ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 2271

Safety of Adalimumab±Methotrexate for the Treatment of Polyarticular Juvenile Idiopathic Arthritis (pJIA)

Hermine I. Brunner1, Nicola Ruperto2, Kabita Nanda3, Mary Toth4, Ivan Foeldvari5, John F. Bohnsack6, Diana Milojevic7, C. Egla Rabinovich8, Daniel J Kingsbury9, Katherine Marzan10, Pierre Quartier11, Kirsten Minden12, Elizabeth Chalom1, Gerd Horneff13, Rolf M. Kuester14, Jason A Dare15, Mareike Bereswill16, Jasmina Kalabic16, Hartmut Kupper16, Daniel J Lovell1 and Alberto Martini2, 1PRCSG, Cincinnati Children’s Hospital Medical Center, Cincinnati, OH, 2PRINTO-IRCCS Gaslini, Genova, Italy, 3University of Washington School of Medicine and Seattle Children's Hospital, Bayside, NY, 4Akron Children's Hospital, Akron, OH, 5Department of Pediatric Rheumatology, Hamburger Zentrum für Kinder und Jugendrheumatologie, Hamburg, Germany, 6University of Utah, Department of Pediatrics, Salt Lake City, UT, 7The Floating Hospital for Children at Tufts Medical Center, Boston, MA, 8Duke University Medical Center, Durham, NJ, 9Randall Children’s Hospital at Legacy Emanuel, Portland, OR, 10Children's Hospital Los Angeles, Los Angeles, CA, 11Hopital Necker-Enfants Malades, Paris, France, 12Kinderklinik der Charite, Otto-Heubner Centrum, Berlin, Germany, 13Asklepios Clinic Sankt Augustin, Sankt Augustin, Germany, 14Orthopädiezentrum Altona, Hamburg, Germany, 15Arkansas Children’s Hospital, Little Rock, AR, 16AbbVie Deutschland GmbH & Co. KG, Ludwigshafen, Germany

Meeting: 2017 ACR/ARHP Annual Meeting

Date of first publication: September 18, 2017

Keywords: , ,

Session Information

Date: Tuesday, November 7, 2017

Title: Pediatric Rheumatology – Clinical and Therapeutic Aspects Poster III: Juvenile Arthritis

Session Type: ACR Poster Session C

Session Time: 9:00AM-11:00AM

Background/Purpose: JIA is the most common chronic inflammatory rheumatic disease of childhood. Due to their known safety and efficacy, TNF inhibitors are used for long-term control of pJIA disease. The purpose of this analysis was to evaluate the 7 year (y) safety of Adalimumab treatment with or without methotrexate (ADA±MTX) when used in current clinical practice for treatment of patients (pts) with active pJIA.

Methods: This is a 7 y interim analysis of an ongoing, multicenter, non-interventional, observational registry of pts with pJIA with up to10 y safety follow-up. Included pts were treated with either ADA±MTX or MTX alone as comparison arm according to routine clinical care in US, EU, and Australia. MedDRA observational adverse events (AEs) were recorded from 1st day in the registry through last contact, irrespective of the duration of registry treatment.

Results: In January 2014, enrollment was complete. As of June 1, 2016 cut-off date, 838 pts (301- MTX arm and 537 – ADA±MTX arm) were treated in the registry. There were 39 pts who rolled over from MTX to the ADA±MTX arm. At registry entry mean pJIA disease duration was 1.3 y and 3.7 y and mean AJC71 was 5.8 and 5.2 for MTX and ADA±MTX arms, respectively. CHAQ disability index was 0.6 for both arms. The mean duration of study drug exposure in registry was 2.0 y (range: 0.0 – 7.1) and 2.5 y (range: 0.0 – 7.9) for MTX and ADA±MTX arms, respectively. The mean duration of observation in registry was 3.9 y (range: 0.0 – 7.2) and 3.5 y (range: 0.0 – 7.9) for MTX and ADA±MTX arms, respectively. Overall, 213 pts (70.8%) in MTX and 225 pts (41.9%) in ADA±MTX arms discontinued registry drug through 7 y. The main reasons for registry drug discontinuation for MTX arm: pts required additional therapy (32.6%), other (13.3%), lack of efficacy (11.6%), AEs (9.3%), or pts achieved JIA remission (8.6%), and for ADA±MTX arm: lack of efficacy (17.9%), other (7.3%), lost to follow-up (5.6%), AEs (5.4%), or pts achieved JIA remission (5.0%). Frequencies and rates of treatment-emergent AEs (from 1st dose date of registry drug in registry up to last dose + 70 days in registry, excluding AEs occurring during treatment interruption) were similar to those reported for observational AEs (from 1st day in registry up to last contact irrespective of drug treatment duration) (Table). The rate of serious infections was similar between MTX and ADA±MTX arms. One pt (0.2%) reported an event of opportunistic infection (fungal oesophagitis) in ADA±MTX arm. No reports of deaths, malignancies, active tuberculosis, oral candidiasis, demyelination, or congestive heart failure.

Conclusion: Overall, ADA±MTX was well-tolerated in these pts with pJIA with no new safety signals. The retention rate for registry drug was higher in ADA±MTX arm compared to MTX arm.

