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Chromatin activation as a unifying principle underlying pathogenic mechanisms in multiple myeloma.


ABSTRACT: Multiple myeloma (MM) is a plasma cell neoplasm associated with a broad variety of genetic lesions. In spite of this genetic heterogeneity, MMs share a characteristic malignant phenotype whose underlying molecular basis remains poorly characterized. In the present study, we examined plasma cells from MM using a multi-epigenomics approach and demonstrated that, when compared to normal B cells, malignant plasma cells showed an extensive activation of regulatory elements, in part affecting coregulated adjacent genes. Among target genes up-regulated by this process, we found members of the NOTCH, NF-kB, MTOR signaling, and TP53 signaling pathways. Other activated genes included sets involved in osteoblast differentiation and response to oxidative stress, all of which have been shown to be associated with the MM phenotype and clinical behavior. We functionally characterized MM-specific active distant enhancers controlling the expression of thioredoxin (TXN), a major regulator of cellular redox status and, in addition, identified PRDM5 as a novel essential gene for MM. Collectively, our data indicate that aberrant chromatin activation is a unifying feature underlying the malignant plasma cell phenotype.

SUBMITTER: Ordonez R 

PROVIDER: S-EPMC7545147 | biostudies-literature | 2020 Sep

REPOSITORIES: biostudies-literature

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Chromatin activation as a unifying principle underlying pathogenic mechanisms in multiple myeloma.

Ordoñez Raquel R   Kulis Marta M   Russiñol Nuria N   Chapaprieta Vicente V   Carrasco-Leon Arantxa A   García-Torre Beatriz B   Charalampopoulou Stella S   Clot Guillem G   Beekman Renée R   Meydan Cem C   Duran-Ferrer Martí M   Verdaguer-Dot Núria N   Vilarrasa-Blasi Roser R   Soler-Vila Paula P   Garate Leire L   Miranda Estíbaliz E   San José-Enériz Edurne E   Rodriguez-Madoz Juan R JR   Ezponda Teresa T   Martínez-Turrilas Rebeca R   Vilas-Zornoza Amaia A   Lara-Astiaso David D   Dupéré-Richer Daphné D   Martens Joost H A JHA   El-Omri Halima H   Taha Ruba Y RY   Calasanz Maria J MJ   Paiva Bruno B   San Miguel Jesus J   Flicek Paul P   Gut Ivo I   Melnick Ari A   Mitsiades Constantine S CS   Licht Jonathan D JD   Campo Elias E   Stunnenberg Hendrik G HG   Agirre Xabier X   Prosper Felipe F   Martin-Subero Jose I JI  

Genome research 20200820 9


Multiple myeloma (MM) is a plasma cell neoplasm associated with a broad variety of genetic lesions. In spite of this genetic heterogeneity, MMs share a characteristic malignant phenotype whose underlying molecular basis remains poorly characterized. In the present study, we examined plasma cells from MM using a multi-epigenomics approach and demonstrated that, when compared to normal B cells, malignant plasma cells showed an extensive activation of regulatory elements, in part affecting coregula  ...[more]

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