Author:
Lamhamedi-Cherradi Salah-Eddine,Maitituoheti Mayinuer,Menegaz Brian A.,Krishnan Sandhya,Vetter Amelia M.,Camacho Pamela,Wu Chia-Chin,Beird Hannah C.,Porter Robert W.,Ingram Davis R.,Ramamoorthy Vandhana,Mohiuddin Sana,McCall David,Truong Danh D.,Cuglievan Branko,Futreal P. Andrew,Velasco Alejandra Ruiz,Anvar Nazanin Esmaeili,Utama Budi,Titus Mark,Lazar Alexander J.,Wang Wei-Lien,Rodriguez-Aguayo Cristian,Ratan Ravin,Livingston John A.,Rai Kunal,MacLeod A. Robert,Daw Najat C.,Hayes-Jordan Andrea,Ludwig Joseph A.
Abstract
ABSTRACTDesmoplastic small round cell tumor (DSRCT) is an aggressive, usually incurable sarcoma subtype that predominantly occurs in post-pubertal young males. Recent evidence suggests that the androgen receptor (AR) can promote tumor progression in DSRCTs. However, the mechanism of AR-induced oncogenic stimulation remains undetermined. Herein, we demonstrate that enzalutamide and AR-directed antisense oligonucleotides (AR-ASO) block 5α-dihydrotestosterone (DHT)-induced DSRCT cell proliferation and reduce xenograft tumor burden. Gene expression analysis and chromatin immunoprecipitation sequencing (ChIP-seq) were performed to elucidate how AR signaling regulates cellular epigenetic programs. Remarkably, ChIP-seq revealed novel DSRCT-specific AR DNA binding sites adjacent to key oncogenic regulators, including WT1 (the C-terminal partner of the pathognomonic fusion protein) and FOXF1. Additionally, AR occupied enhancer sites that regulate the Wnt pathway, neural differentiation, and embryonic organ development, implicating AR in dysfunctional cell lineage commitment. Our findings have immediate clinical implications given the widespread availability of FDA-approved androgen-targeted agents used for prostate cancer.ONE SENTENCE SUMMARYWe demonstrate that DSRCT, an aggressive pediatric cancer, is an AR-driven malignancy capable of responding to androgen deprivation therapy.
Publisher
Cold Spring Harbor Laboratory