Transcription, R-loops, and RNA Splicing in Ewing Sarcoma

Abstract

Ewing sarcoma (EwS) is an aggressive pediatric bone and soft tissue cancer driven primarily by the EWSFLI1 fusion oncogene. EWS-FLI1 acts as a transcription factor and also interferes with normal regulation of transcription and transcription-associated RNA processing. We hypothesized that EWS-FLI1 driven hyper-activation of transcription causes a targetable dependence on RNA splicing in Ewingsarcoma. The specific aims of the project are to 1) determine the mechanistic relationship between EWSFLI1-driven transcription, R-loops, and splicing vulnerabilities in EwS, and 2) establish splicing as a therapeutic target in EwS. We tested the effect of depletion of key splicing factors and found an increased sensitivity in EwS compared to control cells. This was partially rescued by depleting EWSFLI1or by overexpressing RNASEH1, which degrades R-loops. EwS cells were extremely sensitive to splicing inhibition, which showed synergy with multiple chemotherapeutic agents. Splicing inhibition also caused cell cycle arrest and induced apoptosis. This work provides novel insight intotranscription regulation and its dysregulation by EWS-FLI1. In addition, our results point to RNA splicing as a potential new therapeutic target in Ewing sarcoma, which has the potential to benefit all Ewing sarcoma patients, especially those with chemo-resistant disease.

Document Details

Document Type

Technical Report

Publication Date

Jul 01, 2020

Accession Number

AD1106370

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