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Immunotherapeutic Strategies for Neuroblastoma: Present, Past and Future

Journal

VACCINES
Volume 9, Issue 1, Pages -

Publisher

MDPI
DOI: 10.3390/vaccines9010043

Keywords

neuroblastoma; immunotherapy; antibodies; CAR; NK; γ δ T cells

Funding

  1. Italian Ministry of Health, Progetti di Ricerca Corrente 2020

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Neuroblastoma is a common pediatric solid tumor with varying clinical courses, and high-risk patients face poor long-term outcomes and morbidities. Adoptive cell therapy, particularly NK cells and CAR T cells, shows promise in improving the lifespan of these high-risk patients. Future prospects include gamma delta T lymphocytes and CAR NK cells.
Neuroblastoma is the most common extracranial pediatric solid tumor with a heterogeneous clinical course, ranging from spontaneous regression to metastatic disease and death, irrespective of intensive chemotherapeutic regimen. On the basis of several parameters, children affected by neuroblastoma are stratified into low, intermediate and high risk. At present, more than 50% of high-risk patients with metastatic spread display an overall poor long-term outcome also complicated by devastating long-term morbidities. Thus, novel and more effective therapies are desperately needed to improve lifespan of high-risk patients. In this regard, adoptive cell therapy holds great promise and several clinical trials are ongoing, demonstrating safety and tolerability, with no toxicities. Starting from the immunological and clinical features of neuroblastoma, we here discuss the immunotherapeutic approaches currently adopted for high-risk patients and different innovative therapeutic strategies currently under investigation. The latter are based on the infusion of natural killer (NK) cells, as support of consolidation therapy in addition to standard treatments, or chimeric antigen receptor (CAR) T cells directed against neuroblastoma associated antigens (e.g., disialoganglioside GD2). Finally, future perspectives of adoptive cell therapies represented by gamma delta T lymphocyes and CAR NK cells are envisaged.

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