甲型流感和SARS-CoV-2病毒mRNA和蛋白结合疫苗的计算设计和评价

IF 3.6 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Journal, genetic engineering & biotechnology Pub Date : 2023-11-15 DOI:10.1186/s43141-023-00574-x
Amir Elalouf, Tomer Kedarya, Hadas Elalouf, Ariel Rosenfeld
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引用次数: 0

摘要

背景:以色列在一名未接种疫苗的孕妇中确认了首例“氟罗纳”病例——季节性流感(IAV)和SARS-CoV-2的合并感染。这两大流行病已在多个国家得到证实,并强调了管理呼吸道病毒性疾病的重要性。结果:将b细胞表位的4个血凝素、3个神经氨酸酶和4个S蛋白,MHC-I表位的2个血凝素、3个神经氨酸酶和4个S蛋白,以及MHC-II表位的3个血凝素、9个神经氨酸酶和5个S蛋白与连接物和佐剂结合,设计出新型结合疫苗。构建的结合疫苗稳定、无毒、无过敏、抗原性好,得分为0.6466。该疫苗含有14.87%的α螺旋、29.85%的延伸链、9.64%的β转和45.64%的随机线圈,其三维结构在Ramachandran图的最有利区域有94.7%的残基,z分数为-3.33。疫苗与TLR3的分子对接,具有39个氢键和514个非键接触,结合能为-1513.9 kcal/mol,特征值配合物为1.582925e-07。免疫刺激预测表明,结合疫苗能激活T淋巴细胞和B淋巴细胞,产生高水平的Th1细胞因子和抗体。结论:硅设计的IAV和SARS-CoV-2疫苗具有良好的人群覆盖率和免疫应答,具有预测的T细胞和b细胞表位,良好的分子对接,Ramachandran图结果,良好的蛋白表达。它符合安全标准,表明临床前研究和实验性临床试验的潜力。
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Computational design and evaluation of mRNA- and protein-based conjugate vaccines for influenza A and SARS-CoV-2 viruses.

Background: Israel confirmed the first case of "flurona"-a co-infection of seasonal flu (IAV) and SARS-CoV-2 in an unvaccinated pregnant woman. This twindemic has been confirmed in multiple countries and underscores the importance of managing respiratory viral illnesses.

Results: The novel conjugate vaccine was designed by joining four hemagglutinin, three neuraminidase, and four S protein of B-cell epitopes, two hemagglutinin, three neuraminidase, and four S proteins of MHC-I epitopes, and three hemagglutinin, nine neuraminidase, and five S proteins of MHC-II epitopes with linkers and adjuvants. The constructed conjugate vaccine was found stable, non-toxic, non-allergic, and antigenic with 0.6466 scores. The vaccine contained 14.87% alpha helix, 29.85% extended strand, 9.64% beta-turn, and 45.64% random coil, which was modeled to a 3D structure with 94.7% residues in the most favored region of the Ramachandran plot and Z-score of -3.33. The molecular docking of the vaccine with TLR3 represented -1513.9 kcal/mol of binding energy with 39 hydrogen bonds and 514 non-bonded contacts, and 1.582925e-07 of eigenvalue complex. Immune stimulation prediction showed the conjugate vaccine could activate T and B lymphocytes to produce high levels of Th1 cytokines and antibodies.

Conclusion: The in silico-designed vaccine against IAV and SARS-CoV-2 showed good population coverage and immune response with predicted T- and B-cell epitopes, favorable molecular docking, Ramachandran plot results, and good protein expression. It fulfilled safety criteria, indicating potential for preclinical studies and experimental clinical trials.

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