Session Information
Date: Sunday, October 21, 2018
Title: Rheumatoid Arthritis – Treatments Poster I: Strategy and Epidemiology
Session Type: ACR Poster Session A
Session Time: 9:00AM-11:00AM
Background/Purpose: In patients (pts) with early (disease duration ≤24 months [mths]), MTX-naïve RA and poor prognostic factors including anti-citrullinated protein antibody (ACPA) positivity (+), abatacept (ABA) + MTX vs MTX was superior at achieving DAS28 (CRP) <2.6 at 12 mths.1,2 The AVERT-2 trial (clinicaltrials.gov, NCT02504268) further investigates the ability of ABA + MTX to induce validated metrics of remission in pts with ACPA+ early RA (disease duration ≤6 mths).
Methods: Pts were randomized (3:2) to double-blind, weekly SC ABA 125 mg + MTX vs MTX for 56 weeks (wks). Key inclusion criteria: age ≥18 years; RA diagnosis ≤6 mths (ACR/EULAR 2010 criteria); ACPA+; TJC and SJC ≥3; CRP >0.3 mg/dL (ULN)/ESR ≥28 mm/h; SDAI >11; DMARD naïve. Primary endpoint: proportion of pts in SDAI remission (SDAI ≤3.3) at Wk 24 in the first 375 pts randomized (primary analysis population). Hierarchically tested secondary endpoints: DAS28 (CRP) <2.6 at Wk 24 and SDAI ≤3.3 at Wk 52 (primary analysis population), and change from baseline (CfB) in total Sharp/van der Heijde score (SHS; X ray) and Boolean remission at Wk 52 (all randomized pts). Comparisons were made using logistic regression for binary outcomes and rank-based non-parametric analysis of covariance for X ray data.
Results: In the primary analysis population, 225 pts received ABA + MTX and 150 received MTX. Overall, 752 pts were randomized to ABA + MTX (n=451) and MTX (n=301); 63 and 68 discontinued, respectively, by Wk 52. Baseline characteristics were similar across treatment arms in each population (Table 1). The proportion of pts achieving SDAI ≤3.3 at Wk 24 was 21.3% for ABA + MTX and 16.0% for MTX (primary analysis population; p=0.2359; Table 2). Nominally significant benefits in favor of ABA + MTX were observed for all secondary endpoints including mean CfB in total SHS at Wk 52 in all randomized pts (0.5 vs 2.5; nominal p<0.0001; Table 2). Safety profiles were similar across treatment arms; no new safety signals were identified.
Conclusion: Abatacept + MTX vs MTX in ACPA+, early RA did not meet the primary endpoint of a statistically significant difference in SDAI ≤3.3 at Wk 24 in the primary analysis population, but did so at Wk 52. Consistent with previous studies,1,2 the benefits of abatacept + MTX vs MTX were seen for the composite endpoint of DAS28 (CRP) <2.6 at Wk 24 in the primary analysis population, and for the other secondary endpoints in all randomized pts.
References:
- Emery P, et al. Ann Rheum Dis 2015;74:19–26.
- Westhovens R, et al. Ann Rheum Dis 2009;68:1870–7.
Medical writing assistance provided by Sharon Gladwin, PhD (Caudex), funded by Bristol-Myers Squibb.
