Revisiting beta‐2 microglobulin as a prognostic marker in diffuse large B‐cell lymphoma

Author:

Jelicic Jelena1ORCID,Juul‐Jensen Karen1,Bukumiric Zoran2,Runason Simonsen Mikkel3,Roost Clausen Michael4,Ludvigsen Al‐Mashhadi Ahmed35,Schou Pedersen Robert6,Bjørn Poulsen Christian78,Ortved Gang Anne89,Brown Peter89ORCID,El‐Galaly Tarec Christoffer13,Larsen Thomas Stauffer110ORCID

Affiliation:

1. Department of Hematology Odense University Hospital Odense Denmark

2. Faculty of Medicine Institute for Medical Statistics and Informatics, University of Belgrade Belgrade Serbia

3. Department of Hematology, Clinical Cancer Research Center Aalborg University Hospital Aalborg Denmark

4. Department of Hematology Vejle Hospital, Sygehus Lillebaelt Vejle Denmark

5. Department of Hematology Aarhus University Hospital Aarhus Denmark

6. Department of Hematology Regional Hospital Gødstrup Herning Denmark

7. Department of Hematology Zealand University Hospital Roskilde Denmark

8. Department of Clinical Medicine University of Copenhagen Kobenhavn Denmark

9. Department of Hematology Copenhagen University Hospital, Rigshospitalet Copenhagen Denmark

10. Department of Clinical Research University of Southern Denmark Odense Denmark

Abstract

AbstractBackgroundSeveral clinical prognostic models for diffuse large B‐cell lymphoma (DLBCL) have been proposed, including the most commonly used International Prognostic Index (IPI), the National Comprehensive Cancer Network IPI (NCCN‐IPI), and models incorporating beta‐2 microglobulin (β2M). However, the role of β2M in DLBCL patients is not fully understood.MethodsWe identified 6075 patients with newly diagnosed DLBCL treated with immunochemotherapy registered in the Danish Lymphoma Registry.ResultsA total of 3232 patients had data available to calculate risk scores from each of the nine considered risk models for DLBCL, including a model developed from our population. Three of four models with β2M and NCCN‐IPI performed better than the International Prognostic Indexes (IPI, age‐adjusted IPI, and revised IPI). Five‐year overall survival for high‐ and low‐risk patients were 43.6% and 86.4% for IPI and 34.9% and 96.2% for NCCN‐IPI. In univariate analysis, higher levels of β2M were associated with inferior survival, higher tumor burden (advanced clinical stage and bulky disease), previous malignancy and increased age, and creatinine levels. Furthermore, we developed a model (β2M‐NCCN‐IPI) by adding β2M to NCCN‐IPI (c‐index 0.708) with improved discriminatory ability compared to NCCN‐IPI (c‐index 0.698, p < 0.05) and 5‐year OS of 33.1%, 56.2%, 82.4%, and 96.4% in the high, high‐intermediate, low‐intermediate and low‐risk group, respectively.ConclusionInternational Prognostic Indices, except for NCCN‐IPI, fail to accurately discriminate risk groups in the rituximab era. β2M, a readily available marker, could improve the discriminatory performance of NCCN‐IPI and should be re‐evaluated in the development setting of future models for DLBCL.

Publisher

Wiley

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