The Randomized Placebo Phase Study of Rilonacept in the Treatment of Systemic Juvenile Idiopathic Arthritis

Norman T. Ilowite¹, Kristi Prather², Yuliya Lokhnygina³, Laura E. Schanberg⁴, Melissa Elder⁵, Diana Milojevic⁶, James W. Verbsky⁷, Steven J. Spalding⁸, Yukiko Kimura⁹, Lisa F. Imundo¹⁰, Marilynn G. Punaro¹¹, David D. Sherry¹², Stacey E. Tarvin¹³, Lawrence S. Zemel¹⁴, James D. Birmingham¹⁵, Beth S. Gottlieb¹⁶, Michael L. Miller¹⁷, Kathleen M. O'Neil¹⁸, Natasha M. Ruth¹⁹, Carol A. Wallace²⁰, Nora G. Singer²¹ and Christy I. Sandborg²², ¹Pediatrics, The Children's Hospital at Montefiore, Bronx, NY, ²Statistics, Duke Clinical Research Institute, Durham, NC, ³Duke Clinical Research Institute, Durham, NC, ⁴Pediatrics, Duke University Medical Center, Durham, NC, ⁵Pediatrics, University of Florida, Gainesville, HI, ⁶Dept of Pediatric Rheumatology, University of California, San Francisco, San Francisco, CA, ⁷Department of Pediatrics, Medical College of Wisconsin, Milwaukee, WI, ⁸Pediatric Institute, Department of Pediatric Rheumatology, The Cleveland Clinic, Cleveland, OH, ⁹Pediatric Rheumatology, Joseph M Sanzari Children’s Hospital, Hackensack University Medical Center, Hackensack, NJ, ¹⁰Pediatric and Adult Rheumatology Columbia University Medical Center, New York, NY, ¹¹Pediatric Rheumatology, Texas Scottish Rite Hospital, Dallas, TX, ¹²Pediatric Rheumatology, Children's Hospital of Philadelphia, Philadelphia, PA, ¹³Pediatric Rheumatology, Riley Hospital for Children, Indianapolis, IN, ¹⁴Pediatric Rheumatology Collaborative Study Group, Cincinnati, OH, ¹⁵Medicine & Pediatrics, Rheumatology, Michigan State University College of Human Medicine, Grand Rapids, MI, ¹⁶Pediatric Rheumatology, Cohen Children's Medical Center of New York, New Hyde Park, NY, ¹⁷Rheumatology, Childrens Memorial Hospital, Chicago, IL, ¹⁸Division of Pediatric Rheumatology, University of Oklahoma Health Sciences Center, Oklahoma City, OK, ¹⁹Pediatric Rheumatology, Medical University of South Carolina, Charleston, SC, ²⁰University of Washington School of Medicine and Seattle Children's Hospital, Seattle, WA, ²¹Rheumatology, MetroHealth Medical Center, Cleveland, OH, ²²Pediatric Rheumatology, Stanford University, Palo Alto, CA

Meeting: 2013 ACR/ARHP Annual Meeting

Keywords: clinical trials, IL-1, juvenile idiopathic arthritis (JIA), pediatric rheumatology and treatment

Session Information

Title: Pediatric Rheumatology - Clinical and Therapeutic Aspects II: Autoinflammatory Disease and Systemic Juvenile Idiopathic Arthritis

Session Type: Abstract Submissions (ACR)

Background/Purpose: The RAndomized Placebo Phase Study Of Rilonacept in the Treatment of Systemic Juvenile Idiopathic Arthritis (RAPPORT) is a multicenter controlled trial using a 4 week randomized placebo phase. The study design reasons that if a treatment is effective, subjects who begin active treatment earlier will respond sooner, on average, than subjects who begin active treatment later. Rilonacept is a fusion protein consisting of human cytokine receptor extracellular domains of both receptor components required for IL-1 signaling: the IL-1 Type I receptor and the IL-1 receptor accessory protein as well as the Fc portion of human IgG1.

Methods: RAPPORT consisted of a double-blind phase (weeks 0-4), a treatment phase (weeks 4-24) and an open label Long Term Extension phase (24 weeks -21 months). The primary endpoint was time to response, using adapted JIA ACR 30 response criteria requiring absence of fever for 2 weeks and meeting pre-specified criteria for tapering of corticosteroids during the first 12 weeks of the study. We randomized 71 children with at least 2 active joints from 20 sites 1:1 to 2 arms of the study. The rilonacept arm subjects received rilonacept (4.4mg/kg loading dose followed by weekly 2.2mg/kg subcutaneously) and placebo arm subjects received placebo for 4 weeks followed by loading dose of rilonacept at week 4 followed by weekly maintenance doses. After week 14, corticosteroids were dosed according to the treating physician.

