The Macrophage Galactose-Type C-Type Lectin (MGL) Modulates Regulatory T Cell Functions

巨噬细胞半乳糖型 C 型凝集素 (MGL) 调节调节性 T 细胞功能

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作者:Ilaria Grazia Zizzari, Paola Martufi, Federico Battisti, Hassan Rahimi, Salvatore Caponnetto, Filippo Bellati, Marianna Nuti, Aurelia Rughetti, Chiara Napoletano

Abstract

Regulatory T cells (Tregs) are physiologically designed to prevent autoimmune disease and maintain self-tolerance. In tumour microenvironments, their presence is related to a poor prognosis, and they influence the therapeutic outcome due to their capacity to suppress the immune response by cell-cell contact and to release immunosuppressive cytokines. In this study, we demonstrate that Treg immunosuppressive activity can be modulated by the cross-linking between the CD45RA expressed by Tregs and the C-type lectin MGL. This specific interaction strongly decreases the immunosuppressive activity of Tregs, restoring the proliferative capacity of co-cultured T lymphocytes. This effect can be attributed to changes in CD45RA and TCR signalling through the inhibition of Lck and inactivation of Zap-70, an increase in the Foxp3 methylation status and, ultimately, the reduced production of suppressive cytokines. These results indicate a role of MGL as an immunomodulator within the tumour microenvironment interfering with Treg functions, suggesting its possible use in the design of anticancer vaccines.

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