Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum

Steven G. Dubois; Lucas Moreno; John Anderson; Shahab Asgharzadeh; Ro Bagatell; Maja Beck-Popovic; Jen Belle; Pablo Berlanga; Nick J. Bird; Louis Chesler; Adam Durbin; Angelika Eggert; Martin Eilers; Sara M. Federico; Matthias Fischer; Susanne A. Gatz; Rani E. George; Sally George; Kelly C. Goldsmith; Juliet Gray; Andras Heczey; Meredith S. Irwin; Leona Knox; Holger N. Lode; Donna Ludwinski; Margaret E. Macy; Robbie G. Majzner; John M. Maris; Shakeel Modak; Jan J. Molenaar; Daniel A. Morgenstern; Yael P. Mosse; Cormac Owens; C. Patrick Reynolds; Claudia Rossig; Gudrun Schleiermacher; Liz Scott; Paul M. Sondel; Frank Speleman; Max van Noesel; Frank Westermann; Judith Wienke; Adam J. Wolpaw; Julie R. Park; Andrew D. J. Pearson

doi:10.1002/pbc.31831

Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum

Steven G. Dubois^*, Lucas Moreno, John Anderson, Shahab Asgharzadeh, Ro Bagatell, Maja Beck-Popovic, Jen Belle, Pablo Berlanga, Nick J. Bird, Louis Chesler, Adam Durbin, Angelika Eggert, Martin Eilers, Sara M. Federico, Matthias Fischer, Susanne A. Gatz, Rani E. George, Sally George, Kelly C. Goldsmith, Juliet GrayAndras Heczey, Meredith S. Irwin, Leona Knox, Holger N. Lode, Donna Ludwinski, Margaret E. Macy, Robbie G. Majzner, John M. Maris, Shakeel Modak, Jan J. Molenaar, Daniel A. Morgenstern, Yael P. Mosse, Cormac Owens, C. Patrick Reynolds, Claudia Rossig, Gudrun Schleiermacher, Liz Scott, Paul M. Sondel, Frank Speleman, Max van Noesel, Frank Westermann, Judith Wienke, Adam J. Wolpaw, Julie R. Park, Andrew D. J. Pearson

^*Corresponding author for this work

Pharmaceutics

Research output: Contribution to journal › Review article › peer-review

Abstract

High-risk neuroblastoma is a poor prognosis cancer of the sympathetic nervous system that accounts for a disproportionate number of childhood cancer deaths. Many viable biological targets have been identified, and the number of potential combinations is even larger. Several products have attained marketing authorization for treatment of patients with neuroblastoma. Patient outcomes remain poor, with approximately 50% of children with newly diagnosed high-risk neuroblastoma cured of their disease. International, multistakeholder Neuroblastoma Drug Development Strategy (NDDS) meetings were established more than a decade ago. This third NDDS meeting included academia, industry, regulatory, and patient advocacy representatives to prioritize agents and to address key challenges in drug development in this disease. Given the central role that anti-GD2 therapy plays, novel GD2-directed combinations were a key focus, including epigenetic enzymes such as EZH2 and immunologic targets such as IL15 and TIGIT as potential combination partners. GD2-directed chimeric antigen receptor (CAR)-T cells were a top priority, along with emerging CAR-T targets such as B7-H3 and GPC2. Recognizing that combination therapies are likely to be most impactful for patients and for advancing therapies to frontline, another key focus was on high priority combinations of targeted therapies, including Aurora A kinase plus BCL2 or ATR inhibitors. Additional targets and agents were prioritized or deprioritized based upon current data. Access to drugs for clinical trials was viewed as a major barrier to progress. Strategies to overcome this challenge focused on united efforts by the international scientific and advocacy community and early engagement by industry with regulatory authorities.

Original language	English
Number of pages	13
Journal	Pediatric Blood & Cancer
DOIs	https://doi.org/10.1002/pbc.31831
Publication status	E-pub ahead of print - 12 Jun 2025

Bibliographical note

Publisher Copyright:
© 2025 The Author(s). Pediatric Blood & Cancer published by Wiley Periodicals LLC.

