Systematic target actionability reviews of preclinical proof-of-concept papers to match targeted drugs to paediatric cancers

Schubert, Nil A.; Lowery, Caitlin D.; Bergthold, Guillaume; Koster, Jan; Eleveld, Thomas F.; Rodríguez, Ana Isabel Enríquez; Jones, David; Vassal, Gilles; Stancato, Louis F.; Pfister, Stefan M.; Caron, Hubert; Molenaar, Jan J.

doi:10.1016/j.ejca.2020.01.027

Cited by 8 publications

(15 citation statements)

References 59 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This argues a strong case for the need to systematically review proof-of-concept (PoC) preclinical data to match paediatric tumour entities to the most promising therapeutic options. To address this, the target actionability review (TAR) methodology [6] was previously established as part of the innovative therapies for children with cancer paediatric preclinical PoC platform (ITCC-P4), an innovative medicines initiative 2-funded publiceprivate partnership between academic research institutions and pharmaceutical companies [7]. In a pilot TAR evaluating the MDM2-TP53 pathway in primary tumour data and preclinical models of paediatric cancers, we demonstrated that the TAR methodology provided the most comprehensive overview of available preclinical data on targeting of MDM2 in paediatric cancer to date [6].…”

Section: Introductionmentioning

confidence: 99%

Target actionability review to evaluate CDK4/6 as a therapeutic target in paediatric solid and brain tumours

Schubert

Chen

Rodríguez

et al. 2022

European Journal of Cancer

Self Cite

View full text Add to dashboard Cite

Section: Introductionmentioning

confidence: 99%

Target actionability review to evaluate CDK4/6 as a therapeutic target in paediatric solid and brain tumours

Schubert

Chen

Rodríguez

et al. 2022

European Journal of Cancer

Self Cite

View full text Add to dashboard Cite

“…The Pediatric Preclinical Testing Program (PPTP), sponsored by the US NCI, has been operating productively for several years, yielding dozens of publications on drug screens in various pediatric cancer models [ 47 ]. A European consortium formed the Innovative Therapy for Children with Cancer Paediatric Preclinical Proof-of-Concept Platform (ITCC-P4), a joint academic–pharmaceutical industry platform to characterize and prioritize targets in high-risk pediatric solid tumors [ 30 , 48 ] and facilitate tumor model development and drug screening. A pediatric preclinical public–private partnership is also being considered in the US [ 49 ].…”

Section: Key Recommendations: Preclinical/translationalmentioning

confidence: 99%

“…For drug targets not listed on the FDA’s relevant target list or the non-relevant target list (i.e., relevance not yet determined), the current FDA guidance provides a good outline of specific studies needed to establish relevance. In addition, Schubert et al recently published a more comprehensive framework of key experimental evidence for assessing target relevance and priority [ 48 ]. However, as the FDA is tasked with establishing relevance, it is unclear to what extent the sponsor is required to invest in such research.…”

Section: Key Recommendations: Preclinical/translationalmentioning

confidence: 99%

Navigating the Regulatory Landscape to Develop Pediatric Oncology Drugs: Expert Opinion Recommendations

et al. 2021

View full text Add to dashboard Cite

Regulatory changes have been enacted in the United States (US) and European Union (EU) to encourage the development of new treatments for pediatric cancer. Here, we review some of the factors that have hampered the development of pediatric cancer treatments and provide a comparison of the US and EU regulations implemented to address this clinical need. We then provide some recommendations for each stage of the oncology drug development pathway to help researchers maximize their chance of successful drug development while complying with regulations. A key recommendation is the engagement of key stakeholders such as regulatory authorities, pediatric oncologists, academic researchers, patient advocacy groups, and a Pediatric Expert Group early in the drug development process. During drug target selection, sponsors are encouraged to consult the Food and Drug Administration (FDA), European Medicines Agency (EMA), and the FDA target list, in addition to relevant US and European consortia that have been established to characterize and prioritize oncology drug targets. Sponsors also need to carefully consider the resourcing requirements for preclinical testing, which include ensuring appropriate access to the most relevant databases, clinical samples, and preclinical models (cell lines and animal models). During clinical development, sponsors can account for the pharmacodynamic (PD)/pharmacokinetic (PK) considerations specific to a pediatric population by developing pediatric formulations, selecting suitable PD endpoints, and employing sparse PK sampling or modeling/simulation of drug exposures where appropriate. Additional clinical considerations include the specific design of the clinical trial, the potential inclusion of children in adult trials, and the value of cooperative group trials. Plain Language SummaryIn the last few decades, great progress has been made in developing new treatments for adult cancers. However, development of new treatments for childhood cancers has been much slower. To encourage drug companies (sponsors) to develop effective treatments for childhood cancer, authorities in the United States (US) and Europe have made new rules for drug development. Under these new rules, sponsors developing drugs for specific cancers in adults have to consider whether the target of that drug also causes cancers in children. If this is the case, sponsors have to carry out clinical studies of their drug in children who have cancer that is caused by the same drug target. In this article, we describe some reasons for why drug development for childhood cancers has been slow and the rules created to address this problem in the US and Europe. We share some recommendations to help sponsors maximize their chances of developing an effective drug in children while satisfying the new rules. Specifically, sponsors need to be aware of the differences between studying drugs in adults versus children and how these influence the way the drug is tested. We make several recommendations for each stage of the development process, b...

