Immunoproteasome down-modulation enhances the ability of dendritic cells to stimulate antitumor immunity

Author:

Dannull Jens1,Lesher Diem-Thu1,Holzknecht Robert2,Qi Wenning1,Hanna Gabi1,Seigler Hilliard12,Tyler Douglas S.12,Pruitt Scott K.12

Affiliation:

1. Department of Surgery, Duke University Medical Center, Durham; and

2. Department of Surgery, Durham Veterans Administration Medical Center, NC

Abstract

The process of dendritic cell (DC) maturation, critical for effective DC-based immunotherapy, also alters the proteasome such that peptides presented in the context of HLA class I are generated not by the constitutive proteasome, but by the immunoproteasome. Cytotoxic T lymphocytes (CTLs) induced by such DCs might not optimally recognize tumor cells normally expressing the constitutive proteasome. Using small interfering RNA (siRNA) transfection of DCs to inhibit expression of the 3 inducible immunoproteasome subunits in mature DCs, we found that such DCs expressed increased intracellular levels of constitutive proteasomes and presented an altered repertoire of tumor-antigenic peptides. When DCs generated from the monocytes of 3 patients with melanoma were transfected with immunoproteasome siRNA, induced to mature, and then trans-fected with RNA encoding defined melanoma antigens, these DCs were superior inducers of antigen-specific CTLs against autologous melanoma cells. This alteration of DC proteasome composition, which enhances the ability of mature antigen-loaded DCs to stimulate anti-tumor immune responses, may lead to more effective DC-based tumor immunotherapy.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

Reference28 articles.

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