Cancer-on-a-chip model shows that the adenomatous polyposis coli mutation impairs T cell engagement and killing of cancer spheroids

Evaluating the ability of cytotoxic T lymphocytes (CTLs) to eliminate tumor cells is crucial, for instance, to predict the efficiency of cell therapy in personalized medicine. However, the destruction of a tumor by CTLs involves CTL migration in the extra-tumoral environment, accumulation on the tum...

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Veröffentlicht in:	Proceedings of the National Academy of Sciences - PNAS 2024-03, Vol.121 (11), p.e2316500121
Hauptverfasser:	Bonnet, Valentin, Maikranz, Erik, Madec, Marianne, Vertti-Quintero, Nadia, Cuche, Céline, Mastrogiovanni, Marta, Alcover, Andrés, Di Bartolo, Vincenzo, Baroud, Charles N
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Schlagworte:	Adenomatous Polyposis Coli Antigen-presenting cells Biological Sciences Cancer Cell therapy Cytometry Cytotoxicity Destruction Humans Lab-On-A-Chip Devices Leukocyte migration Life Sciences Lymphocytes Lymphocytes T Mutation Neoplasms - genetics Physical Sciences Polyposis coli Precision medicine Spheroids T-Lymphocytes, Cytotoxic Toxicity Tumor cells Tumors
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creator	Bonnet, Valentin Maikranz, Erik Madec, Marianne Vertti-Quintero, Nadia Cuche, Céline Mastrogiovanni, Marta Alcover, Andrés Di Bartolo, Vincenzo Baroud, Charles N
description	Evaluating the ability of cytotoxic T lymphocytes (CTLs) to eliminate tumor cells is crucial, for instance, to predict the efficiency of cell therapy in personalized medicine. However, the destruction of a tumor by CTLs involves CTL migration in the extra-tumoral environment, accumulation on the tumor, antigen recognition, and cooperation in killing the cancer cells. Therefore, identifying the limiting steps in this complex process requires spatio-temporal measurements of different cellular events over long periods. Here, we use a cancer-on-a-chip platform to evaluate the impact of adenomatous polyposis coli (APC) mutation on CTL migration and cytotoxicity against 3D tumor spheroids. The APC mutated CTLs are found to have a reduced ability to destroy tumor spheroids compared with control cells, even though APC mutants migrate in the extra-tumoral space and accumulate on the spheroids as efficiently as control cells. Once in contact with the tumor however, mutated CTLs display reduced engagement with the cancer cells, as measured by a metric that distinguishes different modes of CTL migration. Realigning the CTL trajectories around localized killing cascades reveals that all CTLs transition to high engagement in the 2 h preceding the cascades, which confirms that the low engagement is the cause of reduced cytotoxicity. Beyond the study of APC mutations, this platform offers a robust way to compare cytotoxic cell efficiency of even closely related cell types, by relying on a multiscale cytometry approach to disentangle complex interactions and to identify the steps that limit the tumor destruction.
doi_str_mv	10.1073/pnas.2316500121
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However, the destruction of a tumor by CTLs involves CTL migration in the extra-tumoral environment, accumulation on the tumor, antigen recognition, and cooperation in killing the cancer cells. Therefore, identifying the limiting steps in this complex process requires spatio-temporal measurements of different cellular events over long periods. Here, we use a cancer-on-a-chip platform to evaluate the impact of adenomatous polyposis coli (APC) mutation on CTL migration and cytotoxicity against 3D tumor spheroids. The APC mutated CTLs are found to have a reduced ability to destroy tumor spheroids compared with control cells, even though APC mutants migrate in the extra-tumoral space and accumulate on the spheroids as efficiently as control cells. Once in contact with the tumor however, mutated CTLs display reduced engagement with the cancer cells, as measured by a metric that distinguishes different modes of CTL migration. 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subjects	Adenomatous Polyposis Coli Antigen-presenting cells Biological Sciences Cancer Cell therapy Cytometry Cytotoxicity Destruction Humans Lab-On-A-Chip Devices Leukocyte migration Life Sciences Lymphocytes Lymphocytes T Mutation Neoplasms - genetics Physical Sciences Polyposis coli Precision medicine Spheroids T-Lymphocytes, Cytotoxic Toxicity Tumor cells Tumors
title	Cancer-on-a-chip model shows that the adenomatous polyposis coli mutation impairs T cell engagement and killing of cancer spheroids
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