MultiDimensional ClinOmics for Precision Therapy of Children and Adolescent Young Adults with Relapsed and Refractory Cancer: A Report from the Center for Cancer Research

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2016 Mar 20

PMID 26994145

Citations 60

Authors

Wendy Chang

Andrew S Brohl

Rajesh Patidar

Sivasish Sindiri

Jack F Shern

Jun S Wei

Young K Song

Marielle E Yohe

Berkley Gryder

Shile Zhang

Kathleen A Calzone

Nityashree Shivaprasad

Xinyu Wen

Thomas C Badgett

Markku Miettinen

Kip R Hartman

James C League-Pascual

Toby N Trahair

Brigitte C Widemann

Melinda S Merchant

Rosandra N Kaplan

Jimmy C Lin

Javed Khan

Affiliations

Soon will be listed here.

Abstract

Purpose: We undertook a multidimensional clinical genomics study of children and adolescent young adults with relapsed and refractory cancers to determine the feasibility of genome-guided precision therapy.

Experimental Design: Patients with non-central nervous system solid tumors underwent a combination of whole exome sequencing (WES), whole transcriptome sequencing (WTS), and high-density single-nucleotide polymorphism array analysis of the tumor, with WES of matched germline DNA. Clinically actionable alterations were identified as a reportable germline mutation, a diagnosis change, or a somatic event (including a single nucleotide variant, an indel, an amplification, a deletion, or a fusion gene), which could be targeted with drugs in existing clinical trials or with FDA-approved drugs.

Results: Fifty-nine patients in 20 diagnostic categories were enrolled from 2010 to 2014. Ages ranged from 7 months to 25 years old. Seventy-three percent of the patients had prior chemotherapy, and the tumors from these patients with relapsed or refractory cancers had a higher mutational burden than that reported in the literature. Thirty patients (51% of total) had clinically actionable mutations, of which 24 (41%) had a mutation that was currently targetable in a clinical trial setting, 4 patients (7%) had a change in diagnosis, and 7 patients (12%) had a reportable germline mutation.

Conclusions: We found a remarkably high number of clinically actionable mutations in 51% of the patients, and 12% with significant germline mutations. We demonstrated the clinical feasibility of next-generation sequencing in a diverse population of relapsed and refractory pediatric solid tumors. Clin Cancer Res; 22(15); 3810-20. ©2016 AACR.

Citing Articles

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The economic costs of precision medicine for clinical translational research among children with high-risk cancer.

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Wijeratne S, E Hernandez Gonzalez M, Roach K, Miller K, Schieffer K, Fitch J BMC Genomics. 2024; 25(1):122.

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