Implementation of mechanism of action biology-driven early drug development for children with cancer

Andrew D J Pearson; Ralf Herold; Raphaël Rousseau; Chris Copland; Brigid Bradley-Garelik; Debbie Binner; Renaud Capdeville; Hubert Caron; Jacqueline Carleer; Louis Chesler; Birgit Geoerger; Pamela Kearns; Lynley V Marshall; Stefan M Pfister; Gudrun Schleiermacher; Jeffrey Skolnik; Cesare Spadoni; Jaroslav Sterba; Hendrick van den Berg; Martina Uttenreuther-Fischer; Olaf Witt; Koen Norga; Gilles Vassal

doi:10.1016/j.ejca.2016.04.001

Implementation of mechanism of action biology-driven early drug development for children with cancer

Andrew D J Pearson, Ralf Herold, Raphaël Rousseau, Chris Copland, Brigid Bradley-Garelik, Debbie Binner, Renaud Capdeville, Hubert Caron, Jacqueline Carleer, Louis Chesler, Birgit Geoerger, Pamela Kearns, Lynley V Marshall, Stefan M Pfister, Gudrun Schleiermacher, Jeffrey Skolnik, Cesare Spadoni, Jaroslav Sterba, Hendrick van den Berg, Martina Uttenreuther-FischerOlaf Witt, Koen Norga, Gilles Vassal

Cancer Clinical Trials Unit

Research output: Contribution to journal › Article › peer-review

37 Citations (Scopus)

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Abstract

An urgent need remains for new paediatric oncology drugs to cure children who die from cancer and to reduce drug-related sequelae in survivors. In 2007, the European Paediatric Regulation came into law requiring industry to create paediatric drug (all types of medicinal products) development programmes alongside those for adults. Unfortunately, paediatric drug development is still largely centred on adult conditions and not a mechanism of action (MoA)-based model, even though this would be more logical for childhood tumours as these have much fewer non-synonymous coding mutations than adult malignancies. Recent large-scale sequencing by International Genome Consortium and Paediatric Cancer Genome Project has further shown that the genetic and epigenetic repertoire of driver mutations in specific childhood malignancies differs from more common adult-type malignancies. To bring about much needed change, a Paediatric Platform, ACCELERATE, was proposed in 2013 by the Cancer Drug Development Forum, Innovative Therapies for Children with Cancer, the European Network for Cancer Research in Children and Adolescents and the European Society for Paediatric Oncology. The Platform, comprising multiple stakeholders in paediatric oncology, has three working groups, one with responsibility for promoting and developing high-quality MoA-informed paediatric drug development programmes, including specific measures for adolescents. Key is the establishment of a freely accessible aggregated database of paediatric biological tumour drug targets to be aligned with an aggregated pipeline of drugs. This will enable prioritisation and conduct of early phase clinical paediatric trials to evaluate these drugs against promising therapeutic targets and to generate clinical paediatric efficacy and safety data in an accelerated time frame. Through this work, the Platform seeks to ensure that potentially effective drugs, where the MoA is known and thought to be relevant to paediatric malignancies, are evaluated in early phase clinical trials, and that this approach to generate pre-clinical and clinical data is systematically pursued by academia, sponsors, industry, and regulatory bodies to bring new paediatric oncology drugs to front-line therapy more rapidly.

Original language	English
Pages (from-to)	124-131
Number of pages	8
Journal	European Journal of Cancer
Volume	62
Early online date	31 May 2016
DOIs	https://doi.org/10.1016/j.ejca.2016.04.001
Publication status	Published - Jul 2016

Keywords

Paediatric oncology
Mechanism of action
Targeted cancer drug development

UN SDGs

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

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10.1016/j.ejca.2016.04.001

Pearson_et_al_Implementation_mechanism_action_biology-driven_European_Journal_Cancer
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Cite this

Pearson, A. D. J., Herold, R., Rousseau, R., Copland, C., Bradley-Garelik, B., Binner, D., Capdeville, R., Caron, H., Carleer, J., Chesler, L., Geoerger, B., Kearns, P., Marshall, L. V., Pfister, S. M., Schleiermacher, G., Skolnik, J., Spadoni, C., Sterba, J., van den Berg, H., ... Vassal, G. (2016). Implementation of mechanism of action biology-driven early drug development for children with cancer. European Journal of Cancer, 62, 124-131. Advance online publication. https://doi.org/10.1016/j.ejca.2016.04.001

