Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene

C. H. Chen; T. L. Wang; H. Ji; C. F. Hung; D. M. Pardoll; W. F. Cheng; M. Ling; T. C. Wu

doi:10.1038/sj.gt.3301370

Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene

C. H. Chen, T. L. Wang, H. Ji, C. F. Hung, D. M. Pardoll, W. F. Cheng, M. Ling, T. C. Wu

School of Medicine

Research output: Contribution to journal › Article › peer-review

21 Scopus citations

Abstract

Antigen-specific cancer immunotherapy involves the delivery of tumor-associated antigen to the host for the generation of tumor-specific immune responses and antitumor effects. We hypothesized that different delivery systems may influence the pattern of antigen-specific immune response and the outcome of antitumor effect. We therefore evaluated recombinant vaccinia virus and naked DNA for the generation of antigen-specific immune responses and antitumor effects. We previously found that recombinant vaccinia and naked DNA vaccines containing the chimeric Sig/E7/LAMP-1 gene were capable of controlling the growth of HPV-16 E7-expressing tumor cells (TC-1). In this study, we performed a head-to-head comparison of optimized delivery of Sig/E7/LAMP-1 vaccinia and DNA vaccines using dose-escalating tumor challenge. At a dose of 1 × 10⁶ TC-1 cells per mouse, Sig/E7/LAMP-1 DNA provided 100% protection against subcutaneous growth of tumors, while Vac-Sig/E7/LAMP-1 protected only 40% of the mice. Furthermore, Sig/E7/LAMP-1 DNA vaccines are capable of protecting against challenge with a more stringent subclone of TC-1 (TC-1 P2) established from TC-1 tumors that survived initial Sig/E7/LAMP-1 vaccinia vaccination. Immunological assays revealed that both vaccines induced comparable levels of CD8⁺ T cell precursors and anti-E7 antibody titers. Interestingly, Sig/E7/LAMP-1 vaccinia induced both E7-specific IFN-γ- and IL4-secreting CD4⁺ T cell precursors while Sig/E7/LAMP-1 DNA induced only E7-specific IFN-γ-secreting CD4⁺ T cell precursors. We also found that IL-4 knockout C57BL/6 mice vaccinated with Sig/E7/LAMP-1 vaccinia exhibited a more potent antitumor effect than vaccinated wild-type C57BL/6 mice in our tumor protection experiments. These results suggest that IL-4 may play a detrimental role in the antitumor effect mediated by vaccinia vaccines. Our findings suggested that DNA vaccines may provide better tumor protection than vaccinia vaccines employing the same gene, which may have implications in the future design of antigen-specific cancer immunotherapy.

Original language	English (US)
Pages (from-to)	128-138
Number of pages	11
Journal	Gene Therapy
Volume	8
Issue number	2
DOIs	https://doi.org/10.1038/sj.gt.3301370
State	Published - 2001

Keywords

Cancer vaccine
DNA vaccine
E7
HPV-16
Vaccinia vaccine

ASJC Scopus subject areas

Molecular Medicine
Molecular Biology
Genetics

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10.1038/sj.gt.3301370

Cite this

@article{042d3a36f58249b680e8843f61050099,

title = "Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene",

abstract = "Antigen-specific cancer immunotherapy involves the delivery of tumor-associated antigen to the host for the generation of tumor-specific immune responses and antitumor effects. We hypothesized that different delivery systems may influence the pattern of antigen-specific immune response and the outcome of antitumor effect. We therefore evaluated recombinant vaccinia virus and naked DNA for the generation of antigen-specific immune responses and antitumor effects. We previously found that recombinant vaccinia and naked DNA vaccines containing the chimeric Sig/E7/LAMP-1 gene were capable of controlling the growth of HPV-16 E7-expressing tumor cells (TC-1). In this study, we performed a head-to-head comparison of optimized delivery of Sig/E7/LAMP-1 vaccinia and DNA vaccines using dose-escalating tumor challenge. At a dose of 1 × 106 TC-1 cells per mouse, Sig/E7/LAMP-1 DNA provided 100% protection against subcutaneous growth of tumors, while Vac-Sig/E7/LAMP-1 protected only 40% of the mice. Furthermore, Sig/E7/LAMP-1 DNA vaccines are capable of protecting against challenge with a more stringent subclone of TC-1 (TC-1 P2) established from TC-1 tumors that survived initial Sig/E7/LAMP-1 vaccinia vaccination. Immunological assays revealed that both vaccines induced comparable levels of CD8+ T cell precursors and anti-E7 antibody titers. Interestingly, Sig/E7/LAMP-1 vaccinia induced both E7-specific IFN-γ- and IL4-secreting CD4+ T cell precursors while Sig/E7/LAMP-1 DNA induced only E7-specific IFN-γ-secreting CD4+ T cell precursors. We also found that IL-4 knockout C57BL/6 mice vaccinated with Sig/E7/LAMP-1 vaccinia exhibited a more potent antitumor effect than vaccinated wild-type C57BL/6 mice in our tumor protection experiments. These results suggest that IL-4 may play a detrimental role in the antitumor effect mediated by vaccinia vaccines. Our findings suggested that DNA vaccines may provide better tumor protection than vaccinia vaccines employing the same gene, which may have implications in the future design of antigen-specific cancer immunotherapy.",

keywords = "Cancer vaccine, DNA vaccine, E7, HPV-16, Vaccinia vaccine",

author = "Chen, {C. H.} and Wang, {T. L.} and H. Ji and Hung, {C. F.} and Pardoll, {D. M.} and Cheng, {W. F.} and M. Ling and Wu, {T. C.}",

note = "Funding Information: We would like to thank Drs Richard Roden and Robert J Kurman for helpful discussions. We thank Dr Ephraim Fuchs for providing C57BL/6 IL-4 knockout mice. We would also like to thank Howard Jen for superb technical assistance. This work was supported by NIH 5 po1 34582–01, U19 CA72108–02, RO1 CA72631–01, the Cancer Research Institute and the Richard W TeLinde endowment.",

year = "2001",

doi = "10.1038/sj.gt.3301370",

language = "English (US)",

volume = "8",

pages = "128--138",

journal = "Gene Therapy",

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publisher = "Nature Publishing Group",

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T1 - Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene

AU - Chen, C. H.