Funding

S.G.D. reports consulting fees from Amgen, Bayer, EMD Serono, InhibRx, and Jazz as well as travel expenses from Loxo, Roche, and Salarius. L.M. reports membership of Data Monitoring Committees (DMC) for clinical trials sponsored by the University of Southampton, Karolinska University Hospital and the Royal Marsden NHS Foundation Trust; consulting role for Novartis, Bayer, BMS, Merck, Norgine, and Gilead, travel expenses from Recordati Rare Diseases, participation in educational activities organized by Recordati, Beigene, Y\u2010mAbs, and Bayer and is the President of the SIOPEN (European neuroblastoma research cooperative group), organization which receives royalties for the sales of dinutuximab beta. His institution receives funding for educational activities, advisory role, or conducting industry\u2010sponsored clinical trials. P.B. reports institutional funding and travel expenses from Recordati Rare Diseases and institutional funding, drugs for trials, and travel expenses from Bayer. A.D. is a shareholder of Syros Pharmaceuticals and Foghorn Therapeutics and has received academic grants from the Recordati Rare Diseases Foundation. M.E. is a founder and shareholder of Tucana Biosciences. S.A.G. has/has had an advisory role for EMD Serono/MERCK KGaA, Amgen, and Gilead, has signed a consultancy agreement with AstraZeneca and Schroedinger Therapeutics, and received research funding from AstraZeneca (own grant and fee to institution), G.S.K. (fee to institution), and Bayer (grant to institution and SLA). K.G. reports nonreimbursed consulting for Ymabs Therapeutics and Abbvie. A.H. is a consultant for Waypoint Bio and serves on the Scientific Advisory Board of CARGO Therapeutics; has equity in CARGO; received research support from Kuur/Athenex Therapeutics. M.E.M. reports consulting fees from Recordati Rare Diseases, Ymabs Therapeutics, Abbvie, and Kestrel Therapeutics, as well as travel expenses from Bayer. R.G.M. is a co\u2010founder of, consultant for, and holds equity in Link Cell Therapies and CARGO Therapeutics, has served as a consultant for and holds equity in Lyell Immunopharma, Innervate Radiopharmaceuticals, and Waypoint Bio, and has consulted for NKarta, Arovella Pharmaceuticals, GammaDelta Therapeutics, Aptorum Group, Zai Labs, Immunai, Gadeta, and FATE Therapeutics. J.M.M. is a founder and shareholder in Hula Therapeutics and Bela Therapeutics. D.A.M. reports consulting fees from Y\u2010mAbs Therapeutics, Abbvie, Clarity Pharmaceuticals, and US World Meds; travel expenses from Abbvie and Lilly and speaker fees from Takeda Israel Ltd and YmAbs Therapeutics. Y.P.M. is a founder and shareholder in Bela Therapeutics. A.D.J.P. has consulted for Lilly, Norgine, and Developmental Therapeutics Consortium Limited and been an advisor for Amgen. : This work was supported by Accelerate the Future Fund; Alex's Lemonade Stand Foundation; Dana\u2010Farber Cancer Institute; and Friends for Life. Funding

Funders	Funder number
Recordati Rare Diseases Foundation
AstraZeneca
Gilead
Alex's Lemonade Stand Foundation for Childhood Cancer
Dana-Farber Cancer Institute
Bayer

Keywords

Alk
Atr
B7-h3
Clinical trials
Drug development
Ezh2
Gd2
Gpc2
Mycn
Neuroblastoma
Relapse

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1002/pbc.31831Licence: CC BY-NC-ND

Cite this

Dubois, S. G., Moreno, L., Anderson, J., Asgharzadeh, S., Bagatell, R., Beck-Popovic, M., Belle, J., Berlanga, P., Bird, N. J., Chesler, L., Durbin, A., Eggert, A., Eilers, M., Federico, S. M., Fischer, M., Gatz, S. A., George, R. E., George, S., Goldsmith, K. C., ... Pearson, A. D. J. (2025). Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum. Pediatric Blood & Cancer. Advance online publication. https://doi.org/10.1002/pbc.31831

