ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 1028

Discontinuation of Denosumab and Associated Vertebral Fracture Incidence: Analysis from a Phase 3 Placebo-Controlled Study of Denosumab and Its Open-Label Extension

Jacques P Brown1, S Ferrari2, N Gilchrist3, Jens-Erik Beck Jensen4, N Pannacciulli5, Chris Recknor6, Christian Roux7, Shawna Smith5, Ove Törring8, Ivo Valter9, Rachel B Wagman5, A Wang5 and SR Cummings10, 1Centre Hospitalier de l'Université Laval (CHUL), Quebec City, QC, Canada, 2Geneva University Hospital, Geneva, Switzerland, 3The Princess Margaret Hospital, Christchurch, New Zealand, 4Hvidovre University Hospital, Hvidovre, Denmark, 5Amgen Inc., Thousand Oaks, CA, 6United Osteoporosis Centers, Gainesville, GA, 7Paris Descartes University, Paris, France, 8Karolinska Institutet Sodersjukhuset, Stockholm, Sweden, 9Center for Clinical and Basic Research, Tallinn, Estonia, 10SFCC, CPMC Research Institute & UCSF, San Francisco, CA

Meeting: 2016 ACR/ARHP Annual Meeting

Date of first publication: September 28, 2016

Keywords: , , ,

Session Information

Date: Sunday, November 13, 2016

Title: Osteoporosis and Metabolic Bone Disease – Clinical Aspects and Pathogenesis

Session Type: ACR Concurrent Abstract Session

Session Time: 4:30PM-6:00PM

Background/Purpose: Denosumab (DMAb) treatment has been shown to decrease fracture (Fx) risk. Unlike bisphosphonates, DMAb is a monoclonal antibody against RANKL. Discontinuation is characterized by reversal of effect, including transient increases in bone turnover markers to above-baseline (BL) levels returning to BL within 2 yr and loss of bone mineral density (BMD) to BL levels. An analysis from FREEDOM showed similar subject incidence of Fx in DMAb and placebo (PBO) groups upon discontinuation. Recent reports describe isolated cases of multiple (≥2) vertebral Fx (VFx) after DMAb cessation (Aubrey-Rozier OI 2015; Anastasilakis OI 2015; Popp OI 2016). To better understand VFx incidence—particularly multiple VFx—upon DMAb cessation, we describe VFx risk and possible determinants in subjects who discontinued DMAb during the 3-yr FREEDOM or 7-yr Extension.

Methods: Subjects who received ≥2 doses of investigational product (IP; DMAb 60 mg Q6M or PBO) and discontinued IP but stayed in study ≥7 M after the last dose were included in the analysis. Subjects who discontinued DMAb from FREEDOM or Extension were analyzed as one group. A logistic regression model explored covariates related to off-treatment new VFx or multiple new VFx.

Results: Of 1001 subjects who discontinued DMAb during FREEDOM or Extension, 56 (5.6%) sustained new VFx. Upon DMAb discontinuation, new VFx incidence increased relative to the on-treatment period but stayed within the range of those who discontinued PBO, ie, had never been treated (Table). The same pattern was seen in subjects with prior VFx, who had higher on- and off-treatment VFx rates than the overall population. Among subjects with off-treatment new VFx, a greater percentage of those who discontinued DMAb (34/56 [60.7%]) than PBO (10/29 [34.5%]) sustained multiple new VFx. Logistic regression models found prior VFx before or during treatment to be the strongest predictor of off-treatment new VFx, including multiple VFx (odds ratio 2.1-3.4). Off-treatment femoral neck BMD loss was a weak covariate.

Conclusion: Discontinuation of DMAb is associated with an increase in VFx rate to levels comparable to PBO. Among subjects who sustained new VFx after DMAb cessation, there was a greater incidence of multiple new VFx than in PBO. Subjects with prior VFx are at high risk for off-treatment new VFx and should continue osteoporosis therapy. Consequently those who discontinue DMAb should transition to another therapy after the 6-M dosing interval. Table. Off-treatment vertebral fracture incidence in subjects who discontinued IP in FREEDOM or its Extension

 

FREEDOM

FREEDOM + Extension

Placebo

Denosumab

All subjects

N = 470

N = 1,001

Off-treatment new VFx, n (%)

29 (6.2%)

56 (5.6%)

Off-treatment multiple new VFX, n (%) [among all subjects]

10 (2.1%)

34 (3.4%)

Off-treatment multiple new VFX, n (%) [among all subjects with new VFx]

10 (34.5%)

34 (60.7%)

On-treatment new VFx (per 100 subject-years)

7.0

1.2

Off-treatment new VFx (per 100 subject-years)

8.0

7.1

Subjects with prior VFx before treatment

N = 122 (26%)

N = 255 (25%)

Off-treatment new VFx, n (%)

12 (9.8%)

19 (7.5%)

Off-treatment multiple new VFx, n (%) [among subjects with prior VFx]

5 (4.1%)

15 (5.9%)

Off-treatment multiple new VFx, n (%) [among subjects with prior VFx and new VFx]

5 (41.7%)

15 (78.9%)

On-treatment new VFx (per 100 subject-years)

11.6

1.9

Off-treatment new VFx (per 100 subject-years)

14.4

12.1

 

Disclosure: J. P. Brown, Amgen Inc., Eli Lilly, 2,Amgen Inc., Eli Lilly, Merck, 5,Amgen Inc., Eli Lilly, 8; S. Ferrari, MSD, 2,Amgen Inc., MSD, 5; N. Gilchrist, Amgen Inc., Merck Sharpe Dohme, Pfizer, 2,Canterbury District Health Board, 3,Trustee, 6; J. E. B. Jensen, Eli Lilly and Company, 2,Amgen Inc., Eli Lilly, Merck, 6,Amgen Inc., Elil Lilly, Gilead, Merck, 8; N. Pannacciulli, Amgen Inc., 1,Amgen Inc., 3; C. Recknor, None; C. Roux, MSD, Ultragenyx, 2,Amgen Inc., Alexion, MSD, UCB, 5; S. Smith, Amgen Inc., 1,Amgen Inc., 3; O. Törring, Takeda, 5,Amgen Inc., Genzyme, MEDA, 8; I. Valter, None; R. B. Wagman, Amgen Inc., 1,Amgen Inc., 3; A. Wang, Amgen Inc., 1,Amgen Inc., 3; S. Cummings, Amgen Inc., Merck, Radius, 5.

To cite this abstract in AMA style:

Brown JP, Ferrari S, Gilchrist N, Jensen JEB, Pannacciulli N, Recknor C, Roux C, Smith S, Törring O, Valter I, Wagman RB, Wang A, Cummings S. Discontinuation of Denosumab and Associated Vertebral Fracture Incidence: Analysis from a Phase 3 Placebo-Controlled Study of Denosumab and Its Open-Label Extension [abstract]. Arthritis Rheumatol. 2016; 68 (suppl 10). https://acrabstracts.org/abstract/discontinuation-of-denosumab-and-associated-vertebral-fracture-incidence-analysis-from-a-phase-3-placebo-controlled-study-of-denosumab-and-its-open-label-extension/. Accessed .

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