Despite recent progress in cancer treatment, liver metastases persist as an unmet clinical need. Here, we show that arming liver and tumor-associated macrophages in vivo to co-express tumor antigens (TAs), IFNα, and IL-12 unleashes robust anti-tumor immune responses, leading to the regression of liver metastases. Mechanistically, in vivo armed macrophages expand tumor reactive CD8+ T cells, which acquire features of progenitor exhausted T cells and kill cancer cells independently of CD4+ T cell help. IFNα and IL-12 produced by armed macrophages reprogram antigen presenting cells and rewire cellular interactions, rescuing tumor reactive T cell functions. In vivo armed macrophages trigger anti-tumor immunity in distinct liver metastasis mouse models of colorectal cancer and melanoma, expressing either surrogate tumor antigens, naturally occurring neoantigens or tumor-associated antigens. Altogether, our findings support the translational potential of in vivo armed liver macrophages to expand and rejuvenate tumor reactive T cells for the treatment of liver metastases.
In vivo armed macrophages curb liver metastasis through tumor-reactive T-cell rejuvenation / Notaro, Marco; Borghetti, Maristella; Bresesti, Chiara; Giacca, Giovanna; Kerzel, Thomas; Mercado, Carl Mirko; Beretta, Stefano; Monti, Marco; Merelli, Ivan; Iaia, Silvia; Genua, Marco; Annoni, Andrea; Canu, Tamara; Cristofori, Patrizia; Degl'Innocenti, Sara; Sanvito, Francesca; Rancoita, Paola Maria Vittoria; Ostuni, Renato; Gregori, Silvia; Naldini, Luigi; Squadrito, Mario Leonardo. - In: NATURE COMMUNICATIONS. - ISSN 2041-1723. - 16:1(2025). [10.1038/s41467-025-58369-2]
In vivo armed macrophages curb liver metastasis through tumor-reactive T-cell rejuvenation
Notaro, Marco;Bresesti, Chiara;Giacca, Giovanna;Kerzel, Thomas;Beretta, Stefano;Rancoita, Paola Maria Vittoria;Ostuni, Renato;Naldini, Luigi;
2025-01-01
Abstract
Despite recent progress in cancer treatment, liver metastases persist as an unmet clinical need. Here, we show that arming liver and tumor-associated macrophages in vivo to co-express tumor antigens (TAs), IFNα, and IL-12 unleashes robust anti-tumor immune responses, leading to the regression of liver metastases. Mechanistically, in vivo armed macrophages expand tumor reactive CD8+ T cells, which acquire features of progenitor exhausted T cells and kill cancer cells independently of CD4+ T cell help. IFNα and IL-12 produced by armed macrophages reprogram antigen presenting cells and rewire cellular interactions, rescuing tumor reactive T cell functions. In vivo armed macrophages trigger anti-tumor immunity in distinct liver metastasis mouse models of colorectal cancer and melanoma, expressing either surrogate tumor antigens, naturally occurring neoantigens or tumor-associated antigens. Altogether, our findings support the translational potential of in vivo armed liver macrophages to expand and rejuvenate tumor reactive T cells for the treatment of liver metastases.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