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title = "Implementation of mechanism of action biology-driven early drug development for children with cancer",

abstract = "An urgent need remains for new paediatric oncology drugs to cure children who die from cancer and to reduce drug-related sequelae in survivors. In 2007, the European Paediatric Regulation came into law requiring industry to create paediatric drug (all types of medicinal products) development programmes alongside those for adults. Unfortunately, paediatric drug development is still largely centred on adult conditions and not a mechanism of action (MoA)-based model, even though this would be more logical for childhood tumours as these have much fewer non-synonymous coding mutations than adult malignancies. Recent large-scale sequencing by International Genome Consortium and Paediatric Cancer Genome Project has further shown that the genetic and epigenetic repertoire of driver mutations in specific childhood malignancies differs from more common adult-type malignancies. To bring about much needed change, a Paediatric Platform, ACCELERATE, was proposed in 2013 by the Cancer Drug Development Forum, Innovative Therapies for Children with Cancer, the European Network for Cancer Research in Children and Adolescents and the European Society for Paediatric Oncology. The Platform, comprising multiple stakeholders in paediatric oncology, has three working groups, one with responsibility for promoting and developing high-quality MoA-informed paediatric drug development programmes, including specific measures for adolescents. Key is the establishment of a freely accessible aggregated database of paediatric biological tumour drug targets to be aligned with an aggregated pipeline of drugs. This will enable prioritisation and conduct of early phase clinical paediatric trials to evaluate these drugs against promising therapeutic targets and to generate clinical paediatric efficacy and safety data in an accelerated time frame. Through this work, the Platform seeks to ensure that potentially effective drugs, where the MoA is known and thought to be relevant to paediatric malignancies, are evaluated in early phase clinical trials, and that this approach to generate pre-clinical and clinical data is systematically pursued by academia, sponsors, industry, and regulatory bodies to bring new paediatric oncology drugs to front-line therapy more rapidly.",

keywords = "Paediatric oncology, Mechanism of action, Targeted cancer drug development",

author = "Pearson, {Andrew D J} and Ralf Herold and Rapha{\"e}l Rousseau and Chris Copland and Brigid Bradley-Garelik and Debbie Binner and Renaud Capdeville and Hubert Caron and Jacqueline Carleer and Louis Chesler and Birgit Geoerger and Pamela Kearns and Marshall, {Lynley V} and Pfister, {Stefan M} and Gudrun Schleiermacher and Jeffrey Skolnik and Cesare Spadoni and Jaroslav Sterba and {van den Berg}, Hendrick and Martina Uttenreuther-Fischer and Olaf Witt and Koen Norga and Gilles Vassal",

year = "2016",

month = jul,

doi = "10.1016/j.ejca.2016.04.001",

language = "English",

volume = "62",

pages = "124--131",

journal = "European Journal of Cancer",

issn = "0959-8049",

publisher = "Elsevier",

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Pearson, ADJ, Herold, R, Rousseau, R, Copland, C, Bradley-Garelik, B, Binner, D, Capdeville, R, Caron, H, Carleer, J, Chesler, L, Geoerger, B, Kearns, P, Marshall, LV, Pfister, SM, Schleiermacher, G, Skolnik, J, Spadoni, C, Sterba, J, van den Berg, H, Uttenreuther-Fischer, M, Witt, O, Norga, K & Vassal, G 2016, 'Implementation of mechanism of action biology-driven early drug development for children with cancer', European Journal of Cancer, vol. 62, pp. 124-131. https://doi.org/10.1016/j.ejca.2016.04.001

TY - JOUR

T1 - Implementation of mechanism of action biology-driven early drug development for children with cancer

