RNA-sequencing based first choice of treatment and determination of risk in multiple myeloma

Martina Emde-Rajaratnam; Susanne Beck; Vladimir Benes; Hans Salwender; Uta Bertsch; Christoph Scheid; Mathias Hänel; Katja Weisel; Thomas Hielscher; Marc S Raab; Hartmut Goldschmidt; Anna Jauch; Ken Maes; Elke De Bruyne; Eline Menu; Kim De Veirman; Jérôme Moreaux; Karin Vanderkerken; Anja Seckinger; Dirk Hose

doi:10.3389/fimmu.2023.1286700

RNA-sequencing based first choice of treatment and determination of risk in multiple myeloma

Front Immunol. 2023 Nov 15:14:1286700. doi: 10.3389/fimmu.2023.1286700. eCollection 2023.

Authors

Martina Emde-Rajaratnam¹, Susanne Beck^{1

2}, Vladimir Benes³, Hans Salwender⁴, Uta Bertsch⁵, Christoph Scheid⁶, Mathias Hänel⁷, Katja Weisel⁸, Thomas Hielscher⁹, Marc S Raab⁵, Hartmut Goldschmidt^{5

10}, Anna Jauch¹¹, Ken Maes¹, Elke De Bruyne¹, Eline Menu¹, Kim De Veirman¹, Jérôme Moreaux¹², Karin Vanderkerken¹, Anja Seckinger^#¹, Dirk Hose^#¹

Affiliations

¹ Department of Hematology and Immunology, Myeloma Center Brussels & Labor für Myelomforschung, Vrije Universiteit Brussel (VUB), Jette, Belgium.
² Universitätsklinikum Heidelberg, Molekularpathologisches Zentrum, Heidelberg, Germany.
³ Europäisches Laboratorium für Molekularbiologie, GeneCore, Heidelberg, Germany.
⁴ Asklepios Tumorzentrum Hamburg, AK Altona and St. Georg, Hamburg, Germany.
⁵ Universitätsklinikum Heidelberg, Medizinische Klinik V, Heidelberg, Germany.
⁶ Department I of Internal Medicine, University of Cologne, Cologne, Germany.
⁷ Department of Internal Medicine III, Klinikum Chemnitz GmbH, Chemnitz, Germany.
⁸ Department of Oncology, Hematology and Bone Marrow Transplantation with Section of Pneumology, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.
⁹ Deutsches Krebsforschungszentrum, Abteilung für Biostatistik, Heidelberg, Germany.
¹⁰ Nationales Centrum für Tumorerkrankungen, Heidelberg, Germany.
¹¹ Universität Heidelberg, Institut für Humangenetik, Heidelberg, Germany.
¹² Institute of Human Genetics, UMR 9002 CNRS-UM, Montpellier, France.

^# Contributed equally.

Abstract

Background: Immunotherapeutic targets in multiple myeloma (MM) have variable expression height and are partly expressed in subfractions of patients only. With increasing numbers of available compounds, strategies for appropriate choice of targets (combinations) are warranted. Simultaneously, risk assessment is advisable as patient's life expectancy varies between months and decades.

Methods: We first assess feasibility of RNA-sequencing in a multicenter trial (GMMG-MM5, n=604 patients). Next, we use a clinical routine cohort of untreated symptomatic myeloma patients undergoing autologous stem cell transplantation (n=535, median follow-up (FU) 64 months) to perform RNA-sequencing, gene expression profiling (GEP), and iFISH by ten-probe panel on CD138-purified malignant plasma cells. We subsequently compare target expression to plasma cell precursors, MGUS (n=59), asymptomatic (n=142) and relapsed (n=69) myeloma patients, myeloma cell lines (n=26), and between longitudinal samples (MM vs. relapsed MM). Data are validated using the independent MMRF CoMMpass-cohort (n=767, FU 31 months).

Results: RNA-sequencing is feasible in 90.8% of patients (GMMG-MM5). Actionable immune-oncological targets (n=19) can be divided in those expressed in all normal and >99% of MM-patients (CD38, SLAMF7, BCMA, GPRC5D, FCRH5, TACI, CD74, CD44, CD37, CD79B), those with expression loss in subfractions of MM-patients (BAFF-R [81.3%], CD19 [57.9%], CD20 [82.8%], CD22 [28.4%]), aberrantly expressed in MM (NY-ESO1/2 [12%], MUC1 [12.7%], CD30 [4.9%], mutated BRAF V600E/K [2.1%]), and resistance-conveying target-mutations e.g., against part but not all BCMA-directed treatments. Risk is assessable regarding proliferation, translated GEP- (UAMS70-, SKY92-, RS-score) and de novo (LfM-HRS) defined risk scores. LfM-HRS delineates three groups of 40%, 38%, and 22% of patients with 5-year and 12-year survival rates of 84% (49%), 67% (18%), and 32% (0%). R-ISS and RNA-sequencing identify partially overlapping patient populations, with R-ISS missing, e.g., 30% (22/72) of highly proliferative myeloma.

Conclusion: RNA-sequencing based assessment of risk and targets for first choice treatment is possible in clinical routine.

Keywords: RNA-sequencing; immunotherapeutic targets; multiple myeloma; personalized treatment; proliferation; risk-adapted treatment; survival.

Copyright © 2023 Emde-Rajaratnam, Beck, Benes, Salwender, Bertsch, Scheid, Hänel, Weisel, Hielscher, Raab, Goldschmidt, Jauch, Maes, De Bruyne, Menu, De Veirman, Moreaux, Vanderkerken, Seckinger and Hose.

Publication types

Multicenter Study
Research Support, Non-U.S. Gov't

MeSH terms

B-Cell Maturation Antigen
Hematopoietic Stem Cell Transplantation*
Humans
Multiple Myeloma* / drug therapy
Multiple Myeloma* / therapy
RNA
Transplantation, Autologous

Substances

RNA
B-Cell Maturation Antigen

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. This work was supported by the German Federal Ministry of Education (“CLIOMMICS” (01ZX1309 and 01ZX1609) as well as “CAMPSIMM” (01ES1103)) and the Deutsche Forschungs- gemeinschaft (SFB/TRR79). Publication costs of this manuscript are kindly covered by the German-Speaking Myeloma Multicenter Group e.V.