Circulating tumor cells in metastatic breast cancer patients treated with immune checkpoint inhibitors – a biomarker analysis of the ALICE and ICON trials

Author:

Andresen Nikolai Kragøe123ORCID,Røssevold Andreas Hagen123,Borgen Elin4,Schirmer Cecilie Bendigtsen4,Gilje Bjørnar5,Garred Øystein4,Lømo Jon4,Stensland Marius5,Nordgård Oddmund56ORCID,Falk Ragnhild Sørum7,Mathiesen Randi R.8,Russnes Hege G.349,Kyte Jon Amund1210ORCID,Naume Bjørn38ORCID

Affiliation:

1. Department of Clinical Cancer Research Oslo University Hospital Norway

2. Department of Cancer Immunology, Institute for Cancer Research Oslo University Hospital Norway

3. Institute of Clinical Medicine University of Oslo Norway

4. Department of Pathology Oslo University Hospital Norway

5. Department of Hematology and Oncology Stavanger University Hospital Norway

6. Department of Chemistry, Bioscience and Environmental Technology University of Stavanger Norway

7. Oslo Centre for Biostatistics and Epidemiology Oslo University Hospital Norway

8. Department of Oncology Oslo University Hospital Norway

9. Department of Cancer Genetics, Institute for Cancer Research Oslo University Hospital Norway

10. Faculty of Health Sciences Oslo Metropolitan University Norway

Abstract

Immune checkpoint inhibitors (ICIs) have been introduced in breast cancer (BC) treatment and better biomarkers are needed to predict benefit. Circulating tumor cells (CTCs) are prognostic in BC, but knowledge is limited on CTCs in the context of ICI therapy. In this study, serial sampling of CTCs (CellSearch system) was evaluated in 82 patients with metastatic BC enrolled in two randomized trials investigating ICI plus chemotherapy. Programmed death‐ligand 1 (PD‐L1) expression on CTCs was also measured. Patients with ≥ 2 CTCs per 7.5 mL at baseline had gene expression profiles in tumor suggestive of increased T‐cell activity, including increased tumor inflammation signature (TIS) in both triple‐negative (P = 0.010) and hormone receptor‐positive (P = 0.024) disease. Patients with luminal A BC had higher CTC levels. The association between CTC status and outcome was most apparent 4 weeks into therapy. PD‐L1 expression in CTCs was observed in 6/17 CTC‐positive patients and was associated with inferior survival. In conclusion, our study indicates that CTC numbers may inform on tumor immune composition, as well as prognosis. These findings suggest a potential of using CTCs as an accessible biomarker source in BC patients treated with immunotherapy.

Funder

Helse Sør-Øst RHF

Kreftforeningen

Roche

Publisher

Wiley

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