Characterization of transcriptional heterogeneity and novel therapeutic targets using single cell RNA-sequencing of primary and circulating Ewing sarcoma cells

Author:

Goodspeed AndrewORCID,Bodlak Avery,Duffy Alexis B.,Nelson-Taylor Sarah,Oike NaokiORCID,Porfilio Timothy,Shirai Ryota,Walker Deandra,Treece Amy,Black JenniferORCID,Donaldson Nathan,Cost Carrye,Garrington Tim,Greffe Brian,Luna-Fineman Sandra,Demedis JennaORCID,Lake JessicaORCID,Danis Etienne,Verneris MichaelORCID,Adams Daniel LORCID,Hayashi MasanoriORCID

Abstract

AbstractEwing sarcoma is the second most common bone cancer in children, accounting for 2% of pediatric cancer diagnoses. Patients who present with metastatic disease at the time of diagnosis have a dismal prognosis, compared to the >70% 5-year survival of those with localized disease. Here, we utilized single cell RNA-sequencing to characterize the transcriptional landscape of primary Ewing sarcoma tumors and surrounding tumor microenvironment (TME). Copy-number analysis identified subclonal evolution within patients prior to treatment. Primary tumor samples demonstrate a heterogenous transcriptional landscape with several conserved gene expression programs, including those composed of genes related to proliferation and EWS targets. Single cell RNA-sequencing and immunofluorescence of circulating tumor cells at the time of diagnosis identified TSPAN8 as a novel therapeutic target.

Publisher

Cold Spring Harbor Laboratory

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