Targeting Oxidative Stress in Embryonal Rhabdomyosarcoma

Xiang Chen,Sheila Shurtleff,Steve Skapek,Kristy Boggs,Michael Rusch,Fred Krafcik,Armita Bahrami,Lyudmila Tsurkan,Gang Wu,Jianmin Wang,Viktor Tolleman,Erin Hedlund,Cori Bradley,Chris Morton,Panduka Nagahawatte,Jinghui Zhang,Charles Lu,Lei Wei,Virginia Valentine,John Easton,Donald Yergeau,Monika Wierdl,David Finkelstein,Justina Mcevoy,Matthew Parker,Chunxu Qu,Li Ding,Marcus B Valentine ,Nilsa C Ramirez ,Andrew M Davidoff ,Elizabeth A Stewart ,James R Downing ,John A Sandoval ,Mark E Hatley ,Elaine R Mardis ,Walter H Lang ,Heather L Mulder ,Richard K Wilson ,Alberto S Pappo ,Sara M Federico ,Michael N Edmonson ,Douglas S Hawkins ,Philip M Potter ,Anang A Shelat ,Sheri L Spunt ,Michael A Dyer

doi:10.1016/j.ccr.2013.11.002

Abstract

Rhabdomyosarcoma is a soft-tissue sarcoma with molecular and cellular features of developing skeletal muscle. Rhabdomyosarcoma has two major histologic subtypes, embryonal and alveolar, each with distinct clinical, molecular, and genetic features. Genomic analysis shows that embryonal tumors have more structural and copy number variations than alveolar tumors. Mutations in the RAS/NF1 pathway are significantly associated with intermediate- and high-risk embryonal rhabdomyosarcomas (ERMS). In contrast, alveolar rhabdomyosarcomas (ARMS) have fewer genetic lesions overall and no known recurrently mutated cancer consensus genes. To identify therapeutics for ERMS, we developed and characterized orthotopic xenografts of tumors that were sequenced in our study. High-throughput screening of primary cultures derived from those xenografts identified oxidative stress as a pathway of therapeutic relevance for ERMS.

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