1007/s00198-023-06863-y. Epub 2023 Jul 26.

Comparison of anti-fracture effectiveness of zoledronate, ibandronate and alendronate versus denosumab in a registry-based cohort study

Judith Everts-Graber  1   2 Harald Bonel  3   4   5 Daniel Lehmann  6 Brigitta Gahl  7 HansJörg Häuselmann  8 Ueli Studer  9 Hans-Rudolf Ziswiler  9 Stephan Reichenbach  10   11 Thomas Lehmann  9
Affiliations

Comparison of anti-fracture effectiveness of zoledronate, ibandronate and alendronate versus denosumab in a registry-based cohort study

Judith Everts-Graber et al. Osteoporos Int. 2023 Nov.

Erratum in

Abstract

This registry-based study of 3068 patients with osteoporosis compared the anti-fracture effectiveness of denosumab versus bisphosphonates. Denosumab was associated with significantly greater risk reduction than alendronate or ibandronate for vertebral and any fractures. No difference in fracture risk reduction was found between zoledronate and denosumab.

Purpose: To analyse the fracture risk of patients with osteoporosis receiving bisphosphonates or denosumab in a real-world setting.

Methods: This registry-based cohort study evaluated patients taking denosumab, bisphosphonates or both sequentially. Fractures were analysed using rates, rate ratios and hazard ratios (HR), including both therapies as time-varying co-variates. Fracture risk hazards were adjusted (aHR) for baseline T-Scores and trabecular bone score (TBS) and were additionally analysed with inverse probability treatment weighting.

Results: A total of 3068 patients (89% female; median age at treatment onset, 69 years [63 to 76]) received denosumab (median duration 2.8 years, [2.2 to 4.7]), bisphosphonates (3.4 years, [2.1 to 5.7]) or both sequentially. Thus, 11,078 subject-years were assessed for bisphosphonates (41% alendronate, 36% ibandronate, 23% zoledronate) and 4216 for denosumab. Moreover, 48,375 subject-years were observed before treatment onset, in addition to 2593 years of drug holidays. A total of 1481 vertebral fractures (435 under therapy), 1508 non-vertebral fractures (499 under therapy) and 202 hip fractures (67 under therapy) occurred after age 50. The risks of vertebral, non-vertebral and hip fractures were significantly lower under all bisphosphonates, denosumab and drug holidays than before treatment onset (all p < 0.001). After adjusting for age, baseline T-scores and TBS, denosumab was associated with lower risk than alendronate or ibandronate for vertebral fractures (aHR 0.47 (0.35 to 0.64) and 0.70 [0.53 to 0.91], p < 0.001 and p = 0.009, respectively) and any fractures (aHR 0.62 [0.51 to 0.76] and 0.77 [0.64 to 0.92], p < 0.001 and p = 0.004). With propensity weighting, denosumab was associated with a lower hip fracture risk compared to alendronate (HR 0.54 [0.29 to 0.98], p = 0.044). No difference in fracture risk reduction (vertebral, non-vertebral or hip) was found between zoledronate and denosumab.

Conclusions: When adjusting for disease severity, denosumab was associated with significantly greater risk reduction than alendronate and ibandronate for vertebral fractures. No difference in fracture risk reduction was found between zoledronate and denosumab.

Keywords: Bisphosphonates; Denosumab; Fractures; Osteoporosis; Real-World.

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Conflict of interest statement

JE, DL, BG, SR and TL have nothing to declare and no conflicts of interest. HB received consultancy fees from Novartis. HJH received occasional speaker’s fees from Amgen, Sandoz, Eli Lilly and Labatec. HRZ received consultancy fees from Abbvie, Celgene, Amgen and Mylan/Viatris. US received congress and travel expenses from Sandoz, Pfizer and Janssen Pharmaceutica, and consultancy fees from Novartis and Amgen.

Figures

Fig. 1
Fig. 1
Fracture risk under denosumab versus bisphosphonates. This forest plot shows the fracture hazards (with 95% confidence intervals) under denosumab versus overall bisphosphonate therapy (A), ibandronate (B), alendronate (C) and zoledronate (D) with three statistical methods: Crude hazard ratios, adjusted hazard ratios (adjusted for age, BMD and TBS) and hazard ratios after inverse probability of treatment weighting. The crude and adjusted hazards considered all treatment sequences and all fractures, while the model using propensity weighting accounted for the first treatment sequence and time to first fracture. Abbreviations: BP: bisphosphonate, Dmab: denosumab, HR: hazard ratio, IPTW: inverse probability of treatment weighting
See this image and copyright information in PMC

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