Impact of pretransplant minimal residual disease after cord blood transplantation for childhood acute lymphoblastic leukemia in remission: an Eurocord, PDWP–EBMT analysis

Ruggeri, Annalisa; Gautier, Michel; Dalle, Jean‐Hugues; Caniglia, Maurizio; Locatelli, Franco; Campos, António; Heredia, Cristina Díaz de; Mohty, Mohamad; Hurtado, José María Pérez; Bierings, Marc; Bittencourt, Henrique; Mauad, Marcos Augusto; Purtill, Duncan; Cunha, Renato; Kabbara, Nabil; Gluckman, Éliane; Labopin, Myriam; Peters, Christina; Rocha, Vanderson

doi:10.1038/leu.2012.123

Cited by 47 publications

(44 citation statements)

References 46 publications

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“…9,22 However, in contrast to these previous reports, in the cord-blood group, the overall mortality and rate of relapse were similar among patients with minimal residual disease and those without minimal residual disease. These observations are not entirely consistent with previous reports regarding transplants from cord-blood donors, [23][24][25] in which a higher risk of relapse and a lower rate of leukemia-free survival was seen among patients with minimal residual disease than among those without minimal residual disease.…”

Section: Discussioncontrasting

confidence: 52%

Cord-Blood Transplantation in Patients with Minimal Residual Disease

2016

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Section: Discussioncontrasting

confidence: 52%

Cord-Blood Transplantation in Patients with Minimal Residual Disease

2016

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“…[3][4][5][6][7][8] Although consolidative therapy with HCT can cure some patients with persistent MRD, 7,14,15 most studies suggest that the majority of these patients will relapse post HCT. 3,[6][7][8] The idea that leukemia-free survival would be improved if pre-transplant MRD can be eliminated has scientific rationale, but the theory has not been formally tested. Whether pre-HCT MRD represents a patient who is inadequately treated, or one who has underlying high-risk biology that is predetermined to fail HCT, is currently unknown.…”

Section: Discussionmentioning

confidence: 99%

“…Recent studies show that identifying minimal residual disease (MRD) prior to HCT is the strongest predictor of treatment failure. [3][4][5][6][7][8] Whether eliminating MRD prior to HCT will influence post-HCT outcomes, particularly with regard to reducing relapse, has not yet been established. However, this approach is not without risks, as additional chemotherapy in patients who have already achieved remission could lead to toxic complications that may preclude proceeding to HCT or increase peri-transplant toxicity.…”

Section: Introductionmentioning

confidence: 99%

A clofarabine-based bridging regimen in patients with relapsed ALL and persistent minimal residual disease (MRD)

Gossai

Verneris

Karras

et al. 2013

Bone Marrow Transplant

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In patients with relapsed ALL, minimal residual disease (MRD) identified prior to allogeneic hematopoietic cell transplantation (HCT) is a strong predictor of relapse. We report our experience using a combination of reduced-dosing clofarabine, CY and etoposide as a 'bridge' to HCT in eight patients with high risk or relapsed ALL and pre-HCT MRD. All patients had detectable MRD (40.01%, flow cytometry) at the start of therapy with all eight achieving MRD reduction following one cycle. The regimen was well tolerated with seven grade 3/4 toxicities occurring among four of the eight patients. Five patients (62.5%) are alive, one died from relapse (12.5%) and two from transplant-related mortality (25%). The combination of reduced-dose clofarabine, CY and etoposide as bridging therapy appears to be well tolerated in patients with relapsed ALL and is effective in reducing pre-HCT MRD. (2014) 49, 440-442; doi:10.1038/bmt.2013.195; published online 9 December 2013 Bone Marrow TransplantationKeywords: ALL; MRD; pediatric; transplantation; clofarabine; leukemia INTRODUCTION Improvements in the treatment of children with ALL have resulted in 5-year OS approaching 90%. 1 However, those with relapsed disease continue to respond poorly to traditional salvage approaches, with survival rates hovering around 35-40%. 2 Although allogeneic hematopoietic cell transplantation (HCT) in children with relapsed ALL has the ability to overcome resistant disease and cure some patients, relapse remains a significant barrier to success. Recent studies show that identifying minimal residual disease (MRD) prior to HCT is the strongest predictor of treatment failure. [3][4][5][6][7][8] Whether eliminating MRD prior to HCT will influence post-HCT outcomes, particularly with regard to reducing relapse, has not yet been established. However, this approach is not without risks, as additional chemotherapy in patients who have already achieved remission could lead to toxic complications that may preclude proceeding to HCT or increase peri-transplant toxicity. Also, in prolonging the time to HCT for further chemotherapy, patients may lose their state of remission and increase their disease burden, rather than decrease it. Despite these uncertainties, there is a strong sense among the pediatric oncology and transplant communities that attempts to eliminate MRD prior to HCT are warranted. 9 Clofarabine, a novel purine nucleoside analog granted accelerated FDA approval in 2004 for pediatric relapsed/refractory ALL, has reported promising results as a single agent or part of a multidrug regimen with cyclophosphamide (CY) and etoposide. [10][11][12] Although clofarabine combinations have shown encouraging rates of CR in heavily pre-treated relapsed/refractory patients, 11,12 significant toxicities exist that appear to be dose dependent. 13 In an attempt to reduce and/or eliminate pre-HCT MRD without inducing significant toxicities, we treated eight consecutive patients with reduced dosing of clofarabine, CY and etoposide. The goal of this therapy was to 'b...

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“…Nevertheless, these studies uniformly found excellent long-term outcomes for patients without detectable MRD (that is, 'MRD À ' patients) undergoing myeloablative AlloHCT, with 2-5 year estimates of EFS, relapse-free survival and OS often in the 70-80% range, and more recent series suggesting even better outcomes. [29][30][31][34][35][36][37][39][40][41][42][43][46][47][48][49] Almost without exception, the outcomes for patients with detectable MRD (that is, 'MRD þ ' patients) were significantly inferior, with long-term estimates of EFS of 0-30% and OS of 30-50%, respectively. Although data are more limited for AutoHCT, available information suggests that MRD À patients may have relatively good disease control that appears to approach that seen after AlloHCT, at least in the subset of leukemias that do not harbor the Philadelphia chromosome; on the other hand, MRD þ ALL patients experience exceedingly high rates of relapse after AutoHCT.…”

Section: The Concept and Determination Of Mrdmentioning

confidence: 99%

“…53,57,61,62 However, MRD appears to bear significance as an independent prognostic marker, as suggested by multivariate regression modeling in many of the studies. [27][28][29]36,37,39,[42][43][44][47][48][49]53,54,57,[59][60][61] The association between MRD and risk of BM relapse is likely 'dose-dependent' in ALL 27,28,36,37,41,42,44,47,63 and, possibly, AML, 53,54,60 while MRD assessments may fail to predict extramedullary relapse accurately. 32,45 Interestingly, evidence from logistic regression models suggests that the relative level of MRD has more impact on survival in ALL than in AML.…”

Section: The Concept and Determination Of Mrdmentioning

confidence: 99%