Tracking clonal evolution of drug resistance in ovarian cancer patients by exploiting structural variants in cfDNA

  1. Marc J. Williams
  2. Ignacio Vázquez-García
  3. Grittney Tam
  4. Michelle Wu
  5. Nancy Varice
  6. Eliyahu Havasov
  7. Hongyu Shi
  8. Gryte Satas
  9. Hannah J. Lees
  10. Jake June-Koo Lee
  11. Matthew A. Myers
  12. Matthew Zatzman
  13. Nicole Rusk
  14. Emily Ali
  15. Ronak H Shah
  16. Michael F. Berger
  17. Neeman Mohibullah
  18. Yulia Lakhman
  19. Dennis S. Chi
  20. Nadeem R. Abu-Rustum
  21. Carol Aghajanian
  22. Andrew McPherson
  23. Dmitriy Zamarin
  24. Brian Loomis
  25. Britta Weigelt
  26. Claire F. Friedman
  27. Sohrab P. Shah
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Abstract

Drug resistance is the major cause of therapeutic failure in high-grade serous ovarian cancer (HGSOC). Yet, the mechanisms by which tumors evolve to drug resistant states remains largely unknown. To address this, we aimed to exploit clone-specific genomic structural variations by combining scaled single-cell whole genome sequencing with longitudinally collected cell-free DNA (cfDNA), enabling clonal tracking before, during and after treatment. We developed a cfDNA hybrid capture, deep sequencing approach based on leveraging clone-specific structural variants as endogenous barcodes, with orders of magnitude lower error rates than single nucleotide variants in ctDNA (circulating tumor DNA) detection, demonstrated on 19 patients at baseline. We then applied this to monitor and model clonal evolution over several years in ten HGSOC patients treated with systemic therapy from diagnosis through recurrence. We found drug resistance to be polyclonal in most cases, but frequently dominated by a single high-fitness and expanding clone, reducing clonal diversity in the relapsed disease state in most patients. Drug-resistant clones frequently displayed notable genomic features, including high-level amplifications of oncogenes such as CCNE1 , RAB25 , NOTCH3 , and ERBB2 . Using a population genetics Wright-Fisher model, we found evolutionary trajectories of these features were consistent with drug-induced positive selection. In select cases, these alterations impacted selection of secondary lines of therapy with positive patient outcomes. For cases with matched single-cell RNA sequencing data, pre-existing and genomically encoded phenotypic states such as upregulation of EMT and VEGF were linked to drug resistance. Together, our findings indicate that drug resistant states in HGSOC pre-exist at diagnosis and lead to dramatic clonal expansions that alter clonal composition at the time of relapse. We suggest that combining tumor single cell sequencing with cfDNA enables clonal tracking in patients and harbors potential for evolution-informed adaptive treatment decisions.

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  1. Version published to 10.1101/2024.08.21.609031v1 on bioRxiv