@article{fc0e93dead414359bbb7e0c32c667b7a,

title = "Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum",

abstract = "High-risk neuroblastoma is a poor prognosis cancer of the sympathetic nervous system that accounts for a disproportionate number of childhood cancer deaths. Many viable biological targets have been identified, and the number of potential combinations is even larger. Several products have attained marketing authorization for treatment of patients with neuroblastoma. Patient outcomes remain poor, with approximately 50% of children with newly diagnosed high-risk neuroblastoma cured of their disease. International, multistakeholder Neuroblastoma Drug Development Strategy (NDDS) meetings were established more than a decade ago. This third NDDS meeting included academia, industry, regulatory, and patient advocacy representatives to prioritize agents and to address key challenges in drug development in this disease. Given the central role that anti-GD2 therapy plays, novel GD2-directed combinations were a key focus, including epigenetic enzymes such as EZH2 and immunologic targets such as IL15 and TIGIT as potential combination partners. GD2-directed chimeric antigen receptor (CAR)-T cells were a top priority, along with emerging CAR-T targets such as B7-H3 and GPC2. Recognizing that combination therapies are likely to be most impactful for patients and for advancing therapies to frontline, another key focus was on high priority combinations of targeted therapies, including Aurora A kinase plus BCL2 or ATR inhibitors. Additional targets and agents were prioritized or deprioritized based upon current data. Access to drugs for clinical trials was viewed as a major barrier to progress. Strategies to overcome this challenge focused on united efforts by the international scientific and advocacy community and early engagement by industry with regulatory authorities.",

keywords = "Alk, Atr, B7-h3, Clinical trials, Drug development, Ezh2, Gd2, Gpc2, Mycn, Neuroblastoma, Relapse",

author = "Dubois, {Steven G.} and Lucas Moreno and John Anderson and Shahab Asgharzadeh and Ro Bagatell and Maja Beck-Popovic and Jen Belle and Pablo Berlanga and Bird, {Nick J.} and Louis Chesler and Adam Durbin and Angelika Eggert and Martin Eilers and Federico, {Sara M.} and Matthias Fischer and Gatz, {Susanne A.} and George, {Rani E.} and Sally George and Goldsmith, {Kelly C.} and Juliet Gray and Andras Heczey and Irwin, {Meredith S.} and Leona Knox and Lode, {Holger N.} and Donna Ludwinski and Macy, {Margaret E.} and Majzner, {Robbie G.} and Maris, {John M.} and Shakeel Modak and Molenaar, {Jan J.} and Morgenstern, {Daniel A.} and Mosse, {Yael P.} and Cormac Owens and Reynolds, {C. Patrick} and Claudia Rossig and Gudrun Schleiermacher and Liz Scott and Sondel, {Paul M.} and Frank Speleman and {van Noesel}, Max and Frank Westermann and Judith Wienke and Wolpaw, {Adam J.} and Park, {Julie R.} and Pearson, {Andrew D. J.}",

note = "Publisher Copyright: {\textcopyright} 2025 The Author(s). Pediatric Blood & Cancer published by Wiley Periodicals LLC.",

year = "2025",

month = jun,

day = "12",

doi = "10.1002/pbc.31831",

language = "English",

journal = "Pediatric Blood & Cancer",

issn = "1545-5009",

publisher = "Wiley-Liss Inc.",

}

Dubois, SG, Moreno, L, Anderson, J, Asgharzadeh, S, Bagatell, R, Beck-Popovic, M, Belle, J, Berlanga, P, Bird, NJ, Chesler, L, Durbin, A, Eggert, A, Eilers, M, Federico, SM, Fischer, M, Gatz, SA, George, RE, George, S, Goldsmith, KC, Gray, J, Heczey, A, Irwin, MS, Knox, L, Lode, HN, Ludwinski, D, Macy, ME, Majzner, RG, Maris, JM, Modak, S, Molenaar, JJ, Morgenstern, DA, Mosse, YP, Owens, C, Reynolds, CP, Rossig, C, Schleiermacher, G, Scott, L, Sondel, PM, Speleman, F, van Noesel, M, Westermann, F, Wienke, J, Wolpaw, AJ, Park, JR & Pearson, ADJ 2025, 'Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum', Pediatric Blood & Cancer. https://doi.org/10.1002/pbc.31831

TY - JOUR

T1 - Accelerating Drug Development for Neuroblastoma

T2 - Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum

AU - Dubois, Steven G.

AU - Moreno, Lucas

AU - Anderson, John

AU - Asgharzadeh, Shahab

AU - Bagatell, Ro

AU - Beck-Popovic, Maja

AU - Belle, Jen

AU - Berlanga, Pablo

AU - Bird, Nick J.

AU - Chesler, Louis

AU - Durbin, Adam

AU - Eggert, Angelika

AU - Eilers, Martin

AU - Federico, Sara M.

AU - Fischer, Matthias

AU - Gatz, Susanne A.

AU - George, Rani E.

AU - George, Sally

AU - Goldsmith, Kelly C.

AU - Gray, Juliet

AU - Heczey, Andras

AU - Irwin, Meredith S.

AU - Knox, Leona

AU - Lode, Holger N.

AU - Ludwinski, Donna

AU - Macy, Margaret E.

