Azacitidine in VEXAS: Up-Front Multidisciplinary Treatment or a Last Resort?

VEXAS (vacuoles, E1 enzyme, X-linked, autoinflammatory, somatic) syndrome is a recently characterised adult-onset autoinflammatory disorder driven by acquired mutations in UBA1. We present the diagnostic and therapeutic journey of a 64-year-old man whose multisystem disease illustrates the complexity—and promise—of managing VEXAS through a multidisciplinary lens. Initially labelled as post-viral fatigue, the patient developed escalating systemic features in late 2023, including rash, migratory polyarthritis, lymphadenopathy, non-specific intestinal inflammation, pulmonary infiltrates, thrombocytopoenia, and transfusion-dependent macrocytic anaemia. Skin and bone histopathology revealed small-vessel vasculitis and hyperplastic marrow, respectively. A peripheral blood UBA1 pathogenic variant c.122T>C p.(Met41Thr) was detected (variant allele frequency—also known as VAF—74%) in December 2023, securing the diagnosis. Corticosteroids induced partial remission but could not be weaned without flare. In September 2024, azacitidine was initiated as a disease-modifying agent. Over nine cycles, inflammatory markers normalised, haemoglobin improved from 83 g/L to 144 g/L, and UBA1 VAF fell to 46%. Corticosteroid tapering was achieved down to prednisolone 2.5 mg daily without clinical relapse. Multidisciplinary coordination between haematology, immunology, and rheumatology was pivotal. Input was required to coordinate azatadine infusions, interpret a co-existent DNMT3A pathogenic variant detected on marrow next-generation sequencing (VAF 44%), monitor clinical and molecular remission, and navigate complications, including atrial fibrillation and HSV-1 reactivation. The patient continues on azacitidine with plans for repeat molecular assessment at cycle 12.