1. Academic Validation
  2. Tumor therapy in mice via antigen targeting to a novel, DC-restricted C-type lectin

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

  • J Clin Invest. 2008 Jun;118(6):2098-110. doi: 10.1172/JCI34584.
David Sancho 1 Diego Mourão-Sá Olivier P Joffre Oliver Schulz Neil C Rogers Daniel J Pennington James R Carlyle Caetano Reis e Sousa
Affiliations

Affiliation

  • 1 Immunobiology Laboratory, Cancer Research UK, London Research Institute, London, United Kingdom.
Abstract

The mouse CD8alpha+ 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 CD8alpha+ 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 CD8alpha+ 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.

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