An Exploratory Analysis of Predictors of Response from 12-Weeks of Canakinumab Therapy in Patients with Active Systemic Juvenile Idiopathic Arthritis

Hermine I. Brunner¹, Nicola Ruperto², Isabelle Koné-Paut², Bo Magnusson², Seza Ozen², Flavio Sztajnbok², Jordi Anton², Judith Barash², Reinhard Berner², Fabrizia Corona², Karine Lheritier³, Corine Gaillez³, Alberto Martini² and Daniel Lovell¹, ¹PRCSG, Cincinnati, OH, ²PRINTO-Istituto Gaslini, Genova, Italy, ³Novartis Pharma AG, Basel, Switzerland

Meeting: 2014 ACR/ARHP Annual Meeting

Keywords: Systemic JIA and canakinumab

Session Information

Title: Pediatric Rheumatology - Clinical and Therapeutic Aspects: Juvenile Idiopathic Arthritis

Session Type: Abstract Submissions (ACR)

Background/Purpose

Systemic juvenile idiopathic arthritis (SJIA), an interleukin-1β (IL-1β)-mediated autoinflammatory disease, is characterized by recurrent flares of active disease. Canakinumab (CAN), a selective, human, anti- interleukin-1β monoclonal antibody, has been shown to be efficacious in the treatment of SJIA (Ruperto et al. N Engl J Med 2012). The present study aimed to explore baseline demographics and clinical characteristics that are most predictive of response to CAN in CAN-naïve SJIA patients during the initial 12 weeks of therapy.

Methods

Data from 3 trials were pooled for this analysis. CAN-naïve patients (pts; n=178) aged 2–19 years with active SJIA were enrolled and received sc CAN 4 mg/kg/month; Predictors of response (according to aACR* 30, 70, and Inactive Disease [ID]) at Days (D) 15, 29, 57 and 85 were explored using univariate and multivariate logistic regression analyses. The candidate predictors (categorical variables) of CAN-response considered were: Age group, Gender, Prior NSAIDs (no/yes), Prior MTX (no/yes), Steroids (0, >0 – ≤0.4;> 0.4 mg/kg/day), Number of Active Joints (≤10, 11-≤20, >20) and Joints with Limitation of Motion (≤10, 11-≤20,>20), CRP (elevated/normal) at baseline and at D15. All candidate predictors with p<0.1 in univariate analyses were included in the multivariate analysis. *ACR response plus absence of fever.

Results

By Week 2 there was substantial clinical benefit with 102 pts (57%) and 36 pts (20%) achieving aACR70 and ID, respectively; by Week 12, 108 pts (61%) had aACR70 and 50 pts (28%) ID. The multivariate analysis indicated that normal CRP at D15 is the only predictor significant (all p<0.05) for ID at all time-points (Table).

Table: Inactive Disease – Multivariate logistic regression analysis on 12-week data

	Odds Ratio (95% CI)
Variable*	Day 15	Day 29	Day 57	Day 85
CRP at Day 15 (elevated vs normal)	0.20 (0.07, 0.55)	0.14 (0.04, 0.41)	0.26 (0.10, 0.66)	0.31 (0.12, 0.82)
Number of active joints (11-≤20 vs. ≤10)	0.22 (0.03, 1.66)	0.55 (0.09, 3.41)	0.17 (0.031, 0.97)	0.37 (0.06, 2.10)
Number of active joints (≤10 vs. >20)	2.56 (0.12, 55.39)	1.53 (0.06, 37.44)	16.10 (1.00, 258.12)	25.41 (1.60, 404.61)
Prior NSAID treatment (no vs. yes)	2.01 (0.71, 5.71)	9.33 (2.44, 35.68)	3.10 (1.03, 9.31)	5.31 (1.66, 17.05)
Steroid Level (0 vs. >0.4 mg/kg/day)	5.48 (0.97, 31.01)	8.89 (1.26, 62.64)	2.98 (0.51, 17.46)	11.16 (1.72, 72.34)
Steroid Level (>0.4 vs >0-≤0.4 mg/kg/day)	0.32 (0.08, 1.29)	0.41 (0.09, 1.82)	0.81 (0.25, 2.60)	0.13 (0.03, 0.57)
Prior MTX treatment (no vs. yes)	1.94 (0.75, 5.00)	2.78 (0.93, 8.33)	2.79 (1.04, 7.51)	1.77 (0.65, 4.83)
Prior anti-TNFs treatment (no vs. yes)	1.83 (0.52, 6.49)	3.62 (0.77, 17.00)	2.01 (0.63, 6.38)	3.64 (1.04, 12.77)

Values in bold are significant; *Significant in at least one time point

Conclusion This exploratory analysis suggests that canakinumab-naïve patients with normal CRP (i.e. ≤10 mg/l) at Day 15, lower baseline steroid doses, low number of active joints, no prior NSAID use are most likely to achieve inactive disease up to 12 weeks.

Disclosure:

H. I. Brunner,

Novartis, Genentech, Pfizer, UCB, AstraZeneca, Biogen, Boehringer-Ingelheim, Regeneron,

Novartis, Genentech,

Novartis Pharma AG,

N. Ruperto,

Abbott, Astrazeneca, BMS, Centocor Research & Development, Eli Lilly and Company, “Francesco Angelini”, Glaxo Smith & Kline, Italfarmaco, Novartis, Pfizer Inc., Roche, Sanofi Aventis, Schwarz Biosciences GmbH, Xoma, Wyeth Pharmaceuticals Inc.,,

Astrazeneca, Bristol Myers and Squibb, Janssen Biologics B.V., Roche, Wyeth, Pfizer,,

I. Koné-Paut,

SOBI, Chugai,

Pfizer, SOBI, Novartis, AbbVie, Cellgene, Chugai,

B. Magnusson,
None;

S. Ozen,

Novartis (Turkey),,

SOBI,

F. Sztajnbok,

Institutional grant (UERJ) for participating in the canakinumab trial,

Novartis-Brasil,

J. Anton,

Novartis-,

J. Barash,

Investigator in the Canakinumab study sponsored by Novartis,

R. Berner,
None;

F. Corona,
None;

K. Lheritier,

Novartis .,

C. Gaillez,

Novartis.,

A. Martini,

Bristol-Myers Squibb,Centocor Research & Development,Glaxo Smith & Kline, Novartis, Pfizer Inc, Roche, Sanofi Aventis, Schwarz Biosciences GmbH,

Bristol Myers and Squibb, Centocor Research & Development, Glaxo Smith & Kline, Novartis, Pfizer Inc, Roche, Sanofi Aventis, Schwarz Biosciences GmbH,,

Abbott, Bristol Myers Squibb, Astellas, Boehringer, Italfarmaco, MedImmune, Novartis, NovoNordisk, Pfizer, Sanofi, Roche, Servier,,

D. Lovell,

National Institutes of Health- NIAMS,

AstraZeneca, Centocor, Amgen, Bristol Meyers Squibb, Abbott, Pfizer, Regeneron, Roche, Novartis, UBC, Forest Research Institute, Horizon, Johnson & Johnson,

Novartis, Roche,

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