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Title: | A novel bicistronic DNA vaccine with enhanced protective immune response against Bacillus anthracis through DNA prime-protein boost vaccination approach. |
Other Titles: | Not Available |
Authors: | Sumithra TG Chaturvedi VK Gupta PK Bincy J Siju SJ Sunita SC Reshma KJ Patel CL Rai AK |
ICAR Data Use Licennce: | http://krishi.icar.gov.in/PDF/ICAR_Data_Use_Licence.pdf |
Author's Affiliated institute: | ICAR-Indian Veterinary Research Institute, Izatnagar, UP, 243122, India. |
Published/ Complete Date: | 2021-07-20 |
Project Code: | Not Available |
Keywords: | Anthrax Booster dose Immunoprotective antigens Next-generation vaccine Secretory DNA construct Serum bactericidal activity |
Publisher: | Elsevier Publisher |
Citation: | Sumithra TG, Chaturvedi VK, Gupta PK, Bincy J, Siju SJ, Sunita SC, Reshma KJ, Patel CL, Rai AK. A novel bicistronic DNA vaccine with enhanced protective immune response against Bacillus anthracis through DNA prime-protein boost vaccination approach. Microb Pathog. 2021 Sep;158:105104. doi: 10.1016/j.micpath.2021.105104. Epub 2021 Jul 20. PMID: 34298126. |
Series/Report no.: | Not Available; |
Abstract/Description: | Anthrax, by Bacillus anthracis, remains a dreadful fatal hazard worldwide. The currently used anthrax vaccines are plagued by numerous issues that limit their widespread use. As an immunization approach targeting both extracellular antigens and toxins of B. anthracis may achieve better sterile immunity, the present investigation designed a bicistronic secretory anti-anthrax DNA vaccine targeting immune response against toxin and cells. The efficacy of the vaccine was compared with monocistronic DNA vaccines and the currently used anthrax vaccine. For this, mice were immunized with the developed vaccine containing pag (encoding protective antigen to block toxin) and eag genes (encoding EA1 to target cells) of B. anthracis through DNA-prime/Protein -boost (D/P) and DNA prime/DNA-boost (D/D) approaches. There was a >2 and > 5 fold increase in specific antibody level by D/D and D/P approaches respectively, on 42nd days post-immunization (dpi). Serum cytokine profiling showed that both Th1 and Th2 immune responses were elicited, with more Th2 responses in D/P strategy. More importantly, challenge with 100 times LD50 of B. anthracis at 42nd dpi exhibited maximum cumulative survival (83.33 %) by bicistronic D/P approach. Remarkably, immunization with EA1 delayed mortality onset in infection. The study forms the first report on complement-dependent bactericidal activity of antiEA1 antibodies. In short, co-immunization of PA and EA1 through the developed bicistronic DNA vaccine would be an effective immunization approach in anthrax vaccination. Further, D/P strategy could enhance vaccine-induced immunity against B. anthracis. Altogether, the study generates certain critical insights having direct applications in next-generation vaccine development against anthrax. |
Description: | Not Available |
ISSN: | 0882-4010 |
Type(s) of content: | Research Paper |
Sponsors: | Not Available |
Language: | English |
Name of Journal: | Microbial Pathogenesis |
Journal Type: | Peer reviewed journal |
NAAS Rating: | 8.91 |
Impact Factor: | 3.738 |
Volume No.: | 158 |
Page Number: | 1-9 |
Name of the Division/Regional Station: | Not Available |
Source, DOI or any other URL: | 10.1016/j.micpath.2021.105104 |
URI: | http://krishi.icar.gov.in/jspui/handle/123456789/71570 |
Appears in Collections: | AS-NIVEDI-Publication |
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