Dynamics of genome architecture and chromatin function during human B cell differentiation and neoplastic transformation

Author:

Vilarrasa-Blasi RoserORCID,Soler-Vila Paula,Verdaguer-Dot Núria,Russiñol Núria,Di Stefano MarcoORCID,Chapaprieta VicenteORCID,Clot Guillem,Farabella IreneORCID,Cuscó Pol,Kulis Marta,Agirre XabierORCID,Prosper Felipe,Beekman Renée,Beà SilviaORCID,Colomer DolorsORCID,Stunnenberg Hendrik G.ORCID,Gut IvoORCID,Campo EliasORCID,Marti-Renom Marc A.ORCID,Martin-Subero José IgnacioORCID

Abstract

AbstractTo investigate the three-dimensional (3D) genome architecture across normal B cell differentiation and in neoplastic cells from different subtypes of chronic lymphocytic leukemia and mantle cell lymphoma patients, here we integrate in situ Hi-C and nine additional omics layers. Beyond conventional active (A) and inactive (B) compartments, we uncover a highly-dynamic intermediate compartment enriched in poised and polycomb-repressed chromatin. During B cell development, 28% of the compartments change, mostly involving a widespread chromatin activation from naive to germinal center B cells and a reversal to the naive state upon further maturation into memory B cells. B cell neoplasms are characterized by both entity and subtype-specific alterations in 3D genome organization, including large chromatin blocks spanning key disease-specific genes. This study indicates that 3D genome interactions are extensively modulated during normal B cell differentiation and that the genome of B cell neoplasias acquires a tumor-specific 3D genome architecture.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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