Cellular immunity induced by a novel HPV18 DNA vaccine encoding an E6/E7 fusion consensus protein in mice and rhesus macaques

Yan, Jian; Harris, Kristina A.; Khan, Amir S.; Draghia-Akli, Ruxandra; Sewell, David L.; Weiner, David B.

doi:10.1016/j.vaccine.2008.03.069

Cited by 60 publications

(51 citation statements)

References 38 publications

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“…23,24 Prior studies examining the immunogenicity of novel DNA vaccines with E6/E7 consensus genes targeting HPV16 and HPV18 have shown much promise for future development into a vaccine for clinical use. 12,13 Ideally, clinical trials in humans would be used as the ultimate test to evaluate the vaccines' efficacy. However, various pre-clinical experiments using other models, including human MHC transgenic animals as well as non-human primates, may generate important data regarding the immune potency of these cassettes.…”

Section: Discussionmentioning

confidence: 99%

“…Numerous optimization, delivery and boost strategies have been developed and are currently being studied. 8,[12][13][14][15][16][17][18] Recent work on DNA vaccines for HPV therapy have produced promising preliminary results which have now led to clinical trials targeting the HPV 16 or 18 subtypes. [12][13][14][19][20][21][22] However, there have been no prior reports focusing on HPV subtypes 6 + 11.…”

Section: Induction Of Robust Cellular Immunity Againstmentioning

confidence: 99%

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Induction of robust cellular immunity against HPV6 and HPV11 in mice by DNA vaccine encoding for E6/E7 antigen

Shin

Pankhong

Yan

et al. 2012

Human Vaccines & Immunotherapeutics

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Section: Discussionmentioning

confidence: 99%

Section: Induction Of Robust Cellular Immunity Againstmentioning

confidence: 99%

Induction of robust cellular immunity against HPV6 and HPV11 in mice by DNA vaccine encoding for E6/E7 antigen

Shin

Pankhong

Yan

et al. 2012

Human Vaccines & Immunotherapeutics

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“…Dermal immunization methods target the epidermis, the dermis, or both, and include chemical modification, 38,39 transepidermal immunization, 40,41 gene gun technology, 31 electroporation 42,43 and intradermal injections. 42 Recently, intradermal administration with the RNA interference technique has also been reported.…”

Section: Discussionmentioning

confidence: 99%

Noncarrier naked antigen-specific DNA vaccine generates potent antigen-specific immunologic responses and antitumor effects

Sun

et al. 2009

Gene Ther

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Genetic immunization strategies have largely focused on the use of plasmid DNA with a gene gun. However, there remains a clear need to further improve the efficiency, safety, and cost of potential DNA vaccines. The gold particle-coated DNA format delivered through a gene gun is expensive, time and process consuming, and raises aseptic safety concerns. This study aims to determine whether a low-pressured gene gun can deliver noncarrier naked DNA vaccine without any particle coating, and generate similarly strong antigen-specific immunologic responses and potent antitumor effects compared with gold particle-coated DNA vaccine. Our results show that mice vaccinated with noncarrier naked chimeric CRT/E7 DNA lead to dramatic increases in the numbers of E7-specific CD8 + T-cell precursors and markedly raised titers of E7-specific antibodies. Furthermore, noncarrier naked CRT/E7 DNA vaccine generated potent antitumor effects against subcutaneous E7-expressing tumors and pre-established E7-expressing metastatic pulmonary tumors. In addition, mice immunized with noncarrier naked CRT/E7 DNA vaccine had significantly less burning effects on the skin compared with those vaccinated with gold particle-coated CRT/E7 DNA vaccine. We conclude that noncarrier naked CRT/E7 DNA vaccine delivered with a low-pressured gene gun can generate similarly potent immunologic responses and effective antitumor effects has fewer side effects, and is more convenient than conventional gold particle-coated DNA vaccine.

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“…Immunization induced a potent cellular immune response against both E6 and E7 proteins [107], and it was able to delay the growth of established HPV-tumors [108]. Another plasmid encoding E7-speciic CTL epitopes from HPV 16 and 18 and embedded in biodegradable micro particles (ZYC101a) was tested in a group of patients histologically conirmed CIN 2/3 neoplasia.…”

Section: Dna-based Vaccinesmentioning

confidence: 99%

Prophylactic and Therapeutic Vaccines against Human Papillomavirus Infections

Rosales¹,

Rosales²

2017

Vaccines

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Human papillomaviruses (HPVs) are a large family of double-strand DNA viruses comprising more than 180 types. Infection with HPV is associated with benign and malignant proliferation of skin and mucosae. Low-risk HPVs produce warts, whereas high-risk viruses induce tumors. Because there are no anti-viral drugs for HPV infection, there is a lot of interest in vaccines that can prevent the infection and also in vaccines that can be used to treat established infections and HPV-related tumors. Two prophylactic vaccines have been approved for preventing HPV infection. They seem to be efective when very young people are vaccinated. Unfortunately, many older people are still at risk of infection, mainly in countries where vaccination coverage is not eicient and for those people, novel therapeutic vaccines are being developed. This chapter describes the properties of HPV vaccines used today and the current status of several therapeutic vaccines been developed to treat HPV-induced lesions.

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Cellular immunity induced by a novel HPV18 DNA vaccine encoding an E6/E7 fusion consensus protein in mice and rhesus macaques

Cited by 60 publications

References 38 publications

Induction of robust cellular immunity against HPV6 and HPV11 in mice by DNA vaccine encoding for E6/E7 antigen

Induction of robust cellular immunity against HPV6 and HPV11 in mice by DNA vaccine encoding for E6/E7 antigen

Noncarrier naked antigen-specific DNA vaccine generates potent antigen-specific immunologic responses and antitumor effects

Prophylactic and Therapeutic Vaccines against Human Papillomavirus Infections

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