AU - Pearson, Andrew D J

AU - Herold, Ralf

AU - Rousseau, Raphaël

AU - Copland, Chris

AU - Bradley-Garelik, Brigid

AU - Binner, Debbie

AU - Capdeville, Renaud

AU - Caron, Hubert

AU - Carleer, Jacqueline

AU - Chesler, Louis

AU - Geoerger, Birgit

AU - Kearns, Pamela

AU - Marshall, Lynley V

AU - Pfister, Stefan M

AU - Schleiermacher, Gudrun

AU - Skolnik, Jeffrey

AU - Spadoni, Cesare

AU - Sterba, Jaroslav

AU - van den Berg, Hendrick

AU - Uttenreuther-Fischer, Martina

AU - Witt, Olaf

AU - Norga, Koen

AU - Vassal, Gilles

PY - 2016/7

Y1 - 2016/7

N2 - An urgent need remains for new paediatric oncology drugs to cure children who die from cancer and to reduce drug-related sequelae in survivors. In 2007, the European Paediatric Regulation came into law requiring industry to create paediatric drug (all types of medicinal products) development programmes alongside those for adults. Unfortunately, paediatric drug development is still largely centred on adult conditions and not a mechanism of action (MoA)-based model, even though this would be more logical for childhood tumours as these have much fewer non-synonymous coding mutations than adult malignancies. Recent large-scale sequencing by International Genome Consortium and Paediatric Cancer Genome Project has further shown that the genetic and epigenetic repertoire of driver mutations in specific childhood malignancies differs from more common adult-type malignancies. To bring about much needed change, a Paediatric Platform, ACCELERATE, was proposed in 2013 by the Cancer Drug Development Forum, Innovative Therapies for Children with Cancer, the European Network for Cancer Research in Children and Adolescents and the European Society for Paediatric Oncology. The Platform, comprising multiple stakeholders in paediatric oncology, has three working groups, one with responsibility for promoting and developing high-quality MoA-informed paediatric drug development programmes, including specific measures for adolescents. Key is the establishment of a freely accessible aggregated database of paediatric biological tumour drug targets to be aligned with an aggregated pipeline of drugs. This will enable prioritisation and conduct of early phase clinical paediatric trials to evaluate these drugs against promising therapeutic targets and to generate clinical paediatric efficacy and safety data in an accelerated time frame. Through this work, the Platform seeks to ensure that potentially effective drugs, where the MoA is known and thought to be relevant to paediatric malignancies, are evaluated in early phase clinical trials, and that this approach to generate pre-clinical and clinical data is systematically pursued by academia, sponsors, industry, and regulatory bodies to bring new paediatric oncology drugs to front-line therapy more rapidly.

AB - An urgent need remains for new paediatric oncology drugs to cure children who die from cancer and to reduce drug-related sequelae in survivors. In 2007, the European Paediatric Regulation came into law requiring industry to create paediatric drug (all types of medicinal products) development programmes alongside those for adults. Unfortunately, paediatric drug development is still largely centred on adult conditions and not a mechanism of action (MoA)-based model, even though this would be more logical for childhood tumours as these have much fewer non-synonymous coding mutations than adult malignancies. Recent large-scale sequencing by International Genome Consortium and Paediatric Cancer Genome Project has further shown that the genetic and epigenetic repertoire of driver mutations in specific childhood malignancies differs from more common adult-type malignancies. To bring about much needed change, a Paediatric Platform, ACCELERATE, was proposed in 2013 by the Cancer Drug Development Forum, Innovative Therapies for Children with Cancer, the European Network for Cancer Research in Children and Adolescents and the European Society for Paediatric Oncology. The Platform, comprising multiple stakeholders in paediatric oncology, has three working groups, one with responsibility for promoting and developing high-quality MoA-informed paediatric drug development programmes, including specific measures for adolescents. Key is the establishment of a freely accessible aggregated database of paediatric biological tumour drug targets to be aligned with an aggregated pipeline of drugs. This will enable prioritisation and conduct of early phase clinical paediatric trials to evaluate these drugs against promising therapeutic targets and to generate clinical paediatric efficacy and safety data in an accelerated time frame. Through this work, the Platform seeks to ensure that potentially effective drugs, where the MoA is known and thought to be relevant to paediatric malignancies, are evaluated in early phase clinical trials, and that this approach to generate pre-clinical and clinical data is systematically pursued by academia, sponsors, industry, and regulatory bodies to bring new paediatric oncology drugs to front-line therapy more rapidly.

KW - Paediatric oncology

KW - Mechanism of action

KW - Targeted cancer drug development

U2 - 10.1016/j.ejca.2016.04.001

DO - 10.1016/j.ejca.2016.04.001

M3 - Article

C2 - 27258969

SN - 0959-8049

VL - 62

SP - 124

EP - 131

JO - European Journal of Cancer

JF - European Journal of Cancer

ER -

Implementation of mechanism of action biology-driven early drug development for children with cancer

Abstract

Keywords

UN SDGs

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