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CD40 agonists alter tumor stroma and show efficacy against pancreatic carcinoma in mice and humans
Authors:Beatty Gregory L  Chiorean Elena G  Fishman Matthew P  Saboury Babak  Teitelbaum Ursina R  Sun Weijing  Huhn Richard D  Song Wenru  Li Dongguang  Sharp Leslie L  Torigian Drew A  O'Dwyer Peter J  Vonderheide Robert H
Institution:Abramson Family Cancer Research Institute, University of Pennsylvania School of Medicine, 421 Curie Boulevard, Philadelphia, PA 19104, USA.
Abstract:Immunosuppressive tumor microenvironments can restrain antitumor immunity, particularly in pancreatic ductal adenocarcinoma (PDA). Because CD40 activation can reverse immune suppression and drive antitumor T cell responses, we tested the combination of an agonist CD40 antibody with gemcitabine chemotherapy in a small cohort of patients with surgically incurable PDA and observed tumor regressions in some patients. We reproduced this treatment effect in a genetically engineered mouse model of PDA and found unexpectedly that tumor regression required macrophages but not T cells or gemcitabine. CD40-activated macrophages rapidly infiltrated tumors, became tumoricidal, and facilitated the depletion of tumor stroma. Thus, cancer immune surveillance does not necessarily depend on therapy-induced T cells; rather, our findings demonstrate a CD40-dependent mechanism for targeting tumor stroma in the treatment of cancer.
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