Purged versus non-purged peripheral blood stem-cell transplantation for high-risk neuroblastoma (COG A3973): a randomised phase 3 trial

Kreissman, Susan G.; Seeger, Robert C.; Matthay, Katherine K.; London, Wendy B.; Sposto, Richard; Grupp, Stephan A.; Haas‐Kogan, Daphne A.; LaQuaglia, Michael P.; Yu, Alice L.; Diller, Lisa; Buxton, Allen; Park, Julie R.; Cohn, Susan L.; Maris, John M.; Reynolds, C. Patrick; Villablanca, Judith G.

doi:10.1016/s1470-2045(13)70309-7

Cited by 250 publications

(295 citation statements)

References 26 publications

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“…All patients received HR-NB induction regimens. 5,6,30,31 Therapy before relapse included isotretinoin in 85 (84%) patients and anti-G D2 mAb in 51 (50%) patients. Sites of relapse were osteomedullary (BM and/or bone) (nD34), osteomedullary plus soft tissue (n D 31), or soft tissue (n D 36).…”

Section: Clinical Characteristicsmentioning

confidence: 99%

“…1 Before the routine use of immunotherapy, 3-5 year progression-free survival (PFS) rates in national studies were 20-40%, [2][3][4][5][6] even with inclusion of patients with what is now known to be intermediate-risk NB. 7 The randomized study of the Children's Oncology Group showed significantly better outcome in patients treated post-ASCT with the anti-G D2 chimeric mAb ch14.18 plus granulocyte-macrophage colony-stimulating factor (GM-CSF) plus interleukin-2.…”

Section: Introductionmentioning

confidence: 99%

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Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study

et al. 2015

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Relapse of high-risk neuroblastoma (HR-NB) is deemed invariably fatal yet increasing numbers of HR-NB patients achieve a second complete/very good partial remission (CR/VGPR), hence the urgency to find a successful consolidative therapy. Identifying efficacy in patients without assessable disease, however, is problematic. We report the first study providing outcome data for this group of patients with poor prognosis. To prevent another relapse, HR-NB patients in second or later CR/VGPR received the anti-G D2 murine antibody 3F8 plus granulocyte-macrophage colony-stimulating factor plus isotretinoin in a Phase II trial. Upon meeting the target aim for progression-free survival (PFS) in the initial cohort of 33 patients, the trial was amended to allow patients who developed human anti-mouse antibody (HAMA) to receive rituximab to ablate HAMA with or without low-dose maintenance chemotherapy until immunotherapy could resume. For the total of 101 study patients, 5-year PFS and overall survival (OS) rates were 33% § 5% and 48% § 5%, respectively. Among the 33 long-term progression-free survivors, 19 had MYCN amplification, 19 had previously received anti-G D2 immunotherapy plus isotretinoin (as first-line therapy), and 15 never received maintenance chemotherapy. In a multivariate analysis of prognostic factors, only absence of minimal residual disease in bone marrow after 2 cycles of immunotherapy and before initiation of isotretinoin or anti-HAMA therapy was significantly favorable for both PFS and OS. Therefore, long-term PFS is possible for HR-NB patients who achieve at least a second CR/VGPR and receive consolidation that includes anti-G D2 immunotherapy plus isotretinoin, even if the patients received these biological treatments before relapse. Results from this prospective study will aid in the development of future Phase II studies for this growing ultra high-risk patient population.

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Section: Clinical Characteristicsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study

et al. 2015

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“…The reason to this was considered to be either incomplete purging or residual tumour in the patient. These findings suggest that non-purged peripheral blood stem cell transplants are acceptable to support myeloablative therapy in highrisk neuroblastoma patients [30,31]. Tumour cell purging also significantly increases the price of the procedure, which further questions its necessity.…”

Section: Discussionmentioning

confidence: 99%

Specificities of Autologous Haematopoietic Stem Cell Transplantation in Children: A Single Centre Experience

Jakovljević¹

2014

J Hematol Thrombo Dis

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Background: Autologous haematopoietic stem cell transplantation (AHSCT) is now an integral part of the treatment of high-risk solid tumours in children. However, specific characteristics and problems related to paediatric patients must be taken into account. Considering these tumours are rare, indications, efficacy and practical issues of autologous transplantation have been a topic of research and discussion.