show abstract

“…These are just a couple of the many reasons why industry is beginning to develop deeper ties with the pediatric research community. This deepening relationship is already contributing to advances in the understanding of target biology in pediatric cancers (e.g., "target actionability reviews"), 23 led to the development of an international consensus on the depth and breadth of preclinical data required for moving a promising agent into pediatric clinical development, 24 and resulted in the creation of precompetitive PPPs that bring academia and industry together to identify promising drugs for children dying from cancer. Of note regarding PPPs is the formal voice given to the critical but often overlooked contribution of patient advocacy, which plays a vital role in building bridges to all stakeholders while maintaining a patient focus.…”

Section: Setting the Stage For Industry Collaborationmentioning

confidence: 99%

“…ITCC-P4 has also established a methodology for the systematic in silico evaluation of selected compounds and corresponding actionable molecular targets and pathways in the different pediatric solid tumor entities (target actionability reviews) before the in vitro and in vivo testing phases to comprehensively assess relevant literature and the existing (epi)genomic and transcriptomic data sets of all entities in question. 23 To facilitate the design of preclinical packages for regulatory purposes, a joint ITCC-P4 and PPTC multistakeholder workshop with representatives from regulatory networks and industry, patient advocates, and academia established an international consensus on minimum preclinical testing requirements for the evaluation of compounds in pediatric oncology. 24 The ultimate goal is to deliver a sustainable high-quality preclinical testing platform with unique, fully characterized models and access to molecular information to serve the needs of both the biopharmaceutical industry as part of the new regulatory environment and the academic research community in an effort to continue to gain knowledge on pediatric malignancies and to drive pediatric oncology drug development through science in a much more rigorous and systematic way.…”

Section: Eu Perspective On Academia-industry Collaboration: Development and Status Of The Itcc-p4mentioning

confidence: 99%

Crossing Oceans: Preclinical Collaboration to Improve Pediatric Drug Development

Reaman

Stancato

Vassal

et al. 2020

American Society of Clinical Oncology Educational Book

Self Cite

View full text Add to dashboard Cite

Changes in the regulatory environment affecting pediatric cancer drug development in the United States and the European Union provide unprecedented opportunity to advance the concept of precision medicine to children with cancer. Increasing evidence suggests that new drugs and biologic products directed at molecular targets presumed to be etiologically associated with many adult cancers may well provide therapeutic options for selected subsets of children with cancer despite their histologic and biologic differences. Regulatory requirements for early evaluation of appropriate new drugs for children based on their molecular mechanism of action, rather than the specific clinical indications for which they are developed and/or approved, will shorten the unacceptable time lag between first-in-human and first-in-children studies. The relative scarcity of pediatric patients eligible for biomarker-directed studies and the ever-expanding compendium of new targeted agents mandate rational, science-based decision-making in selecting and prioritizing appropriate drugs to study early in development. A critical component of the evidence base in such decision-making includes preclinical testing of relevant drugs in pediatric tumor-specific in vitro and in vivo models. Established preclinical testing programs with academic investigator–industry collaborations are actively engaged in such activities. International collaboration is required to address the resource constraints and increasing number of potential products to be tested in a timely, efficient, nonduplicative, and cost-effective manner.

show abstract

Systematic target actionability reviews of preclinical proof-of-concept papers to match targeted drugs to paediatric cancers

Cited by 8 publications

References 59 publications

Target actionability review to evaluate CDK4/6 as a therapeutic target in paediatric solid and brain tumours

Target actionability review to evaluate CDK4/6 as a therapeutic target in paediatric solid and brain tumours

Navigating the Regulatory Landscape to Develop Pediatric Oncology Drugs: Expert Opinion Recommendations

Crossing Oceans: Preclinical Collaboration to Improve Pediatric Drug Development

Contact Info

Product

Resources

About