DNA vaccine for cancer immunotherapy.

Benjamin Yang, Jessica Jeang, Andrew Yang, T C Wu, Chien-Fu Hung
Author Information
  1. Benjamin Yang: a Department of Pathology ; Johns Hopkins University ; Baltimore , MD USA.

Abstract

DNA vaccination has emerged as an attractive immunotherapeutic approach against cancer due to its simplicity, stability, and safety. Results from numerous clinical trials have demonstrated that DNA vaccines are well tolerated by patients and do not trigger major adverse effects. DNA vaccines are also very cost effective and can be administered repeatedly for long-term protection. Despite all the practical advantages, DNA vaccines face challenges in inducing potent antigen specific cellular immune responses as a result of immune tolerance against endogenous self-antigens in tumors. Strategies to enhance immunogenicity of DNA vaccines against self-antigens have been investigated including encoding of xenogeneic versions of antigens, fusion of antigens to molecules that activate T cells or trigger associative recognition, priming with DNA vectors followed by boosting with viral vector, and utilization of immunomodulatory molecules. This review will focus on discussing strategies that circumvent immune tolerance and provide updates on findings from recent clinical trials.

Keywords

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Grants

  1. R43CA174436/NCI NIH HHS
  2. P50 CA098252/NCI NIH HHS
  3. P50 CA-DE019032/NCI NIH HHS
  4. 2R01CA114425-06/NCI NIH HHS
  5. P50CA098252,/NCI NIH HHS
  6. R01CA142691/NCI NIH HHS

MeSH Term

Animals
Antigens, Neoplasm
Cancer Vaccines
Dendritic Cells
Humans
Immunotherapy
Mice
Neoplasms
Tumor Escape
Vaccination
Vaccines, DNA

Chemicals

Antigens, Neoplasm
Cancer Vaccines
Vaccines, DNA

Word Cloud

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