ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 2137

Therapeutic Strategies in Newly Diagnosed Still’s Disease: Real-Life Clinicians’ Choices from the METAPHOR Project Worldwide Survey

Francesco Baldo1, Greta Rogani2, Claudia Bracaglia3, Dirk Foell4, Marco Gattorno5, Jordi anton6, Paul Brogan7, Scott Canna8, randy Cron9, Alexiei GROM10, Merav Heshin Bekenstein11, Raju Khubchandani12, Seza Özen13, Pierre Quartier14, Angelo Ravelli15, Grant Schulert16, Mao Mizuta17, Joost Swart18, Rashmi Sinha19, AnnaCarin Horne20, Fabrizio De Benedetti21, Christiaan Scott22, Marija Jelusic23, Masaki Shimizu24, Bruno Fautrel25, Nicolino Ruperto26, Sebastiaan Vastert2 and Francesca Minoia27, 1ASST-Pini-CTO, Milano, Milan, Italy, 2University Medical Center Utrecht, Utrecht, Utrecht, Netherlands, 3IRCCS Ospedale Pediatrico Bambino Gesu', Rome, Rome, Italy, 4Universisty Hospital of Muenster, Muenster, 5IRCCS G. Gaslini, Genova, Genoa, Italy, 6Hospital Sant Joan de Düu. Universitat de Barcelona, Barcelona, Spain, 7UCL Institute of Child Health and Great Ormond Street Hospital NHS Foundation Trust, London, United Kingdom, 8Children's Hospital of Philadelphia, Philadelphia, PA, 9University of Alabama at Birmingham, Birmingham, AL, 10Cincinnati Children’s Hospital Medical Center, Division of Rheumatology, Cincinnati, OH, 11Tel Aviv Medical Center Israel, Binyamina, Tel Aviv, Israel, 12Jaslok Hospital and Research Center, Mumbai, India, 13Hacettepe University Medical Faculty, Ankara, Turkey, 14Hôpital Necker-Enfants Malades, Paris, France, 15IRCCS Istituto Giannina Gaslini, Genoa, Italy, Genoa, Genoa, Italy, 16Cincinnati Children's Hospital Medical Center, Cincinnati, OH, 17Hyogo Prefectural Kobe Children's Hospital, Kobe, Japan, Kobe, Japan, 18Wilhelmina Children's Hospital / UMC Utrecht, Utrecht, Utrecht, Netherlands, 19Systemic JIA Foundation, Cincinnati, OH, 20Karolinska University Hospital, Sollentuna, Sweden, 21Bambino Gesu Children's Hospital, Rome, Rome, Italy, 22Childrens Hospital of Eastern Ontario (CHEO), Ottawa, ON, Canada, 23University of Zagreb School of Medicine, University Hospital Centre Zagreb, Zagreb, Zagreb, Croatia, 24Tokyo Medical and Dental University, Bunkyo-ku, Kanazawa, Japan, 25Sorbonne Université - APHP, Department of Rheumatology, Hôpital Pitié-Salpêtrière, Inserm UMRS 1136-5, PARIS, France, Paris, France, 26Université Milano Bicocca and Fondazione IRCSS S. Gerardo dei Tintori, Monza, Monza and Brianza, Italy, 27Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milano, Milan, Italy

Meeting: ACR Convergence 2025

Keywords: , , , ,

Session Information

Date: Tuesday, October 28, 2025

Title: (2124–2158) Pediatric Rheumatology – Clinical Poster III

Session Type: Poster Session C

Session Time: 10:30AM-12:30PM

Background/Purpose: Despite continuous advances in care and the recent publication of updated international recommendations, relevant discrepancies in the management of Still’s disease (SD) may still exist, due to different clinical presentation and practice setting. The aim of the study is to assess current intial treatment strategies in SD worldwide, and to identify factors influencing clinical decision-making.

Methods: As part of the METAPHOR project, a PReS/PRINTO initiative to optimize treatment in SD and macrophage activation syndrome, a global survey on SD treatment was developed and distributed (Dec 3, 2024–Feb 14, 2025). Topics were selected by 22 experts. The survey included demographic data, clinical practice insights, a patient-led section on unmet needs. International physicians part of the PReS/PRINTO network and adult rheumatologists involved in SD care were invited to complete the anonymous online survey (Dec 3, 2024–Feb 14, 2025).

Results: A total of 206 clinicians, mainly pediatric rheumatologists (91%), from 56 countries completed the survey. In newly diagnosed SD patients without MAS, 34% of respondents would initiate anti-IL1/IL6 biologic without glucocorticoids (GCs); the rest would use GCs alone (24%) or in combination with biologics (42%). Factors favoring GCs use included severe pericarditis (64%), severe arthritis (55%), and refractory disease risk factors (16%), as hyperferritinemia, lung involvement, early onset and Trisomy 21.Anakinra was the most frequently used biologic in 1st line (59%), followed by Tocilizumab (25%). Only 1.5% reported unavailability of any anti-IL1/IL-6 therapy. Factors driving anakinra’s choice were safety (72%), cost (41%), and predominant systemic phenotype (73%), while Tocilizumab was chosen for compliance (56%) and arthritis-dominant profile (80%). Difficult access to medication influenced decisions for Rilonacept (67%), Canakinumab (27%), Anakinra (17%); Tocilizumab was rarely unavailable (1.5%).In systemic-predominant SD, clinicians used NSAIDs (50%), GCs (46%), GCs pulses (42%),and Anakinra (45%) as first-line options. Second-line strategies included Tocilizumab (39%), GCs (31%), Anakinra (29%), GCs pulses (22%), and MTX (21%), while Tocilizumab (37%), JAK inhibitors (29%), and cyclosporin (24%) were the most selected options as third-line therapies. In SD patients with a prominent articular involvement at onset, half of the respondents would not change their therapeutic approach. Physician who modified thor strategy would use as a first line f therapies GCs (47%), oral steroids (44%), Tocilizumab (39%), MTX (34%), and intra-articular steroids (31%). Second-line choices were mostly Tocilizumab and MTX (~40%). Differences in management by clinical phenotype are detailed in Figure 1.

