Immunotherapy advances have been hindered by difficulties in tracking the behaviors of lymphocytes after antigen signaling. Here, we assessed the behavior of T cells active within tumors through the development of the antigen receptor signaling reporter (AgRSR) mouse, fate-mapping lymphocytes responding to antigens at specific times and locations. Contrary to reports describing the ready egress of T cells out of the tumor, we find that intratumoral antigen signaling traps CD8+ T cells in the tumor. These clonal populations expand and become increasingly exhausted over time. By contrast, antigen-signaled regulatory T cell (Treg) clonal populations readily recirculate out of the tumor. Consequently, intratumoral antigen signaling acts as a gatekeeper to compartmentalize CD8+ T cell responses, even within the same clonotype, thus enabling exhausted T cells to remain confined to a specific tumor tissue site.
Intratumoral antigen signaling traps CD8+ T cells to confine exhaustion to the tumor site / Takahashi, M.; So, T. Y.; Chamberlain-Evans, V.; Hughes, R.; Yam-Puc, J. C.; Kania, K.; Ruhle, M.; Mann, T.; Schuijs, M. J.; Coupland, P.; Naisbitt, D.; Halim, T. Y. F.; Lyons, P. A.; Lio, P.; Roychoudhuri, R.; Okkenhaug, K.; Adams, D. J.; Smith, K. G. C.; Jodrell, D. I.; Chapman, M. A.; Thaventhiran, J. E. D.. - In: SCIENCE IMMUNOLOGY. - ISSN 2470-9468. - 9:95(2024). [10.1126/sciimmunol.ade2094]
Intratumoral antigen signaling traps CD8+ T cells to confine exhaustion to the tumor site
Lio P.;
2024
Abstract
Immunotherapy advances have been hindered by difficulties in tracking the behaviors of lymphocytes after antigen signaling. Here, we assessed the behavior of T cells active within tumors through the development of the antigen receptor signaling reporter (AgRSR) mouse, fate-mapping lymphocytes responding to antigens at specific times and locations. Contrary to reports describing the ready egress of T cells out of the tumor, we find that intratumoral antigen signaling traps CD8+ T cells in the tumor. These clonal populations expand and become increasingly exhausted over time. By contrast, antigen-signaled regulatory T cell (Treg) clonal populations readily recirculate out of the tumor. Consequently, intratumoral antigen signaling acts as a gatekeeper to compartmentalize CD8+ T cell responses, even within the same clonotype, thus enabling exhausted T cells to remain confined to a specific tumor tissue site.File | Dimensione | Formato | |
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