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Table 1. Baseline Characteristics |
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Primary analysis population (n=375) |
All randomized patients |
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ABA + MTX |
MTX monotherapy |
ABA + MTX |
MTX monotherapy |
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Age, years |
50 (13) |
50 (15) |
49 (13) |
49 (14) |
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Female, n (%) |
170 (75.6) |
121 (80.7) |
349 (77.4) |
243 (80.7) |
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RA duration, months |
1.3 (1.5) |
1.3 (1.4) |
1.2 (1.4) |
1.3 (1.4) |
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TJC (28 joints) |
13.8 (7.0) |
13.4 (6.7) |
13.2 (6.8) |
13.7 (6.8) |
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SJC (28 joints) |
10.4 (6.0) |
11.1 (5.9) |
10.0 (5.7) |
10.7 (5.9) |
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Pain |
66.2 (21.4) |
65.6 (22.6) |
66.5 (22.5) |
65.4 (22.4) |
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HAQ-DI |
1.6 (0.7) |
1.6 (0.6) |
1.6 (0.7) |
1.6 (0.7) |
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Patient Global Assessment |
65.3 (21.5) |
63.0 (23.7) |
65.7 (22.7) |
62.7 (24.1) |
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Physician Global Assessment |
66.3 (18.4) |
66.4 (20.6) |
65.1 (18.5) |
66.1 (19.8) |
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RF+, n (%) |
210 (93.3) |
136 (90.7) |
420 (93.1) |
279 (92.7) |
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CRP, mg/dL |
2.3 (3.1) |
1.9 (2.1) |
2.0 (2.7) |
1.9 (2.2) |
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DAS28 (CRP) |
5.7 (1.1) |
5.6 (1.0) |
5.6 (1.1) |
5.6 (1.0) |
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SDAI |
39.6 (14.7) |
39.6 (14.1) |
38.2 (14.1) |
39.4 (13.8) |
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Total SHS |
NC |
NC |
9.8 (16.3) |
13.0 (19.8) |
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CS* at Day 1, n (%) |
96 (42.7) |
52 (34.7) |
208 (46.1) |
93 (30.9) |
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Data are mean (SD) unless otherwise indicated *Oral and/or injectable |
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Table 2. Primary and Secondary Efficacy Endpoints |
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ABA + MTX |
MTX monotherapy |
Adjusted OR* (95% CI) |
p value |
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SDAI ≤3.3 at 24 weeks (primary analysis population) |
21.3 (48/225) |
16.0 |
1.4 (0.8, 2.5) |
0.2359 |
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DAS28 (CRP) <2.6 at 24 weeks (primary analysis population) |
38.7 (87/225) |
25.3 (38/150) |
1.9 (1.2, 3.1) |
0.0112† |
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SDAI ≤3.3 at 52 weeks (primary analysis population) |
29.8 (67/225) |
15.3 (23/150) |
2.3 (1.4, 4.0) |
0.0021† |
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Mean (SD) CfB in total SHS at 52 weeks (all randomized) |
0.5 (2.3) n=450 |
2.5 (6.2) n=300 |
– |
<0.0001† |
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Boolean remission at 52 weeks (all randomized) |
21.5 (97/451) |
11.6 (35/301) |
2.1 (1.4, 3.2) |
0.0006† |
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Data are % (n/N) unless otherwise indicated For binary outcomes, patients with missing values due to discontinuation or other reasons and those who took a high dose of corticosteroids within 42 days of the 12-month assessment were imputed as non-remitters |
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To cite this abstract in AMA style:
Emery P, Tanaka Y, Bykerk VP, Huizinga TWJ, Citera G, Nys M, Connolly SE, Johnsen A, Fleischmann R. Efficacy and Safety of Abatacept in Combination with MTX in Early, MTX-Naïve, Anti-Citrullinated Protein Antibody–Positive Patients with RA: Primary and 1-Year Results from a Phase IIIb Study [abstract]. Arthritis Rheumatol. 2018; 70 (suppl 9). https://acrabstracts.org/abstract/efficacy-and-safety-of-abatacept-in-combination-with-mtx-in-early-mtx-naive-anti-citrullinated-protein-antibody-positive-patients-with-ra-primary-and-1-year-results-from-a-phase-iiib-study/. Accessed .« Back to 2018 ACR/ARHP Annual Meeting
ACR Meeting Abstracts - https://acrabstracts.org/abstract/efficacy-and-safety-of-abatacept-in-combination-with-mtx-in-early-mtx-naive-anti-citrullinated-protein-antibody-positive-patients-with-ra-primary-and-1-year-results-from-a-phase-iiib-study/