Molecular Profiling of Hard-to-Treat Childhood and Adolescent Cancers

Fida Khater,Thai Hoa Tran,Josée Brossard,Dorothée Dal Soglio,Thomas Sontag,Natalie Patey,Nada Jabado,Stéphanie Vairy ,Pierre Teira,Henrique Bittencourt,Yvan Samson,Sonia Cellot,Nelson Piché,Sophie Dumoucel,Caroline Laverdière ,Bruno Michon,Pascal St-Onge,Josette Champagne,Michel Duval,Monia Marzouki,Benjamin Ellezam,Jean‐Marie Leclerc ,Sylvie Langlois,Sébastien Perreault,Daniel Sinnett

doi:10.1001/jamanetworkopen.2019.2906

Abstract

Little progress in pediatric cancer treatment has been noted in the past decade, urging the development of novel therapeutic strategies for adolescents and children with hard-to-treat cancers. Use of comprehensive molecular profiling in the clinical management of children and adolescents with cancer appears a suitable approach to improve patient care and outcomes, particularly for hard-to-treat cases. To assess the feasibility of identifying potentially actionable mutations using next-generation sequencing-based assays in a clinically relevant time frame. This diagnostic study reports the results of the TRICEPS study, a prospective genome sequencing study conducted in Québec, Canada. Participants, aged 18 years or younger at diagnosis, with refractory or relapsed childhood and adolescent cancers were enrolled from April 2014 through January 2018. Whole-exome sequencing (WES) of matched tumor normal samples and RNA sequencing of tumor were performed to identify single-nucleotide variants, fusion transcripts, differential gene expression, and copy number alterations. Results reviewed by a team of experts were further annotated, synthesized into a report, and subsequently discussed in a multidisciplinary molecular tumor board. Molecular profiling of pediatric patients with hard-to-treat cancer, identification of actionable and targetable alteration needed for the management of these patients, and proposition of targeted and personalized novel therapeutic strategies. A total of 84 patients with hard-to-treat cancers were included in the analysis. These patients had a mean (range) age of 10.1 (1-21) years and a similar proportion of male (45 [54%]) and female (39 [46%]). Sixty-two patients (74%) had suitable tissues for multimodal molecular profiling (WES and RNA sequencing). The process from DNA or RNA isolation to genomic sequencing and data analysis steps took a median (range) of 24 (4-41) days. Potentially actionable alterations were identified in 54 of 62 patients (87%). Actions were taken in 22 of 54 patients (41%), and 18 (33%) either were on a second or third line of treatment, were in remission, or had stable disease and thus no actions were taken. Incorporating genomic sequencing into the management of hard-to-treat childhood and adolescent cancers appeared feasible; molecular profiling may enable the identification of potentially actionable alterations with clinical implications for most patients, including targeted therapy and clinically relevant information of diagnostic, prognostic, and monitoring significance.

Highlights

Childhood and adolescent cancers constitute a heterogeneous group of rare diseases
Incorporating genomic sequencing into the management of hard-to-treat childhood and adolescent cancers appeared feasible; molecular profiling may enable the identification of potentially actionable alterations with clinical implications for most patients
For patient 19, we sequenced the primary leukemia sample because of low blast count (Յ25%) in the relapsed sample; we confirmed the results in the relapsed material

Summary

Introduction

Childhood and adolescent cancers constitute a heterogeneous group of rare diseases. Multicentric clinical trials have led to the continuing refinement of cancer subtype classification and the development of improved risk-adapted treatment strategies, with overall survival rates currently reaching approximately 80%.1,2 Despite these advances, cases of refractory and recurrent cancers are associated with a poor prognosis and death. The advent of next-generation sequencing (NGS) technologies has revolutionized the study of cancers, offering unprecedented opportunities to fully characterize cancer genomes It has accelerated the search for somatic mutations, which can be applied to whole genomes and transcriptomes to unravel molecular signatures.[7,8,9,10,11,12] In-depth molecular profiling of individual tumors has allowed the identification of potentially actionable mutations that could lead to therapeutic interventions and new drug targets.[11,13,14,15,16] Several initiatives have begun to integrate cancer genomic–based information into the care of patients with childhood cancer. These initiatives have demonstrated the feasibility of such strategies at a single site or across multiple sites.[17,18,19,20,21,22] They have reported many genomic biomarkers or oncogenic drivers that have been proven useful to tailored patient management

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