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dc.contributor.authorKataoka, Asamien
dc.contributor.authorMizumoto, Chisakien
dc.contributor.authorKanda, Junyaen
dc.contributor.authorIwasaki, Makotoen
dc.contributor.authorSakurada, Makien
dc.contributor.authorOka, Tomomien
dc.contributor.authorFujimoto, Masakazuen
dc.contributor.authorYamamoto, Yosukeen
dc.contributor.authorYamashita, Koheien
dc.contributor.authorNannya, Yasuhitoen
dc.contributor.authorOgawa, Seishien
dc.contributor.authorTakaori-Kondo, Akifumien
dc.contributor.alternative片岡, 阿沙美ja
dc.contributor.alternative水本, 智咲ja
dc.contributor.alternative諫田, 淳也ja
dc.contributor.alternative岩﨑, 惇ja
dc.contributor.alternative櫻田, 麻希ja
dc.contributor.alternative岡, 知美ja
dc.contributor.alternative藤本, 正数ja
dc.contributor.alternative山本, 洋介ja
dc.contributor.alternative山下, 浩平ja
dc.contributor.alternative南谷, 泰仁ja
dc.contributor.alternative小川, 誠司ja
dc.contributor.alternative髙折, 晃史ja
dc.date.accessioned2023-06-21T05:26:19Z-
dc.date.available2023-06-21T05:26:19Z-
dc.date.issued2023-06-
dc.identifier.urihttp://hdl.handle.net/2433/283385-
dc.description.abstractVEXAS (vacuoles, E1 enzyme, X-linked, autoinflammatory, somatic) syndrome is caused by UBA1 somatic mutations and is characterized by late-onset systemic autoimmune inflammation and blood abnormalities such as cytopenia, vacuolation of myeloid/erythroblastic cells, and myelodysplastic syndrome (MDS). It is often resistant to immunosuppressive therapy, and no treatment strategy has been established. A 65-year-old man presented with palpable erythema, fever, macrocytic anemia, and arthralgia. He was subsequently diagnosed with MDS complicated by Sweet's disease. Treatment with azacitidine was initiated due to suspected skin invasion by MDS cells and resistance of the skin rash to steroid therapy. Next-generation sequencing of bone marrow samples prior to treatment initiation revealed the presence of UBA1 p.M41L (VAF 0.38) and DNMT3A p.L605fs mutations (VAF 0.184). Based on the findings of systemic inflammation, a diagnosis of VEXAS syndrome was made. The fever and skin rash improved with azacitidine therapy. In conclusion, somatic mutations in UBA1 should be explored in patients with MDS exhibiting systemic autoimmune inflammation. Furthermore, azacitidine may be a good treatment option for systemic autoinflammation in MDS associated with VEXAS syndrome.en
dc.language.isoeng-
dc.publisherJapanese Society of Hematologyen
dc.publisherSpringer Natureen
dc.publisher.alternative日本血液学会ja
dc.rights© Japanese Society of Hematology 2023en
dc.rightsThis manuscript is deposited under the publisher's permission.en
dc.rightsThe original publication is available at www.springerlink.comen
dc.rightsThe full-text file will be made open to the public on 14 January 2024 in accordance with publisher's 'Terms and Conditions for Self-Archiving'.en
dc.rightsThis is not the published version. Please cite only the published version. この論文は出版社版でありません。引用の際には出版社版をご確認ご利用ください。en
dc.subjectVEXAS syndromeen
dc.subjectMyelodysplastic syndromeen
dc.subjectAzacitidineen
dc.subjectUBA1 mutationen
dc.subjectDNMT3A mutationen
dc.titleSuccessful azacitidine therapy for myelodysplastic syndrome associated with VEXAS syndromeen
dc.typejournal article-
dc.type.niitypeJournal Article-
dc.identifier.jtitleInternational Journal of Hematologyen
dc.identifier.volume117-
dc.identifier.issue6-
dc.identifier.spage919-
dc.identifier.epage924-
dc.relation.doi10.1007/s12185-023-03532-y-
dc.textversionauthor-
dc.identifier.pmid36641501-
dcterms.accessRightsembargoed access-
datacite.date.available2024-01-14-
datacite.awardNumber18H02836-
datacite.awardNumber.urihttps://kaken.nii.ac.jp/grant/KAKENHI-PROJECT-18H02836/-
dc.identifier.pissn0925-5710-
dc.identifier.eissn1865-3774-
jpcoar.funderName日本学術振興会ja
jpcoar.awardTitleTP53変異陽性MDSに対する脱メチル化剤有効性メカニズムの解明ja
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