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Electroporation as a "prime/boost" strategy for naked DNA vaccination against a tumor antigen

Authors: Buchan, S., Grønevik, E., Mathiesen, I., King, C.A., Stevenson, F.K. and Rice, J.

Journal: Journal of Immunology

Volume: 174

Issue: 10

Pages: 6292-6298

ISSN: 0022-1767

DOI: 10.4049/jimmunol.174.10.6292

Abstract:

We have developed novel DNA fusion vaccines encoding tumor Ags fused to pathogen-derived sequences. This strategy activates linked T cell help and, using fragment C of tetnus toxin, amplification of anti-tumor Ab, CD4 +, and CD8+ T cell responses is achievable in mice. However, there is concern that simple DNA vaccine injection may produce inadequate responses in larger humans. To overcome this, we tested electroporation as a method to increase the transfection efficiency and immune responses by these tumor vaccines in vivo in mice. Using a DNA vaccine expressing the CTL epitope AH1 from colon carcinoma CT26, we confirmed that effective priming and tumor protection in mice are highly dependent on vaccine dose and volume. However, suboptimal vaccination was rendered effective by electroporation, priming higher levels of AH1-specific CD8+ T cells able to protect mice from tumor growth. Electroporation during priming with our optimal vaccination protocol did not improve CD8+ T cell responses. In contrast, electroporation during boosting strikingly improved vaccine performance. The prime/boost strategy was also effective if electroporation was used at both priming and boosting. For Ab induction, DNA vaccination is generally less effective than protein. However, prime/boost with naked DNA followed by electroporation dramatically increased Ab levels. Thus, the priming qualities of DNA fusion vaccines, integrated with the improved Ag expression offered by electroporation, can be combined in a novel homologous prime/boost approach, to generate superior antitumor immune responses. Therefore, boosting may not require viral vectors, but simply a physical change in delivery, facilitating application to the cancer clinic. Copyright © 2005 by The American Association of Immunologists, Inc.

Source: Scopus

Electroporation as a "prime/boost" strategy for naked DNA vaccination against a tumor antigen.

Authors: Buchan, S., Grønevik, E., Mathiesen, I., King, C.A., Stevenson, F.K. and Rice, J.

Journal: J Immunol

Volume: 174

Issue: 10

Pages: 6292-6298

ISSN: 0022-1767

DOI: 10.4049/jimmunol.174.10.6292

Abstract:

We have developed novel DNA fusion vaccines encoding tumor Ags fused to pathogen-derived sequences. This strategy activates linked T cell help and, using fragment C of tetanus toxin, amplification of anti-tumor Ab, CD4(+), and CD8(+) T cell responses is achievable in mice. However, there is concern that simple DNA vaccine injection may produce inadequate responses in larger humans. To overcome this, we tested electroporation as a method to increase the transfection efficiency and immune responses by these tumor vaccines in vivo in mice. Using a DNA vaccine expressing the CTL epitope AH1 from colon carcinoma CT26, we confirmed that effective priming and tumor protection in mice are highly dependent on vaccine dose and volume. However, suboptimal vaccination was rendered effective by electroporation, priming higher levels of AH1-specific CD8(+) T cells able to protect mice from tumor growth. Electroporation during priming with our optimal vaccination protocol did not improve CD8(+) T cell responses. In contrast, electroporation during boosting strikingly improved vaccine performance. The prime/boost strategy was also effective if electroporation was used at both priming and boosting. For Ab induction, DNA vaccination is generally less effective than protein. However, prime/boost with naked DNA followed by electroporation dramatically increased Ab levels. Thus, the priming qualities of DNA fusion vaccines, integrated with the improved Ag expression offered by electroporation, can be combined in a novel homologous prime/boost approach, to generate superior antitumor immune responses. Therefore, boosting may not require viral vectors, but simply a physical change in delivery, facilitating application to the cancer clinic.

Source: PubMed

Electroporation as a "prime/boost" strategy for naked DNA vaccination against a tumor antigen

Authors: Buchan, S., Gronevik, E., Mathiesen, I., King, C.A., Stevenson, F.K. and Rice, J.

Journal: JOURNAL OF IMMUNOLOGY

Volume: 174

Issue: 10

Pages: 6292-6298

ISSN: 0022-1767

DOI: 10.4049/jimmunol.174.10.6292

Source: Web of Science (Lite)

Electroporation as a "prime/boost" strategy for naked DNA vaccination against a tumor antigen.

Authors: Buchan, S., Grønevik, E., Mathiesen, I., King, C.A., Stevenson, F.K. and Rice, J.

Journal: Journal of immunology (Baltimore, Md. : 1950)

Volume: 174

Issue: 10

Pages: 6292-6298

eISSN: 1550-6606

ISSN: 0022-1767

DOI: 10.4049/jimmunol.174.10.6292

Abstract:

We have developed novel DNA fusion vaccines encoding tumor Ags fused to pathogen-derived sequences. This strategy activates linked T cell help and, using fragment C of tetanus toxin, amplification of anti-tumor Ab, CD4(+), and CD8(+) T cell responses is achievable in mice. However, there is concern that simple DNA vaccine injection may produce inadequate responses in larger humans. To overcome this, we tested electroporation as a method to increase the transfection efficiency and immune responses by these tumor vaccines in vivo in mice. Using a DNA vaccine expressing the CTL epitope AH1 from colon carcinoma CT26, we confirmed that effective priming and tumor protection in mice are highly dependent on vaccine dose and volume. However, suboptimal vaccination was rendered effective by electroporation, priming higher levels of AH1-specific CD8(+) T cells able to protect mice from tumor growth. Electroporation during priming with our optimal vaccination protocol did not improve CD8(+) T cell responses. In contrast, electroporation during boosting strikingly improved vaccine performance. The prime/boost strategy was also effective if electroporation was used at both priming and boosting. For Ab induction, DNA vaccination is generally less effective than protein. However, prime/boost with naked DNA followed by electroporation dramatically increased Ab levels. Thus, the priming qualities of DNA fusion vaccines, integrated with the improved Ag expression offered by electroporation, can be combined in a novel homologous prime/boost approach, to generate superior antitumor immune responses. Therefore, boosting may not require viral vectors, but simply a physical change in delivery, facilitating application to the cancer clinic.

Source: Europe PubMed Central