Somatic Mutations in <i>UBA1</i> and Severe Adult-Onset Autoinflammatory Disease

Beck, David B.; Ferrada, Marcela; Sikora, Keith A.; Ombrello, Amanda K.; Collins, Jason C.; Pei, Wuhong; Balanda, Nicholas; Ross, Daron L.; Cardona, Daniela Ospina; Wu, Zhijie; Patel, Bhavisha; Manthiram, Kalpana; Groarke, Emma M.; Gutierrez-Rodrigues, Fernanda; Hoffmann, Patrycja; Rosenzweig, Sofia; Nakabo, Shuichiro; Dillon, Laura W.; Hourigan, Christopher S.; Tsai, Wanxia Li; Gupta, Sarthak; Carmona‐Rivera, Carmelo; Asmar, Anthony J.; Oda, Hirotsugu; Goodspeed, Wendy; Barron, Karyl S.; Nehrebecky, Michele; Jones, Anne; Laird, Ryan S.; Deuitch, Natalie; Rowczenio, Dorota; Rominger, Emily; Wells, Kristina; Lee, Chyi‐Chia Richard; Wang, Weixin; Trick, Megan; Mullikin, James C.; Wigerblad, Gustaf; Brooks, Stephen R.; Dell’Orso, Stefania; Deng, Zuoming; Chae, Jae Jin; Dulau‐Florea, Alina; Novacic, Danica; Colbert, Robert A.; Kaplan, Mariana J.; Gadina, Massimo; Savic, Sinisa; Lachmann, Helen; Abu‐Asab, Mones; Solomon, Benjamin D.; Retterer, Kyle; Gahl, William A.; Burgess, Shawn M.; Aksentijevich, Ivona; Young, Neal S.; Calvo, Katherine R.; Werner, Achim; Kastner, Daniel L.; Grayson, Peter C.

doi:10.1056/nejmoa2026834

Cited by 746 publications

(1,170 citation statements)

References 42 publications

(34 reference statements)

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“…In addition, a medical history that may cause copper deficiency, such as total parenteral hyperalimentation, is suggestive to diagnosis. In contrast, in VEXAS syndrome, numerous round vacuoles consisting of lipid droplets and disordered cellular organelles occur in myeloid and erythroid precursors [1,2,14].…”

Section: Open Accessmentioning

confidence: 94%

“…To the Editor, VEXAS (vacuoles, E1 enzyme, X-linked, autoinflammatory, somatic) syndrome is a newly-described adult-onset inflammatory syndrome characterized by fevers, cytopenias, vacuoles in myeloid and erythroid precursor cells, dysplastic bone marrow, neutrophilic cutaneous and pulmonary infiltrates, nose and ear chondritis and vasculitis. The syndrome is associated with somatic mutations affecting methionine-41 (p.Met41) in UBA1, an X-chromosome gene encoding ubiquitin-like modifier-activating enzyme 1 [1]. Among the initial 25 patients reported with VEXAS syndrome, 6 met the World Health Organization (WHO) diagnostic criteria for myelodysplastic syndromes (MDS).…”

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confidence: 99%

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VEXAS syndrome in myelodysplastic syndrome with autoimmune disorder

et al. 2021

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VEXAS (vacuoles, E1 enzyme, X-linked, autoinflammatory, somatic) syndrome is a newly-described adult-onset inflammatory syndrome characterized by vacuoles in myeloid and erythroid precursor cells and somatic mutations affecting methionine-41 (p.Met41) in UBA1. The VEXAS syndrome often overlaps with myelodysplastic syndromes (MDS) with autoimmune disorders (AD). By screening the UBA1 gene sequences derived from MDS patients with AD from our center, we identified one patient with a p.Met41Leu missense mutation in UBA1, who should have been diagnosed as MDS comorbid with VEXAS syndrome. This patient respond poorly to immune suppressive drugs. Patients with MDS and AD who have characteristic vacuoles in myeloid and erythroid precursor cells should be screened for UBA1 mutation, these patients are likely to have VEXAS syndrome and unlikely to improve with immunosuppressive drugs and should be considered for other alternative therapies.

