Optimization of In Vivo Electroporation Conditions and Delivery of DNA Vaccine Encoding SARS-CoV-2 RBD Using the Determined Protocol

Author:

Kisakov Denis NikolaevichORCID,Kisakova Lyubov Alexandrovna,Borgoyakova Maria BorisovnaORCID,Starostina Ekaterina Vladimirovna,Taranov Oleg SvyatoslavovichORCID,Ivleva Elena Konstantinovna,Pyankov Oleg Viktorovich,Zaykovskaya Anna VladimirovnaORCID,Shcherbakov Dmitry Nikolaevich,Rudometov Andrey Pavlovich,Rudometova Nadezda Borisovna,Volkova Natalia Vyacheslavovna,Gureev Vadim NikolaevichORCID,Ilyichev Alexander Alexeyevich,Karpenko Larisa IvanovnaORCID

Abstract

Vaccination against SARS-CoV-2 and other viral infections requires safe, effective, and inexpensive vaccines that can be rapidly developed. DNA vaccines are candidates that meet these criteria, but one of their drawbacks is their relatively weak immunogenicity. Electroporation (EP) is an effective way to enhance the immunogenicity of DNA vaccines, but because of the different configurations of the devices that are used for EP, it is necessary to carefully select the conditions of the procedure, including characteristics such as voltage, current strength, number of pulses, etc. In this study, we determined the optimal parameters for delivery DNA vaccine by electroporation using the BEX CO device. BALB/c mice were used as a model. Plasmid DNA phMGFP was intramuscular (I/M) injected into the quadriceps muscle of the left hind leg of animals using insulin syringes, followed by EP. As a result of the experiments, the following EP parameters were determined: direct and reverse polarity rectangular DC current in three pulses, 12 V voltage for 30 ms and 950 ms intervals, with a current limit of 45 mA. The selected protocol induced a low level of injury and provided a high level of GFP expression. The chosen protocol was used to evaluate the immunogenicity of the DNA vaccine encoding the receptor-binding domain (RBD) of the SARS-CoV-2 protein (pVAXrbd) injected by EP. It was shown that the delivery of pVAXrbd via EP significantly enhanced both specific humoral and cellular immune responses compared to the intramuscular injection of the DNA vaccine.

Funder

The study was supported by the Ministry of Science and Higher Education of the Russian Federation

Publisher

MDPI AG

Subject

Pharmaceutical Science

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1. Immunogenic Effects and Clinical Applications of Electroporation-Based Treatments;Vaccines;2023-12-30

2. The use of electroporation to deliver DNA-based vaccines;Expert Review of Vaccines;2023-12-18

3. Approaches to Improve the Immunogenicity of Plasmid DNA-Based Vaccines against COVID-19;Population Genetics - From DNA to Evolutionary Biology [Working Title];2023-12-13

4. DNA Vaccine Encoding the Artificial T-Cell Polyepitope Immunogen of Tick-Borne Encephalitis Virus;Bulletin of Experimental Biology and Medicine;2023-11

5. Artificial COVID-19 T-Cell Immunogen;Bulletin of Experimental Biology and Medicine;2023-10

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