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UTX inactivation in germinal center B cells promotes the development of multiple myeloma with extramedullary disease.

Ola RizqNaoya MimuraMotohiko OshimaShuji MomoseNaoya TakayamaNaoki ItokawaShuhei KoideAsuka ShibamiyaYurie Miyamoto-NagaiMohamed RizkYaeko Nakajima-TakagiKazumasa AoyamaChangshan WangAtsunori SarayaMasanori SeimiyaMariko WatanabeSatoshi YamasakiTatsuhiro ShibataKiyoshi YamaguchiYoichi FurukawaTetsuhiro ChibaEmiko SakaidaChiaki NakasekoJun-Ichi TamaruYu-Tzu TaiKenneth C AndersonHiroaki HondaAtsushi Iwama
Published in: Leukemia (2023)
UTX/KDM6A, a histone H3K27 demethylase and a key component of the COMPASS complex, is frequently lost or mutated in cancer; however, its tumor suppressor function remains largely uncharacterized in multiple myeloma (MM). Here, we show that the conditional deletion of the X-linked Utx in germinal center (GC) derived cells collaborates with the activating Braf V600E mutation and promotes induction of lethal GC/post-GC B cell malignancies with MM-like plasma cell neoplasms being the most frequent. Mice that developed MM-like neoplasms showed expansion of clonal plasma cells in the bone marrow and extramedullary organs, serum M proteins, and anemia. Add-back of either wild-type UTX or a series of mutants revealed that cIDR domain, that forms phase-separated liquid condensates, is largely responsible for the catalytic activity-independent tumor suppressor function of UTX in MM cells. Utx loss in concert with Braf V600E only slightly induced MM-like profiles of transcriptome, chromatin accessibility, and H3K27 acetylation, however, it allowed plasma cells to gradually undergo full transformation through activation of transcriptional networks specific to MM that induce high levels of Myc expression. Our results reveal a tumor suppressor function of UTX in MM and implicate its insufficiency in the transcriptional reprogramming of plasma cells in the pathogenesis of MM.
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