Nature Communications (Oct 2024)

Epigenetic memory of radiotherapy in dermal fibroblasts impairs wound repair capacity in cancer survivors

  • Xiaowei Bian,
  • Minna Piipponen,
  • Zhuang Liu,
  • Lihua Luo,
  • Jennifer Geara,
  • Yongjian Chen,
  • Traimate Sangsuwan,
  • Monica Maselli,
  • Candice Diaz,
  • Connor A. Bain,
  • Evelien Eenjes,
  • Maria Genander,
  • Michael Crichton,
  • Jenna L. Cash,
  • Louis Archambault,
  • Siamak Haghdoost,
  • Julie Fradette,
  • Pehr Sommar,
  • Martin Halle,
  • Ning Xu Landén

DOI
https://doi.org/10.1038/s41467-024-53295-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 20

Abstract

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Abstract Radiotherapy (RT), a common cancer treatment, unintentionally harms surrounding tissues, including the skin, and hinders wound healing years after treatment. This study aims to understand the mechanisms behind these late-onset adverse effects. We compare skin biopsies from previously irradiated (RT+) and non-irradiated (RT−) sites in breast cancer survivors who underwent RT years ago. Here we show that the RT+ skin has compromised healing capacity and fibroblast functions. Using ATAC-seq, we discover altered chromatin landscapes in RT+ fibroblasts, with THBS1 identified as a crucial epigenetically primed wound repair-related gene. This is further confirmed by single-cell RNA-sequencing and spatial transcriptomic analysis of human wounds. Notably, fibroblasts in both murine and human post-radiation wound models show heightened and sustained THBS1 expression, impairing fibroblast motility and contractility. Treatment with anti-THBS1 antibodies promotes ex vivo wound closure in RT+ skin from breast cancer survivors. Our findings suggest that fibroblasts retain a long-term radiation memory in the form of epigenetic changes. Targeting this maladaptive epigenetic memory could mitigate RT’s late-onset adverse effects, improving the quality of life for cancer survivors.