Further characterization of clinical and laboratory features in VEXAS syndrome: large‐scale analysis of a multicentre case series of 116 French patients*

Sophie Georgin‐Lavialle(Sorbonne Université), Benjamin Terrier(Université Paris Cité), Alexis F. Guédon(Inserm), Maël Heiblig(Hospices Civils de Lyon), T. Comont(Université Fédérale de Toulouse Midi-Pyrénées), Estibaliz Lazaro(Hôpital Cardiologique du Haut-Lévêque), Valentin Lacombe(Université d'Angers), Louis Terriou, Samuel Ardois(Centre Hospitalier Universitaire de Rennes), Jean‐David Bouaziz(Inserm), Alexis Mathian(Assistance Publique – Hôpitaux de Paris), G. Le Guenno(Hôpital Saint-André), Achille Aouba(Université de Caen Normandie), R. Outh(Centre Hospitalier de Perpignan), A. Meyer(Hôpital Civil, Strasbourg), Marielle Roux‐Sauvat, Mikaël Ebbo(Aix-Marseille Université), Lin‐Pierre Zhao, Adrien Bigot(Université de Tours), Yvan Jamilloux(Hospices Civils de Lyon), Vivien Guillotin(Hôpital Saint-André), Edouard Flamarion(Université Paris Cité), Pierrick Henneton(Société Française de Médecine Vasculaire), Guillaume Vial(Hôpital Saint-André), Vincent Jachiet(Sorbonne Université), Julien Rossignol(Université Paris Cité), S. Vinzio(Groupe Hospitalier Mutualiste de Grenoble), Thierry Weitten(Centre Hospitalier Intercommunal Castres-Mazamet), J. Vinit, C. Deligny(Centre Hospitalier Universitaire de Martinique), S. Humbert(Centre Hospitalier Universitaire de Besançon), Maxime Samson(Maison des Sciences sociales et des Humanités de Dijon), N. Magy‐Bertrand(Centre Hospitalier Universitaire de Besançon), T. Moulinet(Centre National de la Recherche Scientifique), R. Bourguiba(Sorbonne Université), Thomas Hanslik(Hôpital Ambroise-Paré), Claude Bachmeyer(Sorbonne Université), Marie Sébert(Assistance Publique – Hôpitaux de Paris), Marie Kostine(Hôpital Cardiologique du Haut-Lévêque), Boris Bienvenu(Hôpital Saint Joseph), P. Biscay(Clinique Mutualiste de l'Estuaire), É. Liozon(Hôpital Dupuytren), L. Sailler(Université Fédérale de Toulouse Midi-Pyrénées), François Chasset(Sorbonne Université), Alexandra Audemard‐Verger(Université de Tours), Eugénie Duroyon, Guillaume Sarrabay(Université de Montpellier), Felippe Borlot(Centre Hospitalier de Béziers), C. Diéval(Centre Hospitalier de Rochefort), Thomas Cluzeau, Paola Marianetti(Centre Hospitalier Universitaire de Reims), Hervé Lobbes(Hôpital Saint-André), Guilaine Boursier(Université de Montpellier), Mathieu Gerfaud‐Valentin(Hospices Civils de Lyon), Juliette Jeannel(Université Paris Cité), Amélie Servettaz(Centre Hospitalier Universitaire de Reims), Sylvain Audia(Maison des Sciences sociales et des Humanités de Dijon), M. Larue(Hôpitaux Universitaires Henri-Mondor), Basile Henriot(Centre Hospitalier René-Dubos), B. Faucher(Aix-Marseille Université), J. Graveleau(Centre Hospitalier Universitaire de Nantes), B. De Sainte Marie(Hôpital Saint-André), Joris Galland(Int'Air Medical (France)), Laurence Bouillet(Centre Hospitalier Universitaire de Grenoble), Catherine Arnaud(Université Fédérale de Toulouse Midi-Pyrénées), Lionel Adès(Assistance Publique – Hôpitaux de Paris), Fabrice Carrat(Inserm), Pierre Hirsch(Sorbonne Université), Pierre Fenaux(Assistance Publique – Hôpitaux de Paris), O. Fain(Sorbonne Université), Pierre Sujobert(Centre Hospitalier Universitaire de Besançon), Olivier Kosmider, A. Mékinian(Sorbonne Université), French VEXAS group, GFEV, GFM, CEREMAIA, MINHEMON
British Journal of Dermatology
October 11, 2021
10.1111/bjd.20805
Cited by 410Open Access
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Abstract

BACKGROUND: A new autoinflammatory syndrome related to somatic mutations of UBA1 was recently described and called VEXAS syndrome ('Vacuoles, E1 Enzyme, X-linked, Autoinflammatory, Somatic syndrome'). OBJECTIVES: To describe clinical characteristics, laboratory findings and outcomes of VEXAS syndrome. METHODS: One hundred and sixteen patients with VEXAS syndrome were referred to a French multicentre registry between November 2020 and May 2021. The frequency and median of parameters and vital status, from diagnosis to the end of the follow-up, were recorded. RESULTS: The main clinical features of VEXAS syndrome were found to be skin lesions (83%), noninfectious fever (64%), weight loss (62%), lung involvement (50%), ocular symptoms (39%), relapsing chondritis (36%), venous thrombosis (35%), lymph nodes (34%) and arthralgia (27%). Haematological disease was present in 58 cases (50%): myelodysplastic syndrome (MDS; n = 58) and monoclonal gammopathy of unknown significance (n = 12; all patients with MGUS also have a MDS). UBA1 mutations included p.M41T (45%), p.M41V (30%), p.M41L (18%) and splice mutations (7%). After a median follow-up of 3 years, 18 patients died (15·5%; nine of infection and three due to MDS progression). Unsupervised analysis identified three clusters: cluster 1 (47%; mild-to-moderate disease); cluster 2 (16%; underlying MDS and higher mortality rates); and cluster 3 (37%; constitutional manifestations, higher C-reactive protein levels and less frequent chondritis). The 5-year probability of survival was 84·2% in cluster 1, 50·5% in cluster 2 and 89·6% in cluster 3. The UBA1 p.Met41Leu mutation was associated with a better prognosis. CONCLUSIONS: VEXAS syndrome has a large spectrum of organ manifestations and shows different clinical and prognostic profiles. It also raises a potential impact of the identified UBA1 mutation.

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