Single cell RNA-sequencing of Ewing sarcoma tumors demonstrates transcriptional heterogeneity and clonal evolution

Author:

Goodspeed AndrewORCID,Bodlak Avery,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,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 even 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. We also were able to identify the composition of the TME and molecularly dissect the transcriptional profile of circulating tumor cells in peripheral blood at the time of diagnosis.

Publisher

Cold Spring Harbor Laboratory

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