Tumor therapy in mice via antigen targeting to a novel, DC-restricted C-type lectin
David Sancho, Diego Mourão-Sá, Olivier P. Joffre, Oliver Schulz, Neil C. Rogers, Daniel J. Pennington, James R. Carlyle, Caetano Reis e Sousa
David Sancho, Diego Mourão-Sá, Olivier P. Joffre, Oliver Schulz, Neil C. Rogers, Daniel J. Pennington, James R. Carlyle, Caetano Reis e Sousa
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Research Article Immunology

Tumor therapy in mice via antigen targeting to a novel, DC-restricted C-type lectin

Abstract

The mouse CD8α+ DC subset excels at cross-presentation of antigen, which can elicit robust CTL responses. A receptor allowing specific antigen targeting to this subset and its equivalent in humans would therefore be useful for the induction of antitumor CTLs. Here, we have characterized a C-type lectin of the NK cell receptor group that we named DC, NK lectin group receptor-1 (DNGR-1). DNGR-1 was found to be expressed in mice at high levels by CD8+ DCs and at low levels by plasmacytoid DCs but not by other hematopoietic cells. Human DNGR-1 was also restricted in expression to a small subset of blood DCs that bear similarities to mouse CD8α+ DCs. The selective expression pattern and observed endocytic activity of DNGR-1 suggested that it could be used for antigen targeting to DCs. Consistent with this notion, antigen epitopes covalently coupled to an antibody specific for mouse DNGR-1 were selectively cross-presented by CD8α+ DCs in vivo and, when given with adjuvants, induced potent CTL responses. When the antigens corresponded to tumor-expressed peptides, treatment with the antibody conjugate and adjuvant could prevent development or mediate eradication of B16 melanoma lung pseudometastases. We conclude that DNGR-1 is a novel, highly specific marker of mouse and human DC subsets that can be exploited for CTL cross-priming and tumor therapy.

Authors

David Sancho, Diego Mourão-Sá, Olivier P. Joffre, Oliver Schulz, Neil C. Rogers, Daniel J. Pennington, James R. Carlyle, Caetano Reis e Sousa

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Figure 7

Anti–DNGR-1–S1 plus anti-CD40 is effective in prevention and therapy of OVA-expressing B16 melanoma.

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Anti–DNGR-1–S1 plus anti-CD40 is effective in prevention and therapy of ...
(A) Tumor prevention experiments were carried out as depicted. Data represent lung tumor counts in each mouse in 1 experiment out of 2 (n = 6 mice/group). (B) Tumor therapy experiments were carried out as depicted. Lower left panel shows representative photographs of lungs from mice treated as indicated. Right panel shows quantification of tumors in each mouse in 1 representative experiment out of 3 (n = 6 mice/group). (C) SIINFEKL-H2Kb tetramer-positive cells in spleens from mice depicted in B. Left panels show representative histograms of gated CD8+Thy1.2+ splenocytes. Right panel shows frequency of tetramer-positive CD8+ T cells in 1 representative experiment out of 3 (n = 6 mice/group). (D) Left panel shows splenocytes from individual mice depicted in B restimulated in vitro with SIINFEKL peptide (1 μM). IFN-γ levels after 5 days of culture are indicated for 1 representative experiment out of 3 (n = 6 mice/group). Right panel shows CTL activity after restimulation measured as in Figure 6C. One experiment (n = 6 mice/group, restimulated individually) out of 3 is shown. Data are the average ± SEM of all cultures. P values were calculated using Student’s t test.