Salvage Second Hematopoietic Cell Transplantation in Myeloma

Michaelis, Laura C.; Saad, Ayman; Zhong, Xiaobo; Le‐Rademacher, Jennifer; Freytes, César O.; Marks, David I.; Lazarus, Hillard M.; Bird, Jennifer M.; Holmberg, Leona; Kamble, Rammurti T.; Kumar, Shaji; Lill, Michael; Meehan, Kenneth R.; Saber, Wael; Schriber, Jeffrey; Tay, Jason; Vogl, Dan T.; Wirk, Baldeep; Savani, Bipin N.; Gale, Robert Peter; Vesole, David H.; Schiller, Gary J.; Abidi, Muneer H.; Anderson, Kenneth C.; Nishihori, Taiga; Kalaycio, Matt; Vose, Julie M.; Moreb, Jan S.; Drobyski, William R.; Munker, Reinhold; Roy, Vivek; Ghobadi, Armin; Holland, H. Kent; Nath, Rajneesh; To, LB; Maiolino, Ângelo; Kassim, Adetola A.; Giralt, Sergío; Landau, Heather; Schouten, Harry C.; Maziarz, Richard T.; Joseph, Michael; Kindwall‐Keller, Tamila L.; Stiff, Patrick J.; Gibson, John; Lonial, Sagar; Krishnan, Amrita; Dispenzieri, Angela; Hari, Parameswaran

doi:10.1016/j.bbmt.2013.01.004

Cited by 99 publications

(80 citation statements)

References 31 publications

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“…[101][102][103] The primary endpoint is safety and tolerability, and an important secondary endpoint is an intrapatient comparison of time to progression (TTP) after salvage auto-HCT+CART19 cells to TTP after first auto-HCT. As TTP after salvage auto-HCT is typically significantly shorter than after first auto-HCT, 104,105 any improvement in this expected TTP would provide a preliminary signal of efficacy that would support additional studies in larger numbers of patients.…”

Section: Car T Cellsmentioning

confidence: 90%

Beyond consolidation: auto-SCT and immunotherapy for plasma cell myeloma

Lendvai

Cohen

Cho

2015

Bone Marrow Transplant

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Autologous hematopoietic cell transplantation (auto-HCT) is the standard consolidation therapy for plasma cell myeloma patients following induction therapy. Auto-HCT improves disease-free survival (DFS), but is generally not curative. The allogeneic HCT experience demonstrated that T-cell immunotherapy can confer long-term DFS. Preclinical and clinical data indicate that myelomaassociated Ags elicit humoral and cellular immune responses (IRs) in myeloma patients. These findings strongly suggest that the immunotherapeutic strategies, including immune checkpoint inhibitors, therapeutic cancer vaccines and adoptive cellular therapies, are promising avenues of clinical research that may be most applicable in the minimal residual disease state following auto-HCT. These strategies are designed to prime or augment antimyeloma IRs and promote a 'host-vs-myeloma' effect that may result in durable DFS. Innovative clinical trials investigating immune checkpoint inhibitors and cancer vaccines have demonstrated that robust immunity against myeloma-associated Ags can be elicited in the setting of auto-HCT. A diverse array of immunotherapeutic strategies have entered clinical trials in myeloma, including PD-1/PD-L1 inhibitors, DC/myeloma cell fusion vaccines and adoptive chimeric Ag receptor T-cell therapy, and further investigation of combinations of immunologic and pharmaceutical agents are expected in the near future. In this review, we will discuss the preclinical data supporting immunotherapy in auto-HCT for myeloma, clinical investigation of these strategies and the future prospects of immunotherapy in pursuit of the goal of curative therapy.

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Section: Car T Cellsmentioning

confidence: 90%

Beyond consolidation: auto-SCT and immunotherapy for plasma cell myeloma

Lendvai

Cohen

Cho

2015

Bone Marrow Transplant

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“…This study provides evidence for the efficacy of salvage HDT-SCT compared with salvage cyclophosphamide (not a common treatment choice), essentially comparing 2 alkylator regimens in RRMM patients. Another large retrospective registry study 71 reported risk of progression of 51%, 82%, and 91% at 1, 3, and 5 years, respectively. These analyses were done at the time when the currently FDA-approved newer agents (CFZ, POM) were unavailable and the role of maintenance therapies with LEN and BTZ was not yet established.…”

mentioning

confidence: 98%

“…HDT-SCT2 may be a reasonable option to consider for young transplant-eligible patients with good performance status (PS) who derived a long PFS after HDT-SCT1. Among patients not receiving maintenance therapies after HDT-SCT, if the relapse is beyond the expected PFS (18-23 months), [71][72][73] HDT-SCT2 is an option to consider. For patients who have relapsed while receiving maintenance therapy, and the duration of remission is beyond the expected PFS (39-41 months for LEN maintenance 72,73 and 35 months for BTZ maintenance), 74 HDT-SCT2 may also be offered.…”

mentioning

confidence: 99%

Treatment options for relapsed and refractory multiple myeloma

Nooka

Kastritis

Lonial

2015

Blood

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142

130

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Over the last few decades, significant improvement in outcomes has been observed for myeloma patients, mainly as a result of the use of currently available approved antimyeloma agents, along with combining autologous stem cell transplantation in the treatment of myeloma.With more targeted agents in development, the treatment of a myeloma patient at relapse has become complicated and, as a consequence, results in vast heterogeneity in treatment patterns. Although a consensus on the timing of initiation of treatment, the choice of agents to be used, and the role of transplant is less clear, we describe an evidence-based approach and the factors to consider upon relapse. We describe additional newer agents and targets that are under development, with the goal of achievement of durable remissions for myeloma patients. (Blood. 2015;125(20):3085-3099)

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“…Although median event free survival was longer for patients treated with early ASCT (39 mo vs 13 mo) the median OS was not significantly different between the two groups (64.6 mo vs 64 mo, P = 0.92), and 90% of the patients randomised to the VMPC arm were able to receive the planned delayed ASCT at the time of relapse [25] . Several analyses, summarised in Table 3, have investigated the role of ASCT as a salvage therapy for MM [29,[44][45][46][47][48][49][50][51] . These works are not always comparable, due to the different nature of the works (both prospective and retrospective) and to the fact that ASCT was …”

Section: Delayed Transplantationmentioning

confidence: 99%

“…Cook et al [49] 2011 106 Retrospective 19 mo (relapse from first transplant) Yes 63% NR 37 Jimenez-Zepeda et al [51] [45] 2013 187 Retrospective 32 mo Yes 68% 5% at 5 yr 29% at 5 yr Shah et al [68] Brioli A. ASCT in MM in some cases given as a salvage treatment after a previous ASCT [44][45][46] , whilst in others patients received ASCT after relapsing from a treatment not including transplantation [29,47,48] . One of the biggest records is the one published by Sellner et al [44] , in which 200 MM patients retreated with ASCT at the time of relapse were retrospectively analysed.…”

Section: Orr (%) Pfs (Mo) Os (Mo)mentioning

confidence: 99%

First linevsdelayed transplantation in myeloma: Certainties and controversies

Brioli¹

2016

WJT

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Salvage Second Hematopoietic Cell Transplantation in Myeloma

Cited by 99 publications

References 31 publications

Beyond consolidation: auto-SCT and immunotherapy for plasma cell myeloma

Beyond consolidation: auto-SCT and immunotherapy for plasma cell myeloma

Treatment options for relapsed and refractory multiple myeloma

First linevsdelayed transplantation in myeloma: Certainties and controversies

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