Development of a genotype-matched Newcastle disease DNA vaccine candidate adjuvanted with IL-28b for the control of targeted velogenic strains of Newcastle disease virus in Africa

被引:0
作者
Amoia, Charlie F. [1 ,2 ,3 ]
Chengula, Augustino A. [1 ]
Hakizimana, Jean N. [4 ]
Wambura, Philemon N. [1 ]
Munir, Muhammad [5 ]
Misinzo, Gerald [1 ,2 ,4 ]
Weger-Lucarelli, James [3 ,6 ]
机构
[1] Sokoine Univ Agr, Dept Vet Microbiol Parasitol & Biotechnol, POB 3019, Morogoro 67125, Tanzania
[2] Sokoine Univ Agr, SACIDS Fdn One Hlth, SACIDS Africa Ctr Excellence Infect Dis, POB 3297, Morogoro 67125, Tanzania
[3] Virginia Polytech Inst & State Univ Virginia Tech, Ctr Emerging Zoonot & Arthropod borne Pathogens, Blacksburg, VA 24061 USA
[4] Sokoine Univ Agr, SACIDS Fdn One Hlth, Tambo Africa Res Chair Viral Epidem, POB 3297, Morogoro 67125, Tanzania
[5] Univ Lancaster, Fac Hlth & Med, Div Biomed & Life Sci, Lancaster LA1 4YG, England
[6] Virginia Tech, Virginia Maryland Coll Vet Med, Dept Biomed Sci & Pathobiol, Blacksburg, VA 24060 USA
关键词
Newcastle Disease virus; Genotype-matched; DNA vaccine; Interferon lambda-3; IL-28b; Molecular adjuvant; PROTECTION; CHALLENGE; SEQUENCES; CHICKENS; EFFICACY; PROTEIN;
D O I
10.1007/s11259-024-10590-y
中图分类号
S85 [动物医学(兽医学)];
学科分类号
0906 ;
摘要
Newcastle disease virus (NDV) is an extremely contagious and deadly virus that affects numerous bird species, posing serious threats to poultry production on a global scale. In addition to implementing biosecurity practices in farming systems, vaccination remains the most effective means of controlling Newcastle disease (ND). However, while existing commercial vaccines provide some level of protection, the effectiveness of these vaccines can be questionable, particularly in field settings where the complexity of vaccination program implementation poses significant challenges, especially against virulent genotypes of NDV. A genotype-matched NDV DNA vaccine could potentially offer a more effective vaccination approach than currently available live attenuated vaccines. By being specifically tailored to match circulating strains, such a vaccine might improve efficacy and reduce the risk of vaccine failure due to genotype mismatch. To develop an alternative vaccine approach, two ND DNA vaccines were constructed in this study. Each vaccine developed in this study contains the fusion (F) and haemagglutinin-neuraminidase (HN) genes of a virulent NDV genotype VII isolate from Tanzania. Interferon lambda-3 (IFN lambda 3; IL-28b), which has demonstrated capacity to significantly enhance specific adaptive immune responses and decreased levels of inflammatory cytokines, as well as improved protective responses at a high viral challenge dose, was included in one of the developed vaccines. These plasmids were designated pTwist-F-HN-VII-IL28b and pTwist-F-HN-VII. The two plasmids differed in that pTwist-F-HN-VII-IL28b contained the cytokine adjuvant IL-28b. Transfection of cells and subsequent immunofluorescence assays indicated that both plasmids expressed high levels of NDV F-HN proteins. In vivo immunization demonstrated that chicks intramuscularly immunized with pTwist-F-HN-VII-IL28b exhibited significant immune responses compared to chicks immunized with pTwist-F-HN-VII or the commonly used LaSota vaccine (LaSota), which was used as a control. The protective efficacy of pTwist-F-HN-VII-IL28b was 80% after challenge with the highly virulent NDV strain ON148423, compared to 60% for chicks vaccinated using LaSota, and pTwist-F-HN-VII. The findings of this study indicate that IL-28b can be employed as a molecular adjuvant for NDV vaccines. This study represents a key milestone in Newcastle disease vaccine research, particularly in the development of a genotype-matched DNA vaccine candidate. Additionally, this study demonstrated that the combination of F, HN, and IL-28b elicits an efficacious immune response against virulent NDV strains.
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页数:16
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