The road to cure in multiple myeloma: incorporation of novel agents into autologous stem cell transplantation


https://doi.org/10.4081/hmr.v3i3.558
Vol. 3 No. 3: 7th Meeting New Insights in Hematology Venice, Italy, 26-29 April 2009
Published: June 12, 2009
Abstract Views: 174
PDF: 112
Publisher's note
All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article or claim that may be made by its manufacturer is not guaranteed or endorsed by the publisher.

Authors

Because of its potential of significantly increasing the rate of complete response (CR) up to the 30% range and prolonging the duration of event-free survival (EFS) and overall survival (OS) by approximately one year when compared with conventional chemotherapy, since the mid 1990s autologous stem-cell transplantation (ASCT) has been considered the standard of care for younger patients with newly diagnosed multiple myeloma (MM). More recently, introduction into the clinical practice of novel agents targeting the myeloma clone in its bone marrow microenvironment has changed the treatment paradigm for patients who are candidates for ASCT. In particular, recognition that thalidomide and bortezomib exibit remarkable activity in advanced refractory MM has stimulated their testing in different clinical scenarios, such as induction therapy in preparation for ASCT. Studies of thalidomide- dexamethasone (TD), eventually combined with a third drug such as doxorubicin (TAD) or cyclophosphamide (CTD), provided demonstration of increased rates of at least very good partial response (VGPR) with thalidomide- based regimens in comparison with traditional therapy given before ASCT. Since most of these studies were intended to explore pre-transplantation induction therapy, EFS and OS comparisons were frequently hampered. A large trial addressed this issue by randomizing patients to receive or not thalidomide upfront incorporated into melphalan- based double ASCT. In comparison with the no thalidomide arm of the study, addition of thalidomide to double ASCT significantly increased the CR rate, up to 62%, and prolonged EFS, whose 5-year estimate was 56%. After a median follow-up of 8 years, a survival advantage has recently become apparent among the one third of patients with metaphase cytogenetic abnormalities, a finding initially not reported. Similarly to thalidomide, also bortezomib has been incorporated into newer induction regimens in an attempt to increase the CR rate before ASCT and to ultimately improve post-autotransplantation outcome. Two large phase III studies conducted in France and Italy have explored the role of bortezomib- dexamethasone (VD) and VD combined with thalidomide (VTD) in comparison with VAD and TD, respectively, as induction therapy for younger patients who are candidates to receive ASCT. In both of them, VD and VTD were superior to the control group in terms of CR and ³VGPR, a finding confirmed also in high-risk patients carrying chromosome abnormalities. Importantly, high-quality responses effected by bortezomib-based regimens were furtherly increased following the first ASCT and resulted in significantly longer progression-free survival. Although data so far available suggest that novel agents and ASCT are complementary, a key issue is whether treatment with novel agents delays or eliminates the need for autotransplantation. Randomized clinical trials comparing these two approaches will definitely answer this unresolved question within the next few years.

Supporting Agencies


Cavo, M., Zamagni, E., Tacchetti, P., Brioli, A., Pallotti, C., Pantani, L., Ceccolini, M., Petrucci, A., Testoni, N., Terragna, C., Marzocchi, G., Durante, S., Tosi, P., & Baccarani, M. (2009). The road to cure in multiple myeloma: incorporation of novel agents into autologous stem cell transplantation. Hematology Meeting Reports (formerly Haematologica Reports), 3(3). https://doi.org/10.4081/hmr.v3i3.558
Authors who publish with this journal agree to the following terms: Authors retain copyright and grant the journal right of first publication with the work simultaneously licensed under a Creative Commons Attribution License that allows others to share the work with an acknowledgement of the work's authorship and initial publication in this journal. Authors are able to enter into separate, additional contractual arrangements for the non-exclusive distribution of the journal's published version of the work (e.g., post it to an institutional repository or publish it in a book), with an acknowledgement of its initial publication in this journal. Authors are permitted and encouraged to post their work online (e.g., in institutional repositories or on their website) prior to and during the submission process, as it can lead to productive exchanges, as well as earlier and greater citation of published work (See The Effect of Open Access).

Downloads

Citations

Crossref
Scopus
Google Scholar
Europe PMC