Diffuse Large B-Cell Lymphoma Classification System That Associates Normal B-Cell Subset Phenotypes With Prognosis

Author:

Dybkær Karen1,Bøgsted Martin1,Falgreen Steffen1,Bødker Julie S.1,Kjeldsen Malene K.1,Schmitz Alexander1,Bilgrau Anders E.1,Xu-Monette Zijun Y.1,Li Ling1,Bergkvist Kim S.1,Laursen Maria B.1,Rodrigo-Domingo Maria1,Marques Sara C.1,Rasmussen Sophie B.1,Nyegaard Mette1,Gaihede Michael1,Møller Michael B.1,Samworth Richard J.1,Shah Rajen D.1,Johansen Preben1,El-Galaly Tarec C.1,Young Ken H.1,Johnsen Hans E.1

Affiliation:

1. Karen Dybkær, Martin Bøgsted, Steffen Falgreen, Julie S. Bødker, Malene K. Kjeldsen, Alexander Schmitz, Anders E. Bilgrau, Kim S. Bergkvist, Maria B. Laursen, Maria Rodrigo-Domingo, Sara C. Marques, Sophie B. Rasmussen, Mette Nyegaard, Michael Gaihede, Preben Johansen, Tarec C. El-Galaly, and Hans E. Johnsen, Aalborg University Hospital; Karen Dybkær, Martin Bøgsted, Anders E. Bilgrau, Maria Rodrigo-Domingo, Michael Gaihede, and Hans E. Johnsen, Aalborg University, Aalborg; Michael B. Møller, Odense...

Abstract

Purpose Current diagnostic tests for diffuse large B-cell lymphoma use the updated WHO criteria based on biologic, morphologic, and clinical heterogeneity. We propose a refined classification system based on subset-specific B-cell–associated gene signatures (BAGS) in the normal B-cell hierarchy, hypothesizing that it can provide new biologic insight and diagnostic and prognostic value. Patients and Methods We combined fluorescence-activated cell sorting, gene expression profiling, and statistical modeling to generate BAGS for naive, centrocyte, centroblast, memory, and plasmablast B cells from normal human tonsils. The impact of BAGS-assigned subtyping was analyzed using five clinical cohorts (treated with cyclophosphamide, doxorubicin, vincristine, and prednisone [CHOP], n = 270; treated with rituximab plus CHOP [R-CHOP], n = 869) gathered across geographic regions, time eras, and sampling methods. The analysis estimated subtype frequencies and drug-specific resistance and included a prognostic meta-analysis of patients treated with first-line R-CHOP therapy. Results Similar BAGS subtype frequencies were assigned across 1,139 samples from five different cohorts. Among R-CHOP–treated patients, BAGS assignment was significantly associated with overall survival and progression-free survival within the germinal center B-cell–like subclass; the centrocyte subtype had a superior prognosis compared with the centroblast subtype. In agreement with the observed therapeutic outcome, centrocyte subtypes were estimated as being less resistant than the centroblast subtype to doxorubicin and vincristine. The centroblast subtype had a complex genotype, whereas the centrocyte subtype had high TP53 mutation and insertion/deletion frequencies and expressed LMO2, CD58, and stromal-1–signature and major histocompatibility complex class II–signature genes, which are known to have a positive impact on prognosis. Conclusion Further development of a diagnostic platform using BAGS-assigned subtypes may allow pathogenetic studies to improve disease management.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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