ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 886

Efficacy and Safety of Switching from Adalimumab to Baricitinib: Long-Term Data from Phase 3 Extension Study in Patients with Rheumatoid Arthritis

Michael E Weinblatt1, Peter C. Taylor2, Edward C. Keystone3, Robert A. Ortmann4, Maher Issa4, Li Xie4, Stephanie de Bono4 and Yoshiya Tanaka5, 1Brigham and Women’s Hospital, Boston, MA, 2Botnar Research Centre, Univ of Oxford, Oxford, United Kingdom, 3Mount Sinai Hospital, Toronto, ON, Canada, 4Eli Lilly and Company, Indianapolis, IN, 5University of Occupational and Environmental Health, Kitakyushu, Japan

Meeting: 2018 ACR/ARHP Annual Meeting

Keywords:

Session Information

Date: Sunday, October 21, 2018

Title: 3S087 ACR Abstract: RA–Treatments I: JAK Inhibitors (886–891)

Session Type: ACR Concurrent Abstract Session

Session Time: 2:30PM-4:00PM

Background/Purpose: Baricitinib (bari) is an oral JAK1/JAK2 inhibitor approved for the treatment of moderately to severely active RA in adults in over 40 countries, including European countries, the United States, and Japan. In the 52-week Phase 3 RA-BEAM study, bari 4-mg once daily (QD) showed clinical improvements compared with placebo (PBO) and with adalimumab (ADA) in MTX-inadequate-responder (IR) patients (pts).1 The objective of this analysis was to evaluate efficacy, patient-reported outcomes (PRO), and safety in pts from RA-BEAM who switched treatment from ADA to bari after entering a long-term extension (LTE) study (RA-BEYOND).

Methods: In RA-BEAM (completed September 2015), 1305 pts were randomized 3:3:2 to PBO, bari 4-mg QD, or ADA 40-mg every 2 weeks (wks). At wk 52, pts could enter the LTE, where all pts received open-label bari 4-mg but remained blinded to randomized treatment in RA-BEAM. No ADA washout period was applied. Efficacy, PROs, and safety were evaluated in pts who were not rescued in RA-BEAM and entered the LTE ≥48 wks before the data cutoff of April 1, 2017.

Results: Among pts who completed RA-BEAM without rescue, 381/394 (97%) bari (continued bari), and 238/241 (99%) ADA (switched to bari) pts entered the LTE ≥48 wks before the cutoff date and were included in the analysis. Pts who switched from ADA to bari showed improvements in disease control through 24 wks post-switch in the LTE without evidence of worsening through the following 24 wks (Table 1) and showed further small improvements in PRO assessment of pain and physical function (HAQ-DI) through wk 48 (Figure 1). Of pts who were nonresponders (CDAI >10) at the time of switch (107 and 74 in bari and ADA groups, respectively) approximately half reached low disease activity (CDAI ≤10) by wk 48 (54% and 50%, respectively). Exposure-adjusted incidence rates for treatment-emergent adverse events (TEAEs) and infections, including serious AEs, were similar for pts who switched from ADA to bari and those who continued bari (Table 2).

Conclusion: Switching from ADA to bari without ADA washout was associated with maintenance of disease control through 48 wks post-switch, with some nonresponders being able to achieve LDA as well. There was no increase in TEAEs or serious AEs or infections.

Reference: 1 Taylor PC et al. NEJM, 2017;376:652-62

 

 

Table 1. Percent of patients who reached low disease activity and remission at weeks 24 and 48 after entering the LTE RA-BEYOND study for patients switched to baricitinib

 

Baricitinib to Baricitinib

Adalimumab to Baricitinib

Week 0

Week 24

Week 48

Week 0

Week 24

Week 48

CDAI

 

 

 

 

 

 

     ≤10

273 (71.8)

292 (76.8)

297 (78.2)

164 (68.9)

176 (73.9)

175 (73.5)

     ≤2.8

104 (27.4)

117 (30.8)

120 (31.6)

58 (24.4)

72 (30.3)

67 (28.2)

SDAI

 

 

 

 

 

 

     ≤11

273 (71.8)

296 (77.9)

300 (78.9)

164 (68.9)

181 (76.1)

172 (72.3)

     ≤3.3

108 (28.4)

125 (32.9)

127 (33.4)

59 (24.8)

73 (30.7)

68 (28.6)

DAS28-ESR

 

 

 

 

 

 

     ≤3.2

188 (49.5)

181 (47.6)

203 (53.4)

120 (50.4)

138 (58.0)

120 (50.4)

     <2.6

111 (29.2)

102 (26.8)

128 (33.7)

71 (29.8)

80 (33.6)

71 (29.8)

