DNA damage response signatures are associated with frontline chemotherapy response and routes of tumor evolution in extensive stage small cell lung cancer

  1. Benjamin B. Morris
  2. Simon Heeke
  3. Yuanxin Xi
  4. Lixia Diao
  5. Qi Wang
  6. Pedro Rocha
  7. Edurne Arriola
  8. Myung Chang Lee
  9. Darren R. Tyson
  10. Kyle Concannon
  11. Kavya Ramkumar
  12. C. Allison Stewart
  13. Robert J. Cardnell
  14. Runsheng Wang
  15. Vito Quaranta
  16. Jing Wang
  17. John V. Heymach
  18. Barzin Y. Nabet
  19. David S. Shames
  20. Carl M. Gay
  21. Lauren A. Byers
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Abstract

Introduction

A hallmark of small cell lung cancer (SCLC) is its recalcitrance to therapy. While most SCLCs respond to frontline therapy, resistance inevitably develops. Identifying phenotypes potentiating chemoresistance and immune evasion is a crucial unmet need. Previous reports have linked upregulation of the DNA damage response (DDR) machinery to chemoresistance and immune evasion across cancers. However, it is unknown if SCLCs exhibit distinct DDR phenotypes.

Methods

To study SCLC DDR phenotypes, we developed a new DDR gene analysis method and applied it to SCLC clinical samples, in vitro , and  in vivo model systems. We then investigated how DDR regulation is associated with SCLC biology, chemotherapy response, and tumor evolution following therapy.

Results

Using multi-omic profiling, we demonstrate that SCLC tumors cluster into three DDR phenotypes with unique molecular features. Hallmarks of these DDR clusters include differential expression of DNA repair genes, increased replication stress, and heightened G2/M cell cycle arrest. SCLCs with elevated DDR phenotypes exhibit increased neuroendocrine features and decreased “inflamed” biomarkers, both within and across SCLC subtypes. Clinical analyses demonstrated treatment naive DDR status was associated with different responses to frontline chemotherapy. Using longitudinal liquid biopsies, we found that DDR Intermediate and High tumors exhibited subtype switching and coincident emergence of heterogenous phenotypes following frontline treatment.

Conclusions

We establish that SCLC can be classified into one of three distinct, clinically relevant DDR clusters. Our data demonstrates that DDR status plays a key role in shaping SCLC phenotypes and may be associated with different chemotherapy responses and patterns of tumor evolution. Future work targeting DDR specific phenotypes will be instrumental in improving patient outcomes.

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  1. Version published to 10.1186/s12943-025-02291-0
  2. Version published to 10.1101/2024.07.29.605595 on bioRxiv