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The proliferative history shapes the DNA methylome of B-cell tumors and predicts clinical outcome

Authors
 Duran-Ferrer, Marti  ;  Clot, Guillem  ;  Nadeu, Ferran  ;  Beekman, Renee  ;  Baumann, Tycho  ;  Nordlund, Jessica  ;  Marincevic-Zuniga, Yanara  ;  Lonnerholm, Gudmar  ;  Rivas-Delgado, Alfredo  ;  Martin, Silvia  ;  Ordonez, Raquel  ;  Castellano, Giancarlo  ;  Kulis, Marta  ;  Queiros, Ana C.  ;  Lee, Seung-Tae  ;  Wiemels, Joseph  ;  Royo, Romina  ;  Puiggros, Montserrat  ;  Lu, Junyan  ;  Gine, Eva  ;  Bea, Silvia  ;  Jares, Pedro  ;  Agirre, Xabier  ;  Prosper, Felipe  ;  Lopez-Otin, Carlos  ;  Puente, Xose S.  ;  Oakes, Christopher C.  ;  Zenz, Thorsten  ;  Delgado, Julio  ;  Lopez-Guillermo, Armando  ;  Campo, Elias  ;  Ignacio Martin-Subero, Jose 
Citation
 NATURE CANCER, Vol.1(11) : 1066-1081, 2020-11 
Journal Title
NATURE CANCER
ISSN
 2662-1347 
Issue Date
2020-11
Abstract
We report a systematic analysis of the DNA methylation variability in 1,595 samples of normal cell subpopulations and 14 tumor subtypes spanning the entire human B-cell lineage. Differential methylation among tumor entities relates to differences in cellular origin and to de novo epigenetic alterations, which allowed us to build an accurate machine learning-based diagnostic algorithm. We identify extensive individual-specific methylation variability in silenced chromatin associated with the proliferative history of normal and neoplastic B cells. Mitotic activity generally leaves both hyper- and hypomethylation imprints, but some B-cell neoplasms preferentially gain or lose DNA methylation. We construct a DNA-methylation-based mitotic clock, called epiCMIT, whose lapse magnitude represents a strong independent prognostic variable in B-cell tumors and is associated with particular driver genetic alterations. Our findings reveal DNA methylation as a holistic tracer of B-cell tumor developmental history, with implications in differential diagnosis and the prediction of clinical outcome. Martin-Subero and colleagues analyze DNA methylation patterns in B-cell tumors and their normal cells of origin, and develop epiCMIT, a methylation-based mitotic clock with prognostic relevance.
DOI
10.1038/s43018-020-00131-2
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Laboratory Medicine (진단검사의학교실) > 1. Journal Papers
Yonsei Authors
Lee, Seung-Tae(이승태) ORCID logo https://orcid.org/0000-0003-1047-1415
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/185001
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