AU - Wang, T. L.

AU - Ji, H.

AU - Hung, C. F.

AU - Pardoll, D. M.

AU - Cheng, W. F.

AU - Ling, M.

AU - Wu, T. C.

N1 - Funding Information: We would like to thank Drs Richard Roden and Robert J Kurman for helpful discussions. We thank Dr Ephraim Fuchs for providing C57BL/6 IL-4 knockout mice. We would also like to thank Howard Jen for superb technical assistance. This work was supported by NIH 5 po1 34582–01, U19 CA72108–02, RO1 CA72631–01, the Cancer Research Institute and the Richard W TeLinde endowment.

PY - 2001

Y1 - 2001

N2 - Antigen-specific cancer immunotherapy involves the delivery of tumor-associated antigen to the host for the generation of tumor-specific immune responses and antitumor effects. We hypothesized that different delivery systems may influence the pattern of antigen-specific immune response and the outcome of antitumor effect. We therefore evaluated recombinant vaccinia virus and naked DNA for the generation of antigen-specific immune responses and antitumor effects. We previously found that recombinant vaccinia and naked DNA vaccines containing the chimeric Sig/E7/LAMP-1 gene were capable of controlling the growth of HPV-16 E7-expressing tumor cells (TC-1). In this study, we performed a head-to-head comparison of optimized delivery of Sig/E7/LAMP-1 vaccinia and DNA vaccines using dose-escalating tumor challenge. At a dose of 1 × 106 TC-1 cells per mouse, Sig/E7/LAMP-1 DNA provided 100% protection against subcutaneous growth of tumors, while Vac-Sig/E7/LAMP-1 protected only 40% of the mice. Furthermore, Sig/E7/LAMP-1 DNA vaccines are capable of protecting against challenge with a more stringent subclone of TC-1 (TC-1 P2) established from TC-1 tumors that survived initial Sig/E7/LAMP-1 vaccinia vaccination. Immunological assays revealed that both vaccines induced comparable levels of CD8+ T cell precursors and anti-E7 antibody titers. Interestingly, Sig/E7/LAMP-1 vaccinia induced both E7-specific IFN-γ- and IL4-secreting CD4+ T cell precursors while Sig/E7/LAMP-1 DNA induced only E7-specific IFN-γ-secreting CD4+ T cell precursors. We also found that IL-4 knockout C57BL/6 mice vaccinated with Sig/E7/LAMP-1 vaccinia exhibited a more potent antitumor effect than vaccinated wild-type C57BL/6 mice in our tumor protection experiments. These results suggest that IL-4 may play a detrimental role in the antitumor effect mediated by vaccinia vaccines. Our findings suggested that DNA vaccines may provide better tumor protection than vaccinia vaccines employing the same gene, which may have implications in the future design of antigen-specific cancer immunotherapy.

AB - Antigen-specific cancer immunotherapy involves the delivery of tumor-associated antigen to the host for the generation of tumor-specific immune responses and antitumor effects. We hypothesized that different delivery systems may influence the pattern of antigen-specific immune response and the outcome of antitumor effect. We therefore evaluated recombinant vaccinia virus and naked DNA for the generation of antigen-specific immune responses and antitumor effects. We previously found that recombinant vaccinia and naked DNA vaccines containing the chimeric Sig/E7/LAMP-1 gene were capable of controlling the growth of HPV-16 E7-expressing tumor cells (TC-1). In this study, we performed a head-to-head comparison of optimized delivery of Sig/E7/LAMP-1 vaccinia and DNA vaccines using dose-escalating tumor challenge. At a dose of 1 × 106 TC-1 cells per mouse, Sig/E7/LAMP-1 DNA provided 100% protection against subcutaneous growth of tumors, while Vac-Sig/E7/LAMP-1 protected only 40% of the mice. Furthermore, Sig/E7/LAMP-1 DNA vaccines are capable of protecting against challenge with a more stringent subclone of TC-1 (TC-1 P2) established from TC-1 tumors that survived initial Sig/E7/LAMP-1 vaccinia vaccination. Immunological assays revealed that both vaccines induced comparable levels of CD8+ T cell precursors and anti-E7 antibody titers. Interestingly, Sig/E7/LAMP-1 vaccinia induced both E7-specific IFN-γ- and IL4-secreting CD4+ T cell precursors while Sig/E7/LAMP-1 DNA induced only E7-specific IFN-γ-secreting CD4+ T cell precursors. We also found that IL-4 knockout C57BL/6 mice vaccinated with Sig/E7/LAMP-1 vaccinia exhibited a more potent antitumor effect than vaccinated wild-type C57BL/6 mice in our tumor protection experiments. These results suggest that IL-4 may play a detrimental role in the antitumor effect mediated by vaccinia vaccines. Our findings suggested that DNA vaccines may provide better tumor protection than vaccinia vaccines employing the same gene, which may have implications in the future design of antigen-specific cancer immunotherapy.

KW - Cancer vaccine

KW - DNA vaccine

KW - E7

KW - HPV-16

KW - Vaccinia vaccine

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Recombinant DNA vaccines protect against tumors that are resistant to recombinant vaccinia vaccines containing the same gene

Abstract

Keywords

ASJC Scopus subject areas

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