Results: The time to response was shorter in the rilonacept arm (median 4 weeks; range 2-10 weeks) than in the placebo arm (median 6 weeks; range 2-12 weeks) (Chi-square 7.235; p=0.007). Twenty-six of 35 (79%)patients in the rilonacept arm and 13 of 33 (39%)in the placebo arm met ACR Pediatric 30 response criteria at week 4 (p=0.004); 21/35 (60%) in the rilonacept arm vs. 10/33 (30%) in the placebo arm met ACR pediatric 50 response criteria (p=0.015); 14/35 (40%) vs. 4/33 (12%) met ACR pediatric 70 criteria (p=0.013). Adverse events were similar in the two arms of the study (Table). Four subjects developed elevations in liver transaminases of ≥ 2 times the upper limit of normal (all while on rilonacept); 2 subjects developed elevations ≥5 times the upper limit of normal. In one, the elevations resolved but recurred on re-challenge and was deemed an SAE. One subject developed EBV induced macrophage activation syndrome.

Conclusion: This is the first double-blind, randomized, placebo-controlled trial of rilonacept to demonstrate efficacy in sJIA. Rilonacept treatment was relatively safe. Significant elevations in aspartate aminotransferase levels were rare but occurred more often in subjects receiving rilonacept than in those on placebo.

Table: Adverse Events
	Double-Blind Phase _______________________		Treatment Phase _______________________		LTE Open-Label Phase ______________
Variable	Rilonacept (N=36)	Placebo (N=35)	Rilonacept (N=35)	Placebo (N=33)	Rilonacept (N=40)
ADVERSE EVENTS
No. of events	16	62	81	123	110
No. of events per patient-year	5.7	23.6	6.2	11.3	3.0
Patients with an event – no. (%)	9 (25%)	19 (54%)	27 (77%)	28 (85%)	28 (70%)
Most frequently reported events – no. of patients (%)¹
Abdominal pain upper	1 (3%)	2 (6%)	3 (9%)	1 (3%)	0
Arthralgia	0	1 (3%)	2 (6%)	6 (18%)	1 (3%)
Cough	0	1 (3%)	2 (6%)	3 (9%)	2 (5%)
Headache	1 (3%)	6 (17%)	1 (3%)	4 (12%)	3 (8%)
Nausea	0	1 (3%)	1 (3%)	2 (6%)	3 (8%)
Pharyngitis streptococcal	0	0	2 (6%)	2 (6%)	4 (10%)
Pyrexia	0	1 (3%)	5 (14%)	1 (3%)	1 (3%)
Rash	2 (6%)	1 (3%)	1 (3%)	3 (9%)	1 (3%)
Upper respiratory tract infection	0	1 (3%)	5 (14%)	9 (27%)	2 (5%)
Vomiting	1 (3%)	2 (6%)	1 (3%)	2 (6%)	4 (10%)
SERIOUS ADVERSE EVENTS
No. of events	0	1	3	1	8
No. of events per patient-year	0.0	0.4	0.2	0.1	0.2
Patients with an event – no. (%)	0	1 (3%)	3 (9%)	1 (3%)	6 (15%)
All reported events – no. of patients (%)
Gastroenteritis salmonella	0	0	0	0	1 (3%)
Histiocytosis haematophagic	0	0	0	0	1 (3%)
Juvenile arthritis	0	1 (3%)	0	1 (3%)	1 (3%)
Elevated liver function tests	0	0	1 (3%)	0	0
Mental status changes	0	0	0	0	1 (3%)
Pericarditis	0	0	0	0	1 (3%)
Pharyngitis streptococcal	0	0	0	0	1 (3%)
Pyrexia	0	0	1 (3%)	0	0
Varicella	0	0	1 (3%)	0	0
Viral upper respiratory tract infection	0	0	0	0	1 (3%)
INFECTIONS
No. of events	2	2	25	29	37
No. of events per patient-year	0.7	0.8	1.9	2.7	1.0
Patients with an event – no. (%)	2 (6%)	2 (6%)	16 (46%)	20 (61%)	14 (35%)

¹The most frequently reported events were defined as events that occurred in at least 10% of all patients during the entire study.

Disclosure:

N. T. Ilowite,

Novartis Pharmaceutical Corporation,

Janssen Pharmaceutica Product, L.P.,

K. Prather,
None;

Y. Lokhnygina,
None;

L. E. Schanberg,

Novartis Pharmaceutical Corporation,

Lilly,

UCB,

GSK,

BMS,

SOBI,

Pfizer Inc,

M. Elder,
None;

D. Milojevic,
None;

J. W. Verbsky,

Baxter,

S. J. Spalding,
None;

Y. Kimura,
None;

L. F. Imundo,
None;

M. G. Punaro,
None;

D. D. Sherry,
None;

S. E. Tarvin,
None;

L. S. Zemel,
None;

J. D. Birmingham,
None;

B. S. Gottlieb,
None;

M. L. Miller,
None;

K. M. O’Neil,

UCB,

N. M. Ruth,
None;

C. A. Wallace,

Amgen,

Pfizer Inc,

Novartis Pharmaceutical Corporation,

N. G. Singer,
None;

C. I. Sandborg,
None.

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