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“…62 Subsequent studies simplified the intensity of the conditioning; dropping the TBI and using two or three drugs. 63,64 As the importance of the high-dose block of therapy has evolved from a 'kill or cure' approach to a cytoreductive cassette in overall therapy, the TRM has fallen from over 10% in an earlier era to the current 2%. 63 Figure 1.…”

Section: Building On a Platform Of High-dose Melphalanmentioning

confidence: 99%

“…63,64 As the importance of the high-dose block of therapy has evolved from a 'kill or cure' approach to a cytoreductive cassette in overall therapy, the TRM has fallen from over 10% in an earlier era to the current 2%. 63 Figure 1. 100-day TRM and year of high-dose procedure for neuroblastoma (with permission, from Ladenstein et al 60 ).…”

Section: Building On a Platform Of High-dose Melphalanmentioning

confidence: 99%

Not too little, not too much—just right! (Better ways to give high dose melphalan)

Shaw

Nath

Lazarus

2014

Bone Marrow Transplant

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Of the 13 286 autologous haematopoietic cell transplant procedures reported in the US in 2010-2012 for plasma cell disorders, 10 557 used single agent, high-dose melphalan. Despite 30 years of clinical and pharmacokinetic (PK) experience with high-dose melphalan, and its continuing central role as cytoreductive therapy for large numbers of patients with myeloma, the pharmacodynamics and pharmacogenomics of melphalan are still in their infancy. The addition of protectant agents such as amifostine and palifermin allows dose escalation to 280 mg/m 2 , but at these doses it is cardiac, rather than gut, toxicity that is doselimiting. Although combination with additional alkylating agents is feasible, the additional TRM may not be justified when so many post-consolidation therapies are available for myeloma patients. Current research should optimise the delivery of this single-agent chemotherapy. This includes the use of newer formulations and real-time PKs. These strategies may allow a safe and effective platform for adding synergistic novel therapies and provide a window of lymphodepletion for the addition of immunotherapies. To best assess the contribution that the dose of drug makes to clinically meaningful endpoints in haematopoietic cell transplantation (HCT), one would choose one drug, ideally used as monotherapy, for one disease and with one source of haematopoietic progenitor cells (HPC). Although this approach may appear quite restrictive, these criteria are fulfilled when high-dose melphalan is used in the context of autologous HCT for plasma cell myeloma. Indeed, melphalan, which has been in use for 60 years, has been used in this way for 30 years. One might think we would know all there is to know about the use of this agent for this indication. However, in fact, we know very little. Several years ago, we briefly reviewed this subject, but the focus was on the various settings in which high-dose melphalan and autologous HCT were used. 1 In this present review, we will not discuss the role of high-dose melphalan in HCT but would direct readers to an excellent recent review on this topic. 2 Instead, we will use that review as our starting point for what we know about the pharmacokinetics (PK) of melphalan for high-dose therapy, in particular for myeloma, and how we may move forward. EARLY WORKHigh-dose melphalan has been in use for decades. The relatively few and reversible non-hematologic toxic effects make it suitable for high-dose therapy, whereas its profound marrow toxicity makes it unsuitable for repeated low-dose exposures. Today, most patients are naïve to melphalan exposure as it is only infrequently used as initial cancer therapy. The toxicity profile means that infusion of HPC can rescue or protect against most of the toxicity of the drug-hence, melphalan is the ideal agent for high-dose therapy with rescue by autologous HCT.Amongst the variety of solid tumours for which subjects first underwent HCT using melphalan were paediatric patients with neuroblastoma; these early reports garnered the inte...

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Purged versus non-purged peripheral blood stem-cell transplantation for high-risk neuroblastoma (COG A3973): a randomised phase 3 trial

Cited by 250 publications

References 26 publications

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study

Specificities of Autologous Haematopoietic Stem Cell Transplantation in Children: A Single Centre Experience

Not too little, not too much—just right! (Better ways to give high dose melphalan)

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Purged versus non-purged peripheral blood stem-cell transplantation for high-risk neuroblastoma (COG A3973): a randomised phase 3 trial

Cited by 250 publications

References 26 publications

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-GD2immunotherapy and isotretinoin: a prospective Phase II study

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-GD2immunotherapy and isotretinoin: a prospective Phase II study

Specificities of Autologous Haematopoietic Stem Cell Transplantation in Children: A Single Centre Experience

Not too little, not too much—just right! (Better ways to give high dose melphalan)

Contact Info

Product

Resources

About

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study

Prolonged progression-free survival after consolidating second or later remissions of neuroblastoma with Anti-G_D2immunotherapy and isotretinoin: a prospective Phase II study