Cutaneous IgA Vasculitis: Emulation of a Target Trial from a European Multicentric Retrospective Study

Elena Biancamaria Mariotti¹, Boris Sorin², William Lutz³, Chloé Grolleau³, Thomas Bettuzzi⁴, Caterina Ricordi⁵, Santos Castañeda⁶, Luisa Herda⁷, Cord Sunderkotter⁷, Rodérau Outh⁸, Romain Paule⁹, Alexandra Audemard-Verger¹⁰, Marzia Caproni¹¹, Angelo Valerio Marzano¹², Pietro Quaglino¹³, Laura Atzori¹⁴, Julien Campagne¹⁵, Mehemt Erkan¹⁶, Nabil Belfeki¹⁷, Marijan Frkovic¹⁸, Nicolas Dupin¹⁹, Raphael Porcher²⁰, Marie Jachiet²¹ and Benjamin Terrier¹⁹, ¹University of Florence, Azienda USL Toscana Centro, Department of Dermatology, Florence, Firenze, Italy, ²Assistance Publique Hôpitaux de Paris, Paris, France, ³University Paris Cité, Hospital Saint Louis, Dermatology department, Paris, Paris, France, ⁴Université Paris Est Créteil Val de Marne, Hôpital Henri-Mondor (APHP), Service de dermatologie, EpiDermE, Paris, France, ⁵AUSL-IRCCS Reggio Emilia, Parma, Italy, ⁶Hospital Universitario de La Princesa, IIS-Princesa, Madrid, Madrid, Spain, ⁷Department of Dermatology and Venereology, Martin Luther University Halle-Wittenberg, Halle (Saale), Halle, Germany, ⁸Department of Internal Medicine, Centre Hospitalier de Perpignan, Perpignan, France., Clermont-Ferrand, France, ⁹Hospital Foch, Service de medicine interne, Suresnes, Paris, Suresnes, France, ¹⁰Department of Internal Medicine, Tours University Hospital, Tours, France., Tours, France, ¹¹University of Florence, Azienda USL Toscana Centro, Department of Dermatology, Florence, Florence, Italy, ¹²Dermatology Unit, Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico, Milan, Milan, Italy, ¹³University of Turin, Department of Medical Sciences, Section of Dermatology, Turin, Torino, Italy, ¹⁴Dermatology Clinic, Department of Medical Sciences and Public Health, University of Cagliari, Cagliari, Cagliari, Italy, ¹⁵Hospital Robert Schuman, Metz, France, ¹⁶Hacettepe University Faculty of Medicine Department of Pediatric Rheumatology Ankara, Türkiye, Ankara, Turkey, ¹⁷Head of the Internal Medicine and Clinical Immunology Department South Île de France Health Hospital Group, Melun Center, Melun, France, ¹⁸Division for clinical immunology and rheumatology, Department of pediatrics UHC Zagreb / School of Medicine Zagreb Croatia, Zagabria, Croatia, ¹⁹Cochin Hospital, Paris, France, ²⁰Université Paris Cité and Université Sorbonne Paris Nord, INSERM, INRAE, Center for Research in Epidemiology and StatisticS (CRESS), Paris, France, Paris, France, ²¹University Paris Cité, Hôpital Saint-Louis, Dermatology department, Paris, Paris, France

Meeting: ACR Convergence 2025

Keywords: autoimmune diseases, Dermatology, glucocorticoids, Therapy, alternative, Vasculitis, Cutaneous

Session Information

Date: Wednesday, October 29, 2025

Title: Abstracts: Vasculitis – Non-ANCA-Associated & Related Disorders II (2699–2704)

Session Type: Abstract Session

Session Time: 11:30AM-11:45AM

Background/Purpose: Immunoglobulin A vasculitis (IgAV) is a small vessel vasculitis marked by IgA, deposition, palpable purpura with lower body predilection and variable joints, kidney and gastrointestinal tract involvement. In 2018, the addendum to the 2012 Chapel Hill Consensus Conference established the recognition of an exclusively or predominantly cutaneous form of the disease, more common in adults. Despite its frequency, standardized management of cutaneous IgA vasculitis remains elusive. The objective of this study was to compare colchicine, dapsone and glucocorticoids (GCs) to induce remission in newly diagnosed or relapsing skin-limited/dominant IgA vasculitis.

