| Literature DB >> 31698451 |
Juan Carlos Rivera-Mulia1, Takayo Sasaki2, Claudia Trevilla-Garcia1, Naoto Nakamichi3, David J H F Knapp3, Colin A Hammond3, Bill H Chang4, Jeffrey W Tyner5,6, Meenakshi Devidas7, Jared Zimmerman2, Kyle N Klein2, Vivek Somasundaram2, Brian J Druker4, Tanja A Gruber8, Amnon Koren9, Connie J Eaves3, David M Gilbert2,10.
Abstract
Human B-cell precursor acute lymphoid leukemias (BCP-ALLs) comprise a group of genetically and clinically distinct disease entities with features of differentiation arrest at known stages of normal B-lineage differentiation. We previously showed that BCP-ALL cells display unique and clonally heritable, stable DNA replication timing (RT) programs (ie, programs describing the variable order of replication and subnuclear 3D architecture of megabase-scale chromosomal units of DNA in different cell types). To determine the extent to which BCP-ALL RT programs mirror or deviate from specific stages of normal human B-cell differentiation, we transplanted immunodeficient mice with quiescent normal human CD34+ cord blood cells and obtained RT signatures of the regenerating B-lineage populations. We then compared these with RT signatures for leukemic cells from a large cohort of BCP-ALL patients with varied genetic subtypes and outcomes. The results identify BCP-ALL subtype-specific features that resemble specific stages of B-cell differentiation and features that seem to be associated with relapse. These results suggest that the genesis of BCP-ALL involves alterations in RT that reflect biologically significant and potentially clinically relevant leukemia-specific epigenetic changes.Entities:
Year: 2019 PMID: 31698451 PMCID: PMC6855107 DOI: 10.1182/bloodadvances.2019000641
Source DB: PubMed Journal: Blood Adv ISSN: 2473-9529