The predominance of Newcastle disease virus genotype VII: genome diversity or poor cross-immunity of non-matched vaccines

S. Shahsavandi, M. Ebrahimi, Majid Tebianain
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Abstract

the of divergence between and on the to suitable by focusing on the F and HN proteins. Comparative bioinformatics analyses based on B- and T-cell epitopes binding affinity, protein secondary structure and physicochemical properties predictions were applied for genotypes II and VII. Results: Although the results showed more differences in HN protein than F protein, there was no major difference between the predicted antigenicity values, epitope regions, affinity binding to MHC-I and MHC-II, secondary structures, surface accessibility, and stability of these immunogens between genotypes II and VII. Conclusion: The results suggest that genotype II-based live vaccines can induce immune responses against NDV; however, an inactivated vaccine formulated by genotype VII should be considered in combination with the traditional live vaccine to provide better protection in controlling programs against ND.
新城疫病毒基因型VII的优势:基因组多样性或不匹配疫苗的交叉免疫差
通过对F和HN蛋白的关注,研究了它们之间和上的差异。基于B和t细胞表位结合亲和力、蛋白质二级结构和物理化学性质预测的比较生物信息学分析应用于基因型II和VII。结果:虽然结果显示HN蛋白比F蛋白差异更大,但基因型II和基因型VII在预测抗原性值、表位区域、与MHC-I和MHC-II的亲和力结合、二级结构、表面可及性和稳定性方面没有明显差异。结论:基因ii型活疫苗可诱导对新城疫的免疫应答;然而,应考虑将基因型VII配制的灭活疫苗与传统活疫苗结合使用,以便在控制ND规划中提供更好的保护。
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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