The heterologous expression of novel recombinant protein composed of HN and F moieties of Newcastle disease virus and immunogenicity evaluation in mouse model.

IF 1.3 Q4 MICROBIOLOGY
Atena Mozafari, Mehregan Rahmani, Yasaman Yasini Nasab, Shahla Shahsavandi, Mahyat Jafari, Ali Hatef Salmanian
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Abstract

Background and objectives: The rapid spread of Newcastle disease (ND), driven by extensive commercial exchange in the poultry industry, necessitates urgent preventive measures. Although effective vaccines against the Newcastle disease virus (NDV) have been used since 1940, recent outbreaks and the limitations of current vaccines highlight the need for improved solutions. Advances in synthetic biology, reverse vaccinology, molecular biology, and recombinant DNA technology over the past 20 years have led to the development of recombinant vaccines, which offer enhanced protection and broader immunogenic coverage against NDV. This study aimed to express the immunogenic domains of Hemagglutinin Neuraminidase (HN) and Fusion (F) glycoproteins, linked to the heat-labile enterotoxin B subunit (LTB) bio-adjuvant, to develop an effective and reliable recombinant vaccine for NDV.

Materials and methods: In this study, the L(HN)2F protein, composed of the LTB bio-adjuvant and the immunogenic regions of the doubled Hemagglutinin Neuraminidase (HN-HN) and Fusion (F) epitope, was expressed in Escherichia coli. Subcutaneous injection was used to evaluate the humoral immune response in mice and the result was compared with B1 vaccine.

Results: The induction of strong humoral immune responses proved the strong immunoreactivity of the recombinant protein.

Conclusion: The IgG elicited by the recombinant proteins was comparable to that of the commercial B1 vaccine against NDV, indicating its potential as a viable candidate for further development and evaluation as a recombinant vaccine against NDV.

由新城疫病毒 HN 和 F 分子组成的新型重组蛋白的异源表达及小鼠模型的免疫原性评价。
背景和目标:在家禽业广泛商业交换的推动下,新城疫(ND)迅速蔓延,因此必须采取紧急预防措施。尽管自 1940 年以来一直在使用有效的新城疫病毒 (NDV) 疫苗,但近期的疫情爆发和现有疫苗的局限性凸显了改进解决方案的必要性。过去 20 年中,合成生物学、反向疫苗学、分子生物学和 DNA 重组技术的进步促进了重组疫苗的发展,重组疫苗可提供更强的保护和更广的 NDV 免疫原覆盖范围。本研究旨在表达血凝素神经氨酸酶(HN)和融合(F)糖蛋白的免疫原结构域,并与热嗜性肠毒素 B 亚基(LTB)生物佐剂连接,以开发一种有效、可靠的 NDV 重组疫苗:本研究在大肠杆菌中表达了 L(HN)2F 蛋白,该蛋白由 LTB 生物佐剂和双倍血凝素神经氨酸酶(HN-HN)及融合(F)表位的免疫原区域组成。采用皮下注射法评估小鼠的体液免疫反应,并将结果与 B1 疫苗进行比较:结果:诱导的强烈体液免疫反应证明了重组蛋白的强免疫活性:结论:重组蛋白诱导的 IgG 与抗 NDV 的商业 B1 疫苗相当,表明其有潜力作为抗 NDV 重组疫苗进行进一步开发和评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
2.40
自引率
7.10%
发文量
96
审稿时长
12 weeks
期刊介绍: The Iranian Journal of Microbiology (IJM) is an international, multi-disciplinary, peer-reviewed journal that provides rapid publication of the most advanced scientific research in the areas of basic and applied research on bacteria and other micro-organisms, including bacteria, viruses, yeasts, fungi, microalgae, and protozoa concerning the development of tools for diagnosis and disease control, epidemiology, antimicrobial agents, clinical microbiology, immunology, Genetics, Genomics and Molecular Biology. Contributions may be in the form of original research papers, review articles, short communications, case reports, technical reports, and letters to the Editor. Research findings must be novel and the original data must be available for review by the Editors, if necessary. Studies that are preliminary, of weak originality or merely descriptive as well as negative results are not appropriate for the journal. Papers considered for publication must be unpublished work (except in an abstract form) that is not under consideration for publication anywhere else, and all co-authors should have agreed to the submission. Manuscripts should be written in English.
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