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Rare subclonal sequencing of breast cancers indicates putative metastatic driver mutations are predominately acquired after dissemination.

Matthew R Lawrence-PaulTien-Chi PanDhruv K PantNatalie N C ShihYan ChenGeorge K BelkaMichael FeldmanAngela DeMicheleLewis A Chodosh
Published in: Genome medicine (2024)
Our results strongly suggest that metastatic driver mutations are sequentially acquired and selected within the same clonal lineage both before, but more commonly after, dissemination from the primary tumor, and that these mutations are biologically consequential. Despite inherent limitations in sampling archival primary tumors, our findings indicate that tumor cells in most patients continue to undergo clinically relevant genomic evolution after their dissemination from the primary tumor. This provides further evidence that metastatic recurrence is a multi-step, mutation-driven process that extends beyond primary tumor dissemination and underscores the importance of longitudinal tumor assessment to help guide clinical decisions.
Keyphrases
  • squamous cell carcinoma
  • small cell lung cancer
  • end stage renal disease
  • ejection fraction
  • chronic kidney disease
  • single cell
  • gene expression
  • peritoneal dialysis
  • prognostic factors
  • copy number
  • cross sectional