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Section: Open Accessmentioning

confidence: 94%

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confidence: 99%

VEXAS syndrome in myelodysplastic syndrome with autoimmune disorder

et al. 2021

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“…However, recently published data suggests myeloid activation may be even further upstream, as early as the bone marrow, given the prominent left shift seen by CyToF in patients with untreated GCA (80). Supporting this, GCA can occur as a paraneoplastic phenomenon to myelodysplastic/ myeloproliferative neoplasms as well as in the recently described somatic, myeloid-activating autoinflammatory condition VEXAS (173,174). Upon breach of vascular immunoprivilege, preactivated monocytes and CD4 + T cells mutually enter the vessel and cooperate to destroy it.…”

Section: Perspectives and Future Directionsmentioning

confidence: 88%

The Immunopathology of Giant Cell Arteritis Across Disease Spectra

2021

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Giant cell arteritis (GCA) is a granulomatous systemic vasculitis of large- and medium-sized arteries that affects the elderly. In recent years, advances in diagnostic imaging have revealed a greater degree of large vessel involvement than previously recognized, distinguishing classical cranial- from large vessel (LV)- GCA. GCA often co-occurs with the poorly understood inflammatory arthritis/bursitis condition polymyalgia rheumatica (PMR) and has overlapping features with other non-infectious granulomatous vasculitides that affect the aorta, namely Takayasu Arteritis (TAK) and the more recently described clinically isolated aortitis (CIA). Here, we review the literature focused on the immunopathology of GCA on the background of the three settings in which comparisons are informative: LV and cranial variants of GCA; PMR and GCA; the three granulomatous vasculitides (GCA, TAK, and CIA). We discuss overlapping and unique features between these conditions across clinical presentation, epidemiology, imaging, and conventional histology. We propose a model of GCA where abnormally activated circulating cells, especially monocytes and CD4+ T cells, enter arteries after an unknown stimulus and cooperate to destroy it and review the evidence for how this mechanistically occurs in active disease and improves with treatment.

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“…On en veut pour preuve la description toute récente de formes congénitales de cristallinopathie αB à transmission dominante [22]. Cet adage vaut aussi pour des maladies beaucoup plus fréquentes comme l'illustre parfaitement, et dans un autre domaine, des mutations somatiques du gène UBA1 dans des pathologies inflammatoires de l'adulte [23]. A contrario, il faut se garder de sur-interpréter des résultats de NGS en validant trop facilement la pathogénicité de certains variants de séquence, ces derniers pouvant être des simples polymorphismes.…”

Section: Des Moyens Limités En Pathologie Neuromusculaireunclassified

L’Homme Gelé (渐冻人) et le déficit en cristalline αB

Urtizberea

Kaplan²

2020

Med Sci (Paris)

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La philosophie confucéenne nous enseigne que la recherche de la vérité n’emprunte pas toujours un chemin rectiligne. L’observation clinique présentée ici l’illustre parfaitement. Il y est question d’un enfant souffrant d’une maladie neuromusculaire rare (en chinois, le mot myopathie se traduit par 渐冻人 soit « homme gelé ») chez qui fut suspecté un déficit en cristalline αB. Les auteurs profitent de l’occasion pour mettre le projecteur sur la Chine, ce grand pays qui n’a pas attendu Alain Peyrefitte pour s’éveiller ou, plus exactement, se réveiller. à la lumière de missions passées et récentes dans l’ex-Empire du Milieu, le point est fait sur les enjeux médico-scientifiques mais aussi sociétaux de ce pays en passe de devenir, peut-être, un géant dans le domaine des maladies neuromusculaires.

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Somatic Mutations in UBA1 and Severe Adult-Onset Autoinflammatory Disease

Cited by 746 publications

References 42 publications

VEXAS syndrome in myelodysplastic syndrome with autoimmune disorder

VEXAS syndrome in myelodysplastic syndrome with autoimmune disorder

The Immunopathology of Giant Cell Arteritis Across Disease Spectra

L’Homme Gelé (渐冻人) et le déficit en cristalline αB

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