VEXAS Syndrome: First Genetically Confirmed Case Report from Tunisia.
Curr Rheumatol Rev 2026 May 07. [Online ahead of print]

Abstract

BACKGROUND

VEXAS syndrome (Vacuoles, E1 enzyme, X-linked, autoinflammatory, somatic) is a recently described adult-onset autoinflammatory disease caused by somatic mutations in the UBA1 gene. Its heterogeneous clinical presentation frequently overlaps with inflammatory, autoimmune, and hematological disorders, resulting in diagnostic delay. We report the first genetically confirmed case of VEXAS syndrome in Tunisia and highlight its clinical complexity, with particular emphasis on cardiac and ocular involvement, as well as therapeutic management in light of current literature.

CASE PRESENTATION

A 70-year-old man followed at a tertiary university hospital in Tunisia presented with recurrent fever, weight loss, inflammatory arthritis, recurrent myopericarditis, ocular inflammation, skin lesions, peripheral neuropathy, and cytopenias. Laboratory investigations showed severe macrocytic anemia and markedly elevated inflammatory markers. After extensive exclusion of infectious, autoimmune, and malignant etiologies, molecular analysis identified a pathogenic somatic UBA1 mutation (p.Met41Thr), confirming the diagnosis of VEXAS syndrome. High-dose systemic corticosteroid therapy resulted in rapid initial clinical and biological improvement; however, infectious complications and disease relapse occurred during dose tapering.

CONCLUSION

This case highlights the multisystemic and progressive nature of VEXAS syndrome and reinforces the role of corticosteroids as first-line therapy, while underlining their limitations. Awareness of this emerging entity and early genetic testing are essential to optimize management and reduce morbidity.

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Authors+Show Affiliations

Oumaima C0009-0005-7572-4809Endocrinology and Internal Medicine Department, University Hospital Center (CHU) Taher Sfar Mahdia, Faculty of Medicine of Monastir - University of Monastir, Tunisia.
Marwa BBEndocrinology and Internal Medicine Department, University Hospital Center (CHU) Taher Sfar Mahdia, Faculty of Medicine of Monastir - University of Monastir, Tunisia. Research Laboratory LR12ES05 Lab-NAFS 'Nutrition - Functional Food & Health' Faculty of Medicine of Monastir - University of Monastir, Tunisia.
Sondes A0000-0001-7797-4899Endocrinology and Internal Medicine Department, University Hospital Center (CHU) Taher Sfar Mahdia, Faculty of Medicine of Monastir - University of Monastir, Tunisia. Research Laboratory LR12ES05 Lab-NAFS 'Nutrition - Functional Food & Health' Faculty of Medicine of Monastir - University of Monastir, Tunisia.
Amel BEndocrinology and Internal Medicine Department, University Hospital Center (CHU) Taher Sfar Mahdia, Faculty of Medicine of Monastir - University of Monastir, Tunisia. Research Laboratory LR12ES05 Lab-NAFS 'Nutrition - Functional Food & Health' Faculty of Medicine of Monastir - University of Monastir, Tunisia.
Rim BDepartment of Internal medicine, Hôpital des Forces de sécurité intérieur, la Marsa Tunisie, Université Tunis el Manar, Faculté de médecine de Tunis, Tunisie.
Houweyda JUniversity of Tunis El Manar Genetics department, Mongi Slim Hospital, Tunis, Tunisia, Faculty of Medicine of Tunis Tunis Tunisia. Research laboratory LR22SP01, Mongi Slim Hospital, Tunis, TunisiA.
Sameh MUniversity Hospital Center (CHU) Taher Sfar Mahdia, Ophthalmology Department, Faculty of Medicine - University of Monastir, Tunisia.
Olfa BEndocrinology and Internal Medicine Department, University Hospital Center (CHU) Taher Sfar Mahdia, Faculty of Medicine of Monastir - University of Monastir, Tunisia. Research Laboratory LR12ES05 Lab-NAFS 'Nutrition - Functional Food & Health' Faculty of Medicine of Monastir - University of Monastir, Tunisia.

Pub Type(s)

Case Reports
Journal Article

Language

eng

PubMed ID

42136441