Treatment resistance to platinum-based chemotherapy in lung and ovarian cancer is driven by a targetable TGFβ senescent secretome.

Platinum-based chemotherapy is commonly used for non-small cell lung cancer (NSCLC) and high-grade serous ovarian cancer (HGSOC) treatments, yet clinical outcomes remain poor. Cellular senescence and its associated secretory phenotype (SASP) can have multiple tumor-promoting activities, but both are largely unexplored in these cancers. In this study, using xenograft, orthotopic and KrasG12V-driven murine NSCLC models, we demonstrate that cisplatin-induced senescence strongly promotes malignant phenotypes and tumor progression, which is stimulated by aging. Mechanistically, we found that a transforming growth factor-beta (TGFβ)-enriched SASP drives pro-proliferative effects through TGFBR1 and AKT/mTOR. TGFBR1 inhibition with galunisertib or senolytic treatment reduces tumor progression driven by cisplatin-induced senescence, and concomitant use of TGFBR1 inhibitors with platinum-based chemotherapy reduces tumor burden and improves survival. Finally, we validate the translational relevance of tumor-promoting TGFβ-enriched SASP using clinical NSCLC and HGSOC samples from patients who received neoadjuvant platinum-based chemotherapy. Together, our findings identify a potential cancer therapy resistance mechanism and provide preclinical proof of concept for future trials.

Keywords

32 Biomedical and Clinical Sciences

Journal Title

Nat Aging

Journal ISSN

2662-8465
2662-8465

Publisher

Springer Science and Business Media LLC

Publisher DOI

https://doi.org/10.1038/s43587-025-01054-2

Rights and licensing

Except where otherwised noted, this item's license is described as Attribution 4.0 International

Sponsorship

Medical Research Council (MR/R000530/1)
Cancer Research UK (A26989)
Addenbrooke's Charitable Trust (ACT) (900365)
Cancer Research UK (C62187/A29760)
Downing College (Unknown)
Cancer Research UK (C63389/A30462)
National Institute for Health and Care Research (IS-BRC-1215-20014)

The Muñoz-Espín laboratory is supported by the Cancer Research UK (CRUK) Cambridge Centre Early Detection Programme (RG86786), by a CRUK Programme Foundation Award (C62187/A29760), by a CRUK Early Detection OHSU Project Award (C62187/A26989), and by a Medical Research Council (MRC) New Investigator Research Grant (NIRG) (MR/R000530/1). E.G.-G. was holder of a “La Caixa” Foundation Scholarship for postgraduate studies at European Universities and funded by the CRUK Cambridge Centre Early Detection Programme. D.M. was funded by a New Investigator Research Grant (NIRG) (MR/R000530/1) and a CRUK Programme Foundation Award (C62187/A29760). S.M. is funded by a CRUK Programme Foundation Award (C62187/A29760). J.G. is funded by a Darley/Sands Downing College Fellowship (G109261). H-L.O. is funded by a CRUK Early Detection OHSU Project Award (C62187/A26989) and M.D. is funded by an Evelyn Trust Fellowship (G113971). V.G. is financially supported by the European Regional Development Fund of the European Union and Greek national funds through the Operational Program Competitiveness, Entrepreneurship and Innovation, under the call RESEARCH - CREATE – INNOVATE (project code: T1EDK02939) and NKUA-SARG grant 70/3/8916. This research was supported by the NIHR Cambridge Biomedical Research Centre (BRC-1215-20014) through funding to R.C.R. and D.M.R. G.J.D. was supported by funding through the Cancer Research UK Cambridge Centre, Thoracic Cancer Programme. M.N. and I.O. were supported by Cancer Research UK Cambridge Institute’s Core Grant (C9545/A29580) (MN) and Cancer Research UK Pioneer Award (C63389/A30462). J.D.B was supported by Cancer Research UK and Cancer Research UK Cambridge Centre (A25177, 22905, 100005) and the NIHR Cambridge Biomedical Research Centre (BRC-1215-20014). M.A.V.R. was supported by a Cancer Research UK Cambridge Centre Clinical Research Training Fellowship (A25177).

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