Methods: Patients with cutaneous IgAV treated with colchicine, dapsone, or GCs were included between January 1, 2014, and May 1, 2024. Data were collected retrospectively from 38 tertiary centers across eight countries in Europe. Inclusion criteria were age >8 years, biopsy-proven diagnosis of IgAV with evidence of IgA deposition in the skin and/or other organs, newly diagnosed or relapsing IgAV with active skin manifestations; absence of severe organ involvement; and a minimum follow-up of 3 months. The primary endpoint was to evaluate the proportion of patients achieving sustained remission of cutaneous involvement at day 90 (SRD90). Treatments were compared pairwise using inverse probability treatment weighting with the propensity score to adjust for confounders. Variables differing between responders and non-responders and susceptible to be associated with the endpoint were included in the propensity score. Patients receiving multiple therapies were counted per treatment line. Missing data were addressed with multiple imputation by chained equations.

Results: Of the 407 cases identified, 208 patients (114 males, 89 females; median age 44.9 years) were included in the study. Most were enrolled at initial diagnosis (174). At day 90, 109 patients (52.4%) had achieved sustained remission of cutaneous involvement. A total of 164 patients contributing to 216 therapeutic lines were analysed: 113 corresponded to colchicine, 83 to GCs, 20 to dapsone. Variables included in the propensity score were age at diagnosis, gender, necrotic lesions, myalgia and number of therapeutic lines. In the univariate analysis, no significant difference but trends were observed in the proportion of patients with SRD90 when comparing GCs vs colchicine (odds ratio [OR] 1.77 95%CI [0.97 – 3.20], p=0.059) and GCs vs dapsone (OR 1.82 95%CI [0.67 – 4.93], p=0.235). No difference was observed between colchicine and dapsone (OR 0.55 95% CI [1.68 – 5.15], p=0.360]). After weighting, GCs vs. colchicine showed balanced covariates (standardized mean differences < 0.10) and the proportion of SRD90 in the GCs group was higher (OR 1.88, 95%CI [1.04 - 3.41], p=0.034). No balance was achieved in comparisons involving dapsone due to low sample size.

Conclusion: GCs were significantly associated with a more favorable outcome than colchicine in achieving sustained remission of cutaneous involvement. The efficacy of dapsone versus colchicine or GCs could not be assessed using propensity scores, but suggests a similar response rate to colchicine and a lower efficacy compared to GCs.

Disclosures: E. Mariotti: None; B. Sorin: None; W. Lutz: None; C. Grolleau: None; T. Bettuzzi: None; C. Ricordi: None; S. Castañeda: None; L. Herda: None; C. Sunderkotter: Boehringer Ingelheim, 6, GSK (Glaxo Smith Klyne), 6, Vifor, 6; R. Outh: None; R. Paule: None; A. Audemard-Verger: None; M. Caproni: None; A. Marzano: None; P. Quaglino: None; L. Atzori: None; J. Campagne: None; M. Erkan: None; N. Belfeki: None; M. Frkovic: None; N. Dupin: None; R. Porcher: None; M. Jachiet: None; B. Terrier: Amgen, 1, AstraZeneca, 1, 2, GlaxoSmithKlein(GSK), 1, 2, Novartis, 1, 2, Roche, 5, Vifor Pharma, 2.

To cite this abstract in AMA style:

Mariotti E, Sorin B, Lutz W, Grolleau C, Bettuzzi T, Ricordi C, Castañeda S, Herda L, Sunderkotter C, Outh R, Paule R, Audemard-Verger A, Caproni M, Marzano A, Quaglino P, Atzori L, Campagne J, Erkan M, Belfeki N, Frkovic M, Dupin N, Porcher R, Jachiet M, Terrier B. Cutaneous IgA Vasculitis: Emulation of a Target Trial from a European Multicentric Retrospective Study [abstract]. Arthritis Rheumatol. 2025; 77 (suppl 9). https://acrabstracts.org/abstract/cutaneous-iga-vasculitis-emulation-of-a-target-trial-from-a-european-multicentric-retrospective-study/. Accessed .

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