AU - Majzner, Robbie G.

AU - Maris, John M.

AU - Modak, Shakeel

AU - Molenaar, Jan J.

AU - Morgenstern, Daniel A.

AU - Mosse, Yael P.

AU - Owens, Cormac

AU - Reynolds, C. Patrick

AU - Rossig, Claudia

AU - Schleiermacher, Gudrun

AU - Scott, Liz

AU - Sondel, Paul M.

AU - Speleman, Frank

AU - van Noesel, Max

AU - Westermann, Frank

AU - Wienke, Judith

AU - Wolpaw, Adam J.

AU - Park, Julie R.

AU - Pearson, Andrew D. J.

PY - 2025/6/12

Y1 - 2025/6/12

N2 - High-risk neuroblastoma is a poor prognosis cancer of the sympathetic nervous system that accounts for a disproportionate number of childhood cancer deaths. Many viable biological targets have been identified, and the number of potential combinations is even larger. Several products have attained marketing authorization for treatment of patients with neuroblastoma. Patient outcomes remain poor, with approximately 50% of children with newly diagnosed high-risk neuroblastoma cured of their disease. International, multistakeholder Neuroblastoma Drug Development Strategy (NDDS) meetings were established more than a decade ago. This third NDDS meeting included academia, industry, regulatory, and patient advocacy representatives to prioritize agents and to address key challenges in drug development in this disease. Given the central role that anti-GD2 therapy plays, novel GD2-directed combinations were a key focus, including epigenetic enzymes such as EZH2 and immunologic targets such as IL15 and TIGIT as potential combination partners. GD2-directed chimeric antigen receptor (CAR)-T cells were a top priority, along with emerging CAR-T targets such as B7-H3 and GPC2. Recognizing that combination therapies are likely to be most impactful for patients and for advancing therapies to frontline, another key focus was on high priority combinations of targeted therapies, including Aurora A kinase plus BCL2 or ATR inhibitors. Additional targets and agents were prioritized or deprioritized based upon current data. Access to drugs for clinical trials was viewed as a major barrier to progress. Strategies to overcome this challenge focused on united efforts by the international scientific and advocacy community and early engagement by industry with regulatory authorities.

AB - High-risk neuroblastoma is a poor prognosis cancer of the sympathetic nervous system that accounts for a disproportionate number of childhood cancer deaths. Many viable biological targets have been identified, and the number of potential combinations is even larger. Several products have attained marketing authorization for treatment of patients with neuroblastoma. Patient outcomes remain poor, with approximately 50% of children with newly diagnosed high-risk neuroblastoma cured of their disease. International, multistakeholder Neuroblastoma Drug Development Strategy (NDDS) meetings were established more than a decade ago. This third NDDS meeting included academia, industry, regulatory, and patient advocacy representatives to prioritize agents and to address key challenges in drug development in this disease. Given the central role that anti-GD2 therapy plays, novel GD2-directed combinations were a key focus, including epigenetic enzymes such as EZH2 and immunologic targets such as IL15 and TIGIT as potential combination partners. GD2-directed chimeric antigen receptor (CAR)-T cells were a top priority, along with emerging CAR-T targets such as B7-H3 and GPC2. Recognizing that combination therapies are likely to be most impactful for patients and for advancing therapies to frontline, another key focus was on high priority combinations of targeted therapies, including Aurora A kinase plus BCL2 or ATR inhibitors. Additional targets and agents were prioritized or deprioritized based upon current data. Access to drugs for clinical trials was viewed as a major barrier to progress. Strategies to overcome this challenge focused on united efforts by the international scientific and advocacy community and early engagement by industry with regulatory authorities.

KW - Alk

KW - Atr

KW - B7-h3

KW - Clinical trials

KW - Drug development

KW - Ezh2

KW - Gd2

KW - Gpc2

KW - Mycn

KW - Neuroblastoma

KW - Relapse

UR - http://www.scopus.com/inward/record.url?scp=105007905703&partnerID=8YFLogxK

U2 - 10.1002/pbc.31831

DO - 10.1002/pbc.31831

M3 - Review article

C2 - 40509548

SN - 1545-5009

JO - Pediatric Blood & Cancer

JF - Pediatric Blood & Cancer

ER -

Accelerating Drug Development for Neuroblastoma: Consensus Statement From the Third Neuroblastoma Drug Development Strategy Forum

Abstract

Bibliographical note

Funding

Keywords

UN SDGs

Access to Document

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Cite this