T cell migration and effector function differences in familial adenomatous polyposis patients with APC gene mutations

Céline Cuche; Marta Mastrogiovanni; Marie Juzans; Hélène Laude; Marie-Noëlle Ungeheuer; Daniel Krentzel; Maria Isabella Gariboldi; Daniel Scott-Algara; Marianne Madec; Sophie Goyard; Camille Floch; Gaëlle Chauveau-Le Friec; Pierre Lafaye; Charlotte Renaudat; Muriel Le Bidan; Christine Micallef; Sandrine Schmutz; Sébastien Mella; Sophie Novault; Milena Hasan; Darragh Duffy; Vincenzo Di Bartolo; Andrés Alcover

doi:10.3389/fimmu.2023.1163466

T cell migration and effector function differences in familial adenomatous polyposis patients with APC gene mutations

Front Immunol. 2023 Jul 18:14:1163466. doi: 10.3389/fimmu.2023.1163466. eCollection 2023.

Authors

Céline Cuche¹, Marta Mastrogiovanni^{1

2}, Marie Juzans^{1

2}, Hélène Laude³, Marie-Noëlle Ungeheuer³, Daniel Krentzel⁴, Maria Isabella Gariboldi⁴, Daniel Scott-Algara¹, Marianne Madec¹, Sophie Goyard^{1

5}, Camille Floch^{1

5}, Gaëlle Chauveau-Le Friec⁶, Pierre Lafaye⁶, Charlotte Renaudat³, Muriel Le Bidan⁷, Christine Micallef⁷, Sandrine Schmutz⁸, Sébastien Mella^{8

9}, Sophie Novault⁸, Milena Hasan⁸, Darragh Duffy¹⁰, Vincenzo Di Bartolo¹, Andrés Alcover¹

Affiliations

¹ Institut Pasteur, Université Paris Cité, INSERM-U1224, Unité Biologie Cellulaire des Lymphocytes, Ligue Nationale Contre le Cancer-Équipe Labellisée Ligue 2018, Paris, France.
² Sorbonne Université, Collège Doctoral, Paris, France.
³ Institut Pasteur, Université Paris Cité, ICAReB-Clin, Paris, France.
⁴ Institut Pasteur, Université Paris Cité, CNRS-UMR3691, Unité Imagerie et Modélisation, Paris, France.
⁵ Institut Pasteur, Université Paris Cité, Plateforme d'Innovation et de Développement de Tests Diagnostiques, Paris, France.
⁶ Institut Pasteur, Université Paris Cité, CNRS-UMR3528, Plateforme d'Ingénierie des Anticorps, Paris, France.
⁷ Association Polyposes Familiales France, Linas, France.
⁸ Institut Pasteur, Université Paris Cité, Unité de Technologie et Service Cytométrie et Biomarqueurs, Paris, France.
⁹ Institut Pasteur, Université Paris Cité, Hub Bioinformatique et Biostatistique, Paris, France.
¹⁰ Institut Pasteur, Université Paris Cité, Unité Immunologie Translationnelle, Paris, France.

Abstract

Familial adenomatous polyposis (FAP) is an inherited disease characterized by the development of large number of colorectal adenomas with high risk of evolving into colorectal tumors. Mutations of the Adenomatous polyposis coli (APC) gene is often at the origin of this disease, as well as of a high percentage of spontaneous colorectal tumors. APC is therefore considered a tumor suppressor gene. While the role of APC in intestinal epithelium homeostasis is well characterized, its importance in immune responses remains ill defined. Our recent work indicates that the APC protein is involved in various phases of both CD4 and CD8 T cells responses. This prompted us to investigate an array of immune cell features in FAP subjects carrying APC mutations. A group of 12 FAP subjects and age and sex-matched healthy controls were studied. We characterized the immune cell repertoire in peripheral blood and the capacity of immune cells to respond ex vivo to different stimuli either in whole blood or in purified T cells. A variety of experimental approaches were used, including, pultiparamater flow cytometry, NanosString gene expression profiling, Multiplex and regular ELISA, confocal microscopy and computer-based image analyis methods. We found that the percentage of several T and natural killer (NK) cell populations, the expression of several genes induced upon innate or adaptive immune stimulation and the production of several cytokines and chemokines was different. Moreover, the capacity of T cells to migrate in response to chemokine was consistently altered. Finally, immunological synapses between FAP cytotoxic T cells and tumor target cells were more poorly structured. Our findings of this pilot study suggest that mild but multiple immune cell dysfunctions, together with intestinal epithelial dysplasia in FAP subjects, may facilitate the long-term polyposis and colorectal tumor development. Although at an initial discovery phase due to the limited sample size of this rare disease cohort, our findings open new perspectives to consider immune cell abnormalities into polyposis pathology.

Keywords: APC; Adenomatous polyposis coli; T cell activation; T cell migration; cytokines; cytoskeleton; familial adenomatous polyposis; immunological synapse.

Copyright © 2023 Cuche, Mastrogiovanni, Juzans, Laude, Ungeheuer, Krentzel, Gariboldi, Scott-Algara, Madec, Goyard, Floch, Chauveau-Le Friec, Lafaye, Renaudat, Le Bidan, Micallef, Schmutz, Mella, Novault, Hasan, Duffy, Di Bartolo and Alcover.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenomatous Polyposis Coli* / genetics
Adenomatous Polyposis Coli* / pathology
Cell Movement / genetics
Colorectal Neoplasms* / genetics
Genes, APC
Humans
Mutation
Pilot Projects
T-Lymphocytes* / immunology

Grants and funding

This work was supported by grants from La Ligue Contre le Cancer-Equipe Labellisée Ligue 2018 and institutional grants from Institut Pasteur and INSERM. MMas was a scholar of the Pasteur Paris University International Doctoral Program and was supported by the Institut Pasteur, the European Union Horizon 2020 Research and Innovation Programme under the Marie Sklodowska-Curie grant agreement 665807 (COFUND-PASTEURDOC) and La Ligue Contre Le Cancer-Allocation doctorale 4ème année de thèse. MJ was supported by La Ligue Contre le Cancer-Allocation doctorale and the Institut Pasteur. MMad and CF were supported by Cancer Initiative Master Fellowships from the Institut Pasteur. DK is a scholar of the Pasteur Paris University International Doctoral Program supported by the Institut Pasteur. MIG is supported by a grant from Agence National de Recherche (ANR) TRANSFACT (ANR-19-CE12-0007-02).