Author
Listed:
- Laura Bornes
(The Netherlands Cancer Institute)
- Lennart J. Winden
(The Netherlands Cancer Institute)
- Veerle C. M. Geurts
(The Netherlands Cancer Institute)
- Beaunelle Bruijn
(KU Leuven Department of Oncology)
- Leyla Azarang
(The Netherlands Cancer Institute)
- Mirthe Lanfermeijer
(The Netherlands Cancer Institute)
- Marika Caruso
(KU Leuven Department of Oncology)
- Natalie Proost
(The Netherlands Cancer Institute)
- Manon Boeije
(The Netherlands Cancer Institute)
- Jeroen O. Lohuis
(The Netherlands Cancer Institute)
- Guillaume Belthier
(The Netherlands Cancer Institute)
- Eulàlia Noguera Delgado
(The Netherlands Cancer Institute)
- Nadia Gruil
(Leiden University Medical Center)
- Judith R. Kroep
(Leiden University Medical Center)
- Marieke Ven
(The Netherlands Cancer Institute)
- Renee Menezes
(The Netherlands Cancer Institute)
- Jelle Wesseling
(The Netherlands Cancer Institute
The Netherlands Cancer Institute – Antoni van Leeuwenhoek
Leiden University Medical Center)
- Marleen Kok
(The Netherlands Cancer Institute
The Netherlands Cancer Institute)
- Sabine Linn
(The Netherlands Cancer Institute
The Netherlands Cancer Institute
Utrecht University Medical Center)
- Annegien Broeks
(The Netherlands Cancer Institute)
- Huub H. Rossum
(The Netherlands Cancer Institute)
- Colinda L. G. J. Scheele
(KU Leuven Department of Oncology)
- Jacco Rheenen
(The Netherlands Cancer Institute)
Abstract
The response of breast cancer to neoadjuvant chemotherapy (NAC) varies substantially, even when tumours belong to the same molecular or histological subtype1. Here we identify the oestrous cycle as an important contributor to this heterogeneity. In three mouse models of breast cancer, we show reduced responses to NAC when treatment is initiated during the dioestrus stage, when compared with initiation during the oestrus stage. Similar findings were observed in retrospective premenopausal cohorts of human patients. Mechanistically, the dioestrus stage exhibits systemic and localized changes, including (1) an increased number of cells undergoing epithelial-to-mesenchymal transition linked to chemoresistance2–4 and (2) decreased tumour vessel diameter, suggesting potential constraints to drug sensitivity and delivery. In addition, an elevated presence of macrophages, previously associated with chemoresistance induction5, characterizes the dioestrus phase. Whereas NAC disrupts the oestrous cycle, this elevated macrophage prevalence persists and depletion of macrophages mitigates the reduced therapy response observed when initiating treatment during dioestrus. Our data collectively demonstrate the oestrous cycle as a crucial infradian rhythm determining chemosensitivity, warranting future clinical studies to exploit optimal treatment initiation timing for enhanced chemotherapy outcomes.
Suggested Citation
Laura Bornes & Lennart J. Winden & Veerle C. M. Geurts & Beaunelle Bruijn & Leyla Azarang & Mirthe Lanfermeijer & Marika Caruso & Natalie Proost & Manon Boeije & Jeroen O. Lohuis & Guillaume Belthier , 2025.
"The oestrous cycle stage affects mammary tumour sensitivity to chemotherapy,"
Nature, Nature, vol. 637(8044), pages 195-204, January.
Handle:
RePEc:nat:nature:v:637:y:2025:i:8044:d:10.1038_s41586-024-08276-1
DOI: 10.1038/s41586-024-08276-1
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