Conclusion: Still’s disease still represents a therapeutic challenge, mainly due to its heterogeneity in clinical expression. Our data reveals significant differences in treatment approaches, driven by clinical phenotype and drug availability. Future research is essential to optimize clustering of patients to foster tailored target treatments, while ensuring equitable access to effective therapies worldwide.

Supporting image 1

Disclosures: F. Baldo: None; G. Rogani: None; C. Bracaglia: None; D. Foell: None; M. Gattorno: Fresenius Kabi SwissBioSim GmbH, 6, Novartis, 1, 2, 5, 6, SOBI, 2, 6; J. anton: Sobi, 1, 5, 6; P. Brogan: Sobi, 6; S. Canna: AB2Bio, 2, Bristol-Myers Squibb(BMS), 2, Novartis, 2, Simcha Therapeutics, 12, In-kind provision of a reagent, Sobi, 6; r. Cron: AbbVie/Abbott, 1, American Board of Pediatrics, 12, Board Question Writer, AS2 Biotherapeutics, 2, CareerPhysician, 1, Neurogene, 2, Pfizer, 1, Sobia, 1, Springer, 9, VIDA Ventures, 2; A. GROM: National Institutes of Health, 5, Novartis, 2, 5, sJIA Foundation, 5, Sobi, 2, 5, Up-To-Date, 9; M. Heshin Bekenstein: None; R. Khubchandani: None; S. Özen: Novartis, 6, Pfizer, 6, Sobi, 6; P. Quartier: AbbVie, 2, 6, Chugai-Roche, 2, 6, Eli Lilly, 2, 6, Novartis, 2, 6, Pfizer, 2, 6, Sanofi, 1, 2, Sobi, 2, 6; A. Ravelli: AbbVie, 2, 5, 6, Alexion, 2, 5, 6, Bristol-Myers Squibb(BMS), 2, 5, 6, Galapagos, 2, 5, 6, Johnson & Johnson, 2, 5, 6, Novartis, 2, 5, 6, Pfizer, 2, 5, 6, Roche, 2, 5, 6, SOBI, 2, 5, 6; G. Schulert: IpiNovoyx, 5, Novartis, 2, SOBI, 2; M. Mizuta: None; J. Swart: None; R. Sinha: None; A. Horne: None; F. De Benedetti: AbbVie, 2, 5, Apollo, 2, 5, Elixiron, 2, 5, Kiniksa, 2, 5, Novartis, 2, 5, Sanofi, 2, 5, Sobi, 2, 5; C. Scott: None; M. Jelusic: None; M. Shimizu: None; B. Fautrel: AbbVie, 2, 5, Amgen, 2, Biogen, 2, BMS, 2, Celltrion, 2, Chugai, 2, Eli Lilly & Co., 2, 5, Fresenius Kabi, 2, Galapagos, 2, Janssen, 2, Medac, 2, MSD, 2, 5, Nordic Pharma, 2, Novartis, 2, OW KIN, 2, Pfizer, 2, 5, Roche, 2, Sandoz, 2, Sanofi-Genzyme, 2, SOBI, 2, UCB, 2, Viatris, 2; N. Ruperto: Abbvie, 2, 6, AClaris, 2, 6, AlfaSigma, 2, 6, Amgen, 2, 6, AstraZeneca, 2, 6, Aurinia, 2, 6, Boehringer-Ingelheim, 2, 6, Bristol Myers and Squibb, 2, 6, Eli Lilly, 2, 6, Galapagos, 2, 6, Genentech, 2, 6, Guidepoint, 2, 6, Idorsia, 2, 6, Janssen, 2, 6, Novartis, 2, 6, Pfizer, 2, 6, Roche, 2, 6, Sanofi, 2, 6, Takeda, 2, 6; S. Vastert: Novartis, 2, 6, Sobi, 2, 5, 6; F. Minoia: None.

To cite this abstract in AMA style:

Baldo F, Rogani G, Bracaglia C, Foell D, Gattorno M, anton J, Brogan P, Canna S, Cron r, GROM A, Heshin Bekenstein M, Khubchandani R, Özen S, Quartier P, Ravelli A, Schulert G, Mizuta M, Swart J, Sinha R, Horne A, De Benedetti F, Scott C, Jelusic M, Shimizu M, Fautrel B, Ruperto N, Vastert S, Minoia F. Therapeutic Strategies in Newly Diagnosed Still’s Disease: Real-Life Clinicians’ Choices from the METAPHOR Project Worldwide Survey [abstract]. Arthritis Rheumatol. 2025; 77 (suppl 9). https://acrabstracts.org/abstract/therapeutic-strategies-in-newly-diagnosed-stills-disease-real-life-clinicians-choices-from-the-metaphor-project-worldwide-survey/. Accessed .

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