Stable Immune Response Induced by Intradermal DNA Vaccination by a Novel Needleless Pyro-Drive Jet Injector

Chang, Chinyang; Sun, Jiao; Hayashi, Hiroki; Suzuki, Atsushi; Sakaguchi, Yuko; Miyazaki, Hiroshi; Nishikawa, Takashige; Nakagami, Hironori; Yamashita, Kazuo; Kaneda, Yasufumi

doi:10.1208/s12249-019-1564-z

Cited by 30 publications

(40 citation statements)

References 34 publications

(28 reference statements)

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“…A range of other devices have been developed and trialled in recent years. For instance, Genetronics Inc (San Diego, CA, USA) patented an injector pen, which uses a spring mechanism to apply needle-free intradermal injection of a liquid [ 176 ]. The Injex30 provided comparable antibody titres to subcutaneous N&S injection in a study with mice vaccinated against hepatitis B surface antigen [ 163 ].…”

Section: Vaccination Into the Dermal Compartment Without Needle Anmentioning

confidence: 99%

Vaccination into the Dermal Compartment: Techniques, Challenges, and Prospects

Hettinga

Carlisle

2020

Vaccines

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In 2019, an ‘influenza pandemic’ and ‘vaccine hesitancy’ were listed as two of the top 10 challenges to global health by the WHO. The skin is a unique vaccination site, due to its immune-rich milieu, which is evolutionarily primed to respond to challenge, and its ability to induce both humoral and cellular immunity. Vaccination into this dermal compartment offers a way of addressing both of the challenges presented by the WHO, as well as opening up avenues for novel vaccine formulation and dose-sparing strategies to enter the clinic. This review will provide an overview of the diverse range of vaccination techniques available to target the dermal compartment, as well as their current state, challenges, and prospects, and touch upon the formulations that have been developed to maximally benefit from these new techniques. These include needle and syringe techniques, microneedles, DNA tattooing, jet and ballistic delivery, and skin permeabilization techniques, including thermal ablation, chemical enhancers, ablation, electroporation, iontophoresis, and sonophoresis.

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Section: Vaccination Into the Dermal Compartment Without Needle Anmentioning

confidence: 99%

Vaccination into the Dermal Compartment: Techniques, Challenges, and Prospects

Hettinga

Carlisle

2020

Vaccines

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“…Our previous studies have shown that the novel jet injector driven by explosives, called pyro-drive jet injector, was efficient for ID administration in rats and mice, leading to efficient expression of transgenes. 8 However, the immune response and the significance of pyro-drive jet injections following DNA vaccination in large animals seem to be unclear, as jet injectors adjusted for ID administration have not been used in the previous studies. In the present study, we evaluated the application of jet injection for gene transfer via ID injection compared with that of needle syringes, using pig skin as a morphological model that mimics human skin in a translational research.…”

Section: Discussionmentioning

confidence: 99%

“…6,7 The injection was efficient in promoting gene transfer, antigen expression, and immune responses in mouse and rat models. [5][6][7][8] However, although the studies using jet injection with small animals are promising, similar results are not always obtained in humans.…”

Section: Introductionmentioning

confidence: 99%

Potent Intradermal Gene Expression of Naked Plasmid DNA in Pig Skin Following Pyro-drive Jet Injection

Miyazaki

Sakaguchi

Terai

2021

Journal of Pharmaceutical Sciences

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Intradermal administration of naked DNA with a conventional needle syringe is a simple and inexpensive method to expose an encoded antigen to the dermal immune system. We aimed to enhance intradermal gene expression with a pyro-drive jet injector using pig skin, which is similar in structure and biomechanical properties to human skin. When Cy3-labeled plasmid (pCy3) was applied to pig skin with the jet injector, pCy3 was distributed preferentially in the intradermal tissue. Precise localization analysis revealed that pCy3 was also detected in the intracellular nucleus, and the frequency was substantially higher with the jet injector than with a needle syringe. When a luciferase expression plasmid (pLuc) was injected transdermally, the luciferase activity was 380-fold higher with the jet injector than with a needle syringe. Furthermore, immunohistochemistry analysis showed that the epidermis was positive for luciferase protein expression. These data indicate that the jet injector facilitates stable intradermal administration, resulting in more efficient gene expression compared to that with conventional syringe methods. Thus, intradermal administration of an antigen-expression plasmid with the pyro-drive jet injector may provide a clinically viable method for future gene therapy.

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“…While publicly available information on the antigen and adjuvant is unavailable, it is evident that they are employing plasmid DNA delivered by a pyro-drive jet injector (PJI), which employs the detonation of small amounts of explosive powder to propel plasmids in a jet into the skin at variable, controllable depths [ 119 ]. In a preclinical evaluation of this technology to vaccinate against the model antigen ovalbumin in mice and rats, they demonstrated that plasmid DNA delivered by PJI induced significantly greater antigen expression and resultant antibody titers compared to needle-injected plasmid DNA [ 120 ]. This technology presents the advantage of needle-free, single step delivery with the potential to optimize the depth of delivery to induce the optimal immune response.…”

Section: Subunit Formulationsmentioning

confidence: 99%

“…Curevac has announced that they will begin Phase 1/2a clinical trials in June of 2020 for a SARS-CoV-2 vaccine, with this vaccine utilizing the same lipid formulation as Pfizer/BioNtech with mRNA encoding S protein of the virus [ 58 , 143 , 144 ]. This change from a protamine based carrier to a lipid based particle may be due to the fact that LNPs are shown to work better when given via standard intramuscular injection [ 145 ], whereas the protamine based formulation only induced neutralizing titers when administered with less common needle-free injection mechanisms similar to those used in previous studies of DNA vaccination [ 58 , 120 ]. Another consideration might be the enhanced storage they announced with their new LNP formulation, noting that they have a formulation suitable for storage at three months at standard refrigeration temperature (5 °C) [ 146 ].…”

Section: Subunit Formulationsmentioning

confidence: 99%