Residual malignant and normal plasma cells shortly after high dose melphalan and stem cell transplantation. Highlight of a putative therapeutic window in Multiple Myeloma?

Anouk Caraux,Jean-Luc Veyrune,Bernard Klein,Salahedine Bouhya,Philippe Quittet,Jérôme Moreaux,Guillaume Cartron,Laure Vincent,Jean-François Rossi,Guilhem Requirand,Gaëlle Olivier

doi:10.18632/oncotarget.650

Abstract

Multiple Myeloma (MM) is an incurable malignant plasma cell disorder. We have evaluated the counts of Multiple Myeloma Cells (MMCs) and normal plasma cells (N-PCs), seven days after high-dose melphalan (HDM) and autologous stem transplantation (ASCT). Two third of patients had detectable minimal residual disease (MRD+) (71.7 MMCs/µL) after induction treatment with dexamethasone and proteasome inhibitor. MMC counts were reduced by 92% (P ≤ .05) but not eradicated 7 days after HDM+ASCT. Post-HDM+ASCT MMCs were viable and bathed in a burst of MMC growth factors, linked with post-HDM aplasia. In one third of patients (MRD- patients), MMCs were not detectable after induction treatment and remained undetectable after HDM+ASCT. Major difference between MRD- and MRD+ patients is that N-PC counts were increased 3 fold (P〈.05) by HDM+ASCT in MRD- patients, but were unaffected in MRD+ patients. Possible explanation could be that clearance of MMCs in MRD- patients makes more niches available for N-PCs. Thus, MMCs are not fully eradicated shortly after HDM, are bathed in high concentrations of MMC growth factors in an almost desert BM, are viable in short-term culture, which suggests providing additional therapies shortly after HDM to kill resistant MMCs before full repair of lesions.

Highlights

Multiple myeloma (MM) is characterized by the accumulation of clonal malignant plasma cells (PCs), primarily in the bone marrow (BM)
We address the question of the effects of High dose melphalan (HDM) and autologous stem cell transplantation (ASCT) on Myeloma Cells (MMCs) and normal plasma cells (N-PCs)
For 17 of the 18 Minimal residual disease (MRD)+ patients, MMCs could still be detected in the BM 7 days after HDM and ASCT, with a 92% reduction in median MMC counts (5.5 MMCs/μL versus 71.7 MMCs/μL, P ≤ .001) (Table 2)

Summary

Introduction

Multiple myeloma (MM) is characterized by the accumulation of clonal malignant plasma cells (PCs), primarily in the bone marrow (BM) It affects every year 86000 new patients throughout the world.[1] MM is still an incurable disease with a median survival in excess of 5 years.[2] For patients below 65-70 years, first line treatment includes 4-6 cycles of induction therapy based on novel agents (proteasome inhibitor or immunomodulatory drugs), high dose dexamethasone (D) and DNA targeting drugs, followed by intensification treatment with high dose melphalan (HDM) supported by autologous stem cell transplantation (ASCT). Autologous hematopoietic stem cells (HSCs) are collected after 3 to 4 cycles of induction therapy, HSC being mobilized into peripheral blood (PB) using granulocyte colonystimulating factor (G-CSF) alone or in combination with cyclophosphamide. The association of immunomodulatory drugs (Thalidomide® or Revlimid®) to proteasome inhibitor (Bortezomib, B) and high doses dexamethasone improves the rates of complete responses after induction and intensification treatment.[3] The major therapeutic questions addressed by large ongoing clinical trials www.impactjournals.com/oncotarget

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