CDAI, Clinical Disease Activity Index; DAS28-ESR, Disease Activity Score 28-joint count erythrocyte sedimentation rate; LTE, long-term extension; SDAI, Simple Disease Activity Index. Baricitinib to Baricitinib = Patients completing RA-BEAM (Week 52) on baricitinib who continued baricitinib in RA-BEYOND. Adalimumab to Baricitinib = Patients completing RA-BEAM on adalimumab who transitioned to baricitinib (week 52) upon entering the LTE. Week 0 = Baseline of LTE. Data are n (%) using non-responder imputation for missing data

 

 

Table 2. Safety through 48 weeks after switch to baricitinib upon entry to RA-BEYOND

 

Baricitinib to Baricitinib
(n = 381; PYE = 262.0)

Adalimumab to Baricitinib
(n = 238; PYE = 224.0)

Patients with ≥1 TEAE

211 (55.4) [80.5]

162 (68.1) [72.3]

     Infections

104 (27.3) [39.7]

87 (36.6) [38.8]

          Herpes zoster

6 (1.6) [2.3]

5 (2.1) [2.2]

     Gastrointestinal disorders

41 (10.8) [15.6]

29 (12.2) [12.9]

AEs that led to permanent study drug discontinuation

7 (1.8) [2.7]

6 (2.5) [2.7]

Patients with ≥1 SAE

32 (8.4) [12.2]

18 (7.6) [8.0]

     Serious infections

10 (2.6) [3.8]

5 (2.1) [2.2]

AE, adverse event; EAIR, exposure-adjusted incidence rate; PYE, patient-years of exposure; SAE, serious adverse event; TEAE, treatment-emergent adverse event.
Data are n (%) [EAIR].

 

Disclosure: M. E. Weinblatt, Amgen, BMS, Crescendo Bioscience, Sanofi/Regeneron, 2,Abbvie, Amgen, BMS, Crescendo Bioscience, Corrono, GSK, Gilead, Eli Lilly and Company, Lycera, Merck, Novartis, Pfizer, Roche, Samsung, Set Point, UCB, 5,Lycero, Can-fite, Scipher, Vorso, Inmedix, 1; P. C. Taylor, Celgene, Eli Lilly and Company, Galapagos, UCB, 2,AbbVie, Eli Lilly and Company, Galapagos, GlaxoSmithKline, Pfizer, UCB, Biogen, Sandoz, Novartis, Janssen, 5; E. C. Keystone, AbbVie, Amgen, Bristol-Myers Squibb, F. Hoffmann-La Roche Inc, Gilead, Janssen Inc, Eli Lilly and Company, Pfizer Pharmaceuticals, Sanofi-Aventis, 2,AbbVie, Amgen, AstraZeneca Pharma, Biotest, Bristol-Myers Squibb Company, Celltrion, Crescendo Bioscience, F. Hoffmann-La Roche Inc, Genentech Inc, Gilead, Janssen Inc, Eli Lilly and Company, Merck, Pfizer Pharmaceuticals, Sandoz, UCB, 5, 9,Amgen, AbbVie, Bristol-Myers Squibb Canada, F. Hoffmann-La Roche Inc., Janssen Inc., Merck, Pfizer Pharmaceuticals, Sanofi Genzyme, UCB, 8; R. A. Ortmann, Eli Lilly and Company, 1, 3; M. Issa, Eli Lilly and Company, 1, 3; L. Xie, Eli Lilly and Company, 1, 3; S. de Bono, Eli Lilly and Company, 1, 3; Y. Tanaka, Mitsubishi-Tanabe, Bristol-Myers, Eisai, Chugai, Takeda, Abbvie, Astellas, Daiichi-Sankyo, Ono, MSD, Taisho-Toyama, 2,Daiichi-Sankyo, Astellas, Eli Lilly, Chugai, Sanofi, Abbvie, Pfizer, YL Biologics, Bristol-Myers, Glaxo-Smithkline, UCB, Mitsubishi-Tanabe, Novartis, Eisai, Takeda, Janssen, Asahi-kasei, 5.

To cite this abstract in AMA style:

Weinblatt ME, Taylor PC, Keystone EC, Ortmann RA, Issa M, Xie L, de Bono S, Tanaka Y. Efficacy and Safety of Switching from Adalimumab to Baricitinib: Long-Term Data from Phase 3 Extension Study in Patients with Rheumatoid Arthritis [abstract]. Arthritis Rheumatol. 2018; 70 (suppl 9). https://acrabstracts.org/abstract/efficacy-and-safety-of-switching-from-adalimumab-to-baricitinib-long-term-data-from-phase-3-extension-study-in-patients-with-rheumatoid-arthritis/. Accessed .

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