EcDNA-borne PVT1 fusion stabilizes oncogenic mRNAs

  1. Hyerim Yi
  2. Shu Zhang
  3. Jason Swinderman
  4. Yanbo Wang
  5. Vishnupriya Kanakaveti
  6. King L. Hung
  7. Ivy Tsz-Lo Wong
  8. Suhas Srinivasan
  9. Ellis J. Curtis
  10. Aarohi Bhargava-Shah
  11. Rui Li
  12. Matthew G. Jones
  13. Jens Luebeck
  14. Yanding Zhao
  15. Julia A. Belk
  16. Katerina Kraft
  17. Quanming Shi
  18. Xiaowei Yan
  19. Simon K. Pritchard
  20. Frances M. Liang
  21. Dean W. Felsher
  22. Luke A. Gilbert
  23. Vineet Bafna
  24. Paul S. Mischel
  25. Howard Y. Chang
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Abstract

Extrachromosomal DNA (ecDNA) amplifications are prevalent drivers of human cancers. We show that ecDNAs exhibit elevated structural variants leading to gene fusions that produce oncogene fusion transcripts. The long noncoding RNA (lncRNA) genePVT1is the most recurrent structural variant across cancer genomes, withPVT1-MYCfusions arising most frequently on ecDNA.PVT1exon 1 is the predominant 5’ partner fused toMYCor other oncogenes on the 3’ end. Mechanistic studies demonstrate thatPVT1exon 1 confers enhanced RNA stability for fusion transcripts, which requiresPVT1exon 1 interaction with SRSF1 protein. Genetic rescue of MYC-addicted cancer models and isoform-specific single-cell RNA sequencing of tumors reveal thatPVT1-MYCbetter supportsMYCdependency and better activates MYC target genesin vivo. Thus, the mutagenic landscape of ecDNA contributes to genome instability and generates chimeric fusions of lncRNA and mRNA genes, selectingPVT15’ region as a stabilizer of oncogene mRNAs.

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