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DC-expressed MHC class I single-chain trimer-based vaccines prime cytotoxic T lymphocytes against exogenous but not endogenous antigens
Authors:Maria L Ordaz  Lonnie Lybarger
Institution:a Department of Immunobiology, The University of Arizona, Tucson, AZ 85724, United States
b Department of Pediatrics, The University of Arizona, Tucson, AZ 85724, United States
c Department of Cell Biology and Anatomy, The University of Arizona, Tucson, AZ 85724, United States
Abstract:The poor immunogenicity of many tumors can be partly explained by the inefficiency of the MHC class I peptide presentation pathway. MHC-I-based single-chain trimers (SCT) represent a new class of molecules with the potential to overcome this limitation. We here evaluated the ability of SCT presenting a melanoma antigen peptide (TRP-2) to prime cytotoxic T lymphocyte (CTL) responses in mice when given as DNA vaccines via Gene Gun or when expressed by dendritic cells. The SCT was unable to induce detectable priming or significant anti-tumor activity of CTL using either vaccination strategy, whereas control SCT (with an exogenous peptide) primed strong responses. This study thus provides the first data related to the use of SCT in combination with DC and their application toward self antigens and suggest this potent technology, alone, is insufficient to overcome self tolerance.
Keywords:Single-chain trimer  MHC-I  Melanoma  Dendritic cell  Gene Gun  Tyrosinase-related protein  Tumor antigen  B16
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