Published 2024 | Version v1
Publication Metadata-only

Neutrophil-like Monocytes Increase in Patients with Colon Cancer and Induce Dysfunctional TIGIT+ NK Cells

Calabrò, Alessia
Drommi, Fabiana
Sidoti Migliore, Giacomo
Pezzino, Gaetana
Vento, Grazia
Freni, José
Costa, Gregorio
Cavaliere, Riccardo
Bonaccorsi, Irene
Sionne, Mariagrazia
Nigro, Stefania
Navarra, Giuseppe
Ferlazzo, Guido
De Pasquale, Claudia
Campana, Stefania
Others:
Calabrò, Alessia
Drommi, Fabiana
Sidoti Migliore, Giacomo
Pezzino, Gaetana
Vento, Grazia
Freni, José
Costa, Gregorio
Cavaliere, Riccardo
Bonaccorsi, Irene
Sionne, Mariagrazia
Nigro, Stefania
Navarra, Giuseppe
Ferlazzo, Guido
De Pasquale, Claudia
Campana, Stefania

Description

Myeloid-derived suppressor cells (MDSCs) are a heterogeneous family of immune cells including granulocytic (CD14neg/CD15+/HLA-DRneg) and monocytic subtypes (CD14+/CD15neg/HLA-DRneg). In the present study, we found a population of monocytes expressing the granulocyte marker CD15 that significantly increased in both peripheral blood (PB) and tumoral tissues of patients with colorectal cancer (CRC). Further phenotypical analysis confirmed the granulocytic-like features of this monocyte subpopulation that is associated with an increase in granulocyte-monocyte precursors (GMPs) in the PB of these patients (pts). Mechanistically, this granulocyte-like monocyte population suppressed NK cell activity by inducing TIGIT and engaging NKp30. Accordingly, an increased frequency of TIGIT+ NK cells with impaired functions was found in both the PB and tumoral tissue of CRC pts. Collectively, we provided new mechanistic explanations for tumor immune escape occurring in CRC by showing the increase in this new kind of MDSC, in both PB and CRC tissue, which is able to significantly impair the effector functions of NK cells, thereby representing a potential therapeutic target for cancer immunotherapy.

Additional details

Identifiers Origin repository
Created:
October 30, 2024
Modified:
October 30, 2024