Table. Overview of the Observational Adverse events

MTX

ADA±MTX

ADA only

ADA + MTX#

N=301

n (%)

PYs=1170.3

E (E/100 PYs)

N=160

n (%)

PYs=517.0

E (E/100 PYs)

N=377

n (%)

PYs=1338.5

E (E/100 PYs)

Any AE

157 (52.2)

505 (43.2)

66 (41.3)

216 (41.8)

178 (47.2)

553 (41.3)

AE at least “possibly drug related” per the investigator

87 (28.9)

197 (16.8)

30 (18.8)

66 (12.8)

88 (23.3)

177 (13.2)

Severe AE

17 (5.6)

23 (2.0)

14 (8.8)

22 (4.3)

25 (6.6)

41 (3.1)

Serious AE

32 (10.6)

52 (4.4)

21 (13.1)

39 (7.5)

56 (14.9)

95 (7.1)

AE leading to discontinuation of study drug or study

28 (9.3)

36 (3.1)

13 (8.1)

19 (3.7)

25 (6.6)

40 (3.0)

Infectious AE

87 (28.9)

179 (15.3)

38 (23.8)

75 (14.5)

105 (27.9)

187 (14.0)

Serious infectious AE

14 (4.7)

17 (1.5)

6 (3.8)

8 (1.5)

22 (5.8)

30 (2.2)

Injection site-related AE

6 (2.0)*

8 (0.7)

5 (3.1)

6 (1.2)

24 (6.4)

32 (2.4)

E, events; PYs, patient years (Observation time irrespectively of study drug treatment duration). *3 patients experienced injection site-related AEs with etanercept injections. During the registry, 52 (17.3%) pts in MTX arm and 45 (8.4%) pts in ADA arm started with a biologic DMARD. #MTX was used at any point of time during the course of the registry.

Disclosure: H. I. Brunner, AbbVie Inc., AstraZeneca, Centocor, Bristol-Myers Squibb, Boehringer-Ingelheim, Pfizer, Regeneron, Hoffman La-Roche, Novartis, Takeda, UCB, and Genentech, 5,AbbVie Inc., AstraZeneca, Centocor, Bristol-Myers Squibb, Boehringer-Ingelheim, Pfizer, Regeneron, Hoffman La-Roche, Novartis, Takeda, UCB, and Genentech, 9,Genentech Pharmaceuticals, 8; N. Ruperto, GASLINI Hospital, 3,Astellas, AstraZeneca, Bristol-Myers Squibb, Italfarmaco, Janssen Biologics B.V., MedImmune, Roche, and Wyeth/Pfizer, 8; K. Nanda, Medac Pharma, Inc, 5; M. Toth, None; I. Foeldvari, AbbVie and Novartis, 9; J. F. Bohnsack, Novartis Pharmaceutical Corporation, 5; D. Milojevic, Genentech and Novartis, 5; C. E. Rabinovich, UCB Pharma, Janssen Research & Development, LLC, Hoffmann-La Roche Inc., and AbbVie, 9; D. J. Kingsbury, AbbVie, 9; K. Marzan, AbbVie, 2; P. Quartier, AbbVie, Novartis, Pfizer, BMS, Chugai-Roche, Medimmune, Servier, and Swedish Orphan Biovitrum, 2,AbbVie, Novartis, Pfizer, BMS, Chugai-Roche, Medimmune, Servier, and Swedish Orphan Biovitrum, 5,Sanofi trial., 9; K. Minden, from Pfizer, AbbVie and Roche/Chugai, 2,Pfizer, AbbVie, Genzyme, and Pharma-Allergan, 5,Pfizer, AbbVie, Genzyme, and Pharma-Allergan, 9; E. Chalom, Abbvie SPeaker's Bureau, 8; G. Horneff, AbbVie, Pfizer, Novartis, and Roche, 2,AbbVie, Novartis, Sobi, Pfizer, and Roche, 9; R. M. Kuester, AbbVie Inc. and Wyeth/Pfizer, 9; J. A. Dare, AbbVie, AstraZeneca, Bristol-Myers Squibb, Horizon Pharma, Medac, Pfizer, Roche, and UCB, 9; M. Bereswill, Abbvie, 3,Abbvie, 1; J. Kalabic, AbbVie Inc, 1,AbbVie Inc, 3; H. Kupper, AbbVie, 1,AbbVie, 3; D. J. Lovell, AbbVie Inc., AstraZeneca, Centocor, Bristol-Myers Squibb, Pfizer, Regeneron, Hoffman La-Roche, Novartis, UBC, Xoma, and Genentech, 5,Wyeth Pharmaceuticals, 8,Amgen and Forest Research, 9; A. Martini, GASLINI Hospital, 3,Astellas, AstraZeneca, Bristol-Myers Squibb, Italfarmaco, and MedImmune, 8,AbbVie Inc., AstraZeneca, Bristol-Myers Squibb, Janssen Biologics B.V., Eli Lilly and Co., “Francesco Angelini”, GlaxoSmithKline, Italfarmaco, Novartis, Pfizer, Roche, Sanofi Aventis, Schwarz Biosciences GmbH, Xoma, and Wyeth Pharmaceuticals, 2.

To cite this abstract in AMA style:

Brunner HI, Ruperto N, Nanda K, Toth M, Foeldvari I, Bohnsack JF, Milojevic D, Rabinovich CE, Kingsbury DJ, Marzan K, Quartier P, Minden K, Chalom E, Horneff G, Kuester RM, Dare JA, Bereswill M, Kalabic J, Kupper H, Lovell DJ, Martini A. Safety of Adalimumab±Methotrexate for the Treatment of Polyarticular Juvenile Idiopathic Arthritis (pJIA) [abstract]. Arthritis Rheumatol. 2017; 69 (suppl 10). https://acrabstracts.org/abstract/safety-of-adalimumab%c2%b1methotrexate-for-the-treatment-of-polyarticular-juvenile-idiopathic-arthritis-pjia/. Accessed .

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