| Literature DB >> 28368397 |
X Guo1, J L Koff1, A B Moffitt2, M Cinar1, S Ramachandiran1, Z Chen3, J M Switchenko3, M Mosunjac4, S G Neill4, K P Mann4, M Bagirov4, Y Du5, Y Natkunam6, H J Khoury1, M R Rossi7, W Harris1, C R Flowers1, I S Lossos8, L H Boise1, S S Dave2, J Kowalski1,3, L Bernal-Mizrachi1.
Abstract
Diffuse large B-cell lymphoma (DLBCL) has been categorized into two molecular subtypes that have prognostic significance, namely germinal center B-cell like (GCB) and activated B-cell like (ABC). Although ABC-DLBCL has been associated with NF-κB activation, the relationships between activation of specific NF-κB signals and DLBCL phenotype remain unclear. Application of novel gene expression classifiers identified two new DLBCL categories characterized by selective p100 (NF-κB2) and p105 (NF-κB1) signaling. Interestingly, our molecular studies showed that p105 signaling is predominantly associated with GCB subtype and histone mutations. Conversely, most tumors with p100 signaling displayed ABC phenotype and harbored ABC-associated mutations in genes such as MYD88 and PIM1. In vitro, MYD88 L265P mutation promoted p100 signaling through TAK1/IKKα and GSK3/Fbxw7a pathways, suggesting a novel role for this protein as an upstream regulator of p100. p100 signaling was engaged during activation of normal B cells, suggesting p100's role in ABC phenotype development. Additionally, silencing p100 in ABC-DLBCL cells resulted in a GCB-like phenotype, with suppression of Blimp, IRF4 and XBP1 and upregulation of BCL6, whereas introduction of p52 or p100 into GC cells resulted in differentiation toward an ABC-like phenotype. Together, these findings identify specific roles for p100 and p105 signaling in defining DLBCL molecular subtypes and posit MYD88/p100 signaling as a regulator for B-cell activation.Entities:
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Year: 2017 PMID: 28368397 DOI: 10.1038/onc.2017.90
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867