Upfront consolidation treatment with 131 I-mIbG followed by myeloablative chemotherapy and hematopoietic stem cell transplantation in high-risk neuroblastoma

I-metaiodobenzylguanidine ( I-mIBG) has a significant targeted antitumor effect for neuroblastoma. However, currently there is a paucity of data for the use of I-mIBG as a "front-line" therapeutic agent in those patients with newly diagnosed high-risk neuroblastoma as part of the condition...

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Published in:Pediatric investigation 2020-09, Vol.4 (3), p.168-177
Main Authors: Feng, Jianhua, Cheng, Frankie Wt, Leung, Alex Wk, Lee, Vincent, Yeung, Eva Wm, Ching Lam, Hoi, Cheung, Jeanny, Lam, Grace Ks, Chow, Terry Tw, Yan, Carol Ls, Kong Li, Chi
Format: Article
Language:English
Subjects:
Antibodies
Blood platelets
Chemotherapy
Granulocytes
Induction therapy
Neuroblastoma
Neutrophils
Patients
Potassium
Radiation therapy
Stem cell transplantation
Stem cells
Toxicity
Transplants & implants
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Summary:I-metaiodobenzylguanidine ( I-mIBG) has a significant targeted antitumor effect for neuroblastoma. However, currently there is a paucity of data for the use of I-mIBG as a "front-line" therapeutic agent in those patients with newly diagnosed high-risk neuroblastoma as part of the conditioning regimen for myeloablative chemotherapy (MAC). To evaluate the feasibility of upfront consolidation treatment with I-mIBG plus MAC and hematopoietic stem cell transplantation (HSCT) in high-risk neuroblastoma patients. A retrospective, single-center study was conducted from 2003-2019 on newly diagnosed high-risk neuroblastoma patients without progressive disease (PD) after the completion of induction therapy. They received I-mIBG infusion and MAC followed by HSCT. A total of 24 high-risk neuroblastoma patients were enrolled with a median age of 3.0 years at diagnosis. After receiving this sequential consolidation treatment, 3 of 13 patients who were in partial response (PR) before I-mIBG treatment achieved either complete response (CR) ( 1) or very good partial response (VGPR) ( 2) after HSCT. With a median follow-up duration of 13.0 months after I-mIBG therapy, the 5-year event-free survival and overall survival rates estimated were 29% and 38% for the entire cohort, and 53% and 67% for the patients who were in CR/VGPR at the time of I-mIBG treatment. Upfront consolidation treatment with I-mIBG plus MAC and HSCT is feasible and tolerable in high-risk neuroblastoma patients, however the survival benefit of this I-mIBG regimen is only observed in the patients who were in CR/VGPR at the time of I-mIBG treatment.
ISSN:2574-2272
2096-3726
2574-2272
DOI:10.1002/ped4.12216