In vitro cross-talk between metastasis-competent circulating tumor cells and platelets in colon cancer: a malicious association during the harsh journey in the blood

Zahra Eslami-S; Luis Enrique Cortés-Hernández; Ilias Glogovitis; Mafalda Antunes-Ferreira; Silvia D'Ambrosi; Keerthi Kurma; Françoise Garima; Laure Cayrefourcq; Myron G Best; Danijela Koppers-Lalic; Thomas Wurdinger; Catherine Alix-Panabières

doi:10.3389/fcell.2023.1209846

In vitro cross-talk between metastasis-competent circulating tumor cells and platelets in colon cancer: a malicious association during the harsh journey in the blood

Front Cell Dev Biol. 2023 Aug 2:11:1209846. doi: 10.3389/fcell.2023.1209846. eCollection 2023.

Authors

Zahra Eslami-S^{1

2

3}, Luis Enrique Cortés-Hernández^{1

2

3}, Ilias Glogovitis^{4

5

6}, Mafalda Antunes-Ferreira^{4

5

6}, Silvia D'Ambrosi^{4

5

6}, Keerthi Kurma^{1

2

3}, Françoise Garima^{1

2

3}, Laure Cayrefourcq^{1

2

3}, Myron G Best^{4

5

6}, Danijela Koppers-Lalic⁷, Thomas Wurdinger^{4

5

6}, Catherine Alix-Panabières^{1

2

3}

Affiliations

¹ Laboratory of Rare Circulating Human Cells-University Medical Center of Montpellier, Montpellier, France.
² CREEC/CANECEV, MIVEGEC (CREES), Université de Montpellier, Centre National de la Recherche Scientifique, Institut de Recherche pour le Développement, Montpellier, France.
³ European Liquid Biopsy Society (ELBS), Hamburg, Germany.
⁴ Department of Neurosurgery, Amsterdam University Medical Centers, Vrije Universiteit Amsterdam, Amsterdam, Netherlands.
⁵ Cancer Center Amsterdam, Amsterdam University Medical Centers, Vrije Universiteit Amsterdam, Amsterdam, Netherlands.
⁶ Brain Tumor Center Amsterdam, Amsterdam University Medical Centers, Vrije Universiteit Amsterdam, Amsterdam, Netherlands.
⁷ Mathematical Institute, Leiden University, Leiden, Netherlands.

Abstract

Background: Platelets are active players in hemostasis, coagulation and also tumorigenesis. The cross-talk between platelets and circulating tumor cells (CTCs) may have various pro-cancer effects, including promoting tumor growth, epithelial-mesenchymal transition (EMT), metastatic cell survival, adhesion, arrest and also pre-metastatic niche and metastasis formation. Interaction with CTCs might alter the platelet transcriptome. However, as CTCs are rare events, the cross-talk between CTCs and platelets is poorly understood. Here, we used our established colon CTC lines to investigate the colon CTC-platelet cross-talk in vitro and its impact on the behavior/phenotype of both cell types. Methods: We exposed platelets isolated from healthy donors to thrombin (positive control) or to conditioned medium from three CTC lines from one patient with colon cancer and then we monitored the morphological and protein expression changes by microscopy and flow cytometry. We then analyzed the transcriptome by RNA-sequencing of platelets indirectly (presence of a Transwell insert) co-cultured with the three CTC lines. We also quantified by reverse transcription-quantitative PCR the expression of genes related to EMT and cancer development in CTCs after direct co-culture (no Transwell insert) with platelets. Results: We observed morphological and transcriptomic changes in platelets upon exposure to CTC conditioned medium and indirect co-culture (secretome). Moreover, the expression levels of genes involved in EMT (p < 0.05) were decreased in CTCs co-cultured with platelets, but not of genes encoding mesenchymal markers (FN1 and SNAI2). The expression levels of genes involved in cancer invasiveness (MYC, VEGFB, IL33, PTGS2, and PTGER2) were increased. Conclusion: For the first time, we studied the CTC-platelet cross-talk using our unique colon CTC lines. Incubation with CTC conditioned medium led to platelet aggregation and activation, supporting the hypothesis that their interaction may contribute to preserve CTC integrity during their journey in the bloodstream. Moreover, co-culture with platelets influenced the expression of several genes involved in invasiveness and EMT maintenance in CTCs.

Keywords: cancer; circulating tumor cells (CTCs); epithelial-to-mesenchymal transition (EMT); metastasis; platelets; tumor-educated platelets (TEPs).

Grants and funding

ZE-S, LC-H, IG, MA-F, SD, DK-L, TW, and CA-P are supported by the ELBA project, which has received funding from the European Union Horizon 2020 Research and Innovation program under the Marie Skłodowska-Curie grant agreement No 765492. ZE-S and LC-H are also supported by SIRIC Montpellier. CA-P is also supported by the National Institute of Cancer (INCa, http://www.e-cancer.fr) INCa_Inserm_DGOS_12553, SIRIC Montpellier, and the ERA-NET TRANSCAN 2 JTC 2016 PROLIPSY, la Fondation ARC pour la Recherche sur le cancer and les Fonds de dotation AFER pour la recherche médicale.