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Hemagglutinin (HA) proteins from H1 and H3 serotypes of influenza A viruses require different antigen designs for the induction of optimal protective antibody responses as studied by codon-optimized HA DNA vaccines

机译：来自H1和H3甲型流感病毒血清型的血凝素（Ha）蛋白质需要不同的抗原设计用于诱导最佳保护性抗体应答，如密码子优化的Ha DNa疫苗所研究的

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Effective antibody responses provide crucial immunity against influenza virus infection. The hemagglutinin (HA) protein is the major target of protective antibody responses induced by viral infection and by vaccination with both inactivated and live-attenuated flu vaccines, but knowledge about the optimal designs of protective HA antigens from different flu serotypes is still limited. In this study, we have significantly improved the immunogenicity of HA-expressing DNA vaccines by using codon-optimized HA sequences for either an H1 serotype (A/NewCal/20/99) or an H3 serotype (A/Panama/2007/99) human influenza A virus and then used these constructs as model antigens to identify the optimal HA antigen designs to elicit high-level protective antibody responses. Two forms of HA antigen, a wild-type, full-length HA and a secreted form with transmembrane (TM) domain-truncated HA, were produced. Both forms of HA DNA vaccines, from either H1 or H3 serotypes, were able to elicit high levels of HA-specific immunoglobulin G responses in immunized rabbits as measured by enzyme-linked immunosorbent assay. Interestingly, the abilities of H1 HA and H3 HA antigens to elicit hemagglutination inhibition (HI) and neutralizing antibody (NAb) responses differ. For the H1 HA antigens, the full-length HA induced significantly higher HI and NAb responses than did the TM-truncated HA. For the H3 HA antigen, both the full-length HA and TM-truncated HA induced high levels of HI and NAb responses. These data indicate that H1 and H3 antigens have different expression requirements for the induction of an optimal protective antibody response and that the structure integrity of HA antigens is critical for eliciting type-specific protective antibody responses. Our findings will have an important impact on future subunit-based flu vaccine development.

机译：有效的抗体反应可提供抵抗流感病毒感染的关键免疫力。血凝素（HA）蛋白是病毒感染以及灭活和减毒活疫苗的疫苗接种诱导的保护性抗体应答的主要靶标，但是关于来自不同流感血清型的保护性HA抗原的最佳设计的知识仍然有限。在这项研究中，我们通过针对H1血清型（A / NewCal / 20/99）或H3血清型（A / Panama / 2007/99）使用密码子优化的HA序列，大大提高了表达HA的DNA疫苗的免疫原性。人甲型流感病毒，然后将这些构建体用作模型抗原，以鉴定引发高水平保护性抗体反应的最佳HA抗原设计。产生了两种形式的HA抗原：野生型，全长HA和具有跨膜（TM）域截短的HA的分泌形式。通过酶联免疫吸附法测定，来自H1或H3血清型的两种形式的HA DNA疫苗均能够在免疫兔中引起高水平的HA特异性免疫球蛋白G反应。有趣的是，H1 HA和H3 HA抗原引发血凝抑制（HI）和中和抗体（NAb）反应的能力有所不同。对于H1 HA抗原，全长HA诱导的HI和NAb应答明显高于TM截短的HA。对于H3 HA抗原，全长HA和TM截短的HA均可诱导高水平的HI和NAb反应。这些数据表明，H1和H3抗原对于诱导最佳保护性抗体应答具有不同的表达要求，并且HA抗原的结构完整性对于引发类型特异性保护性抗体应答至关重要。我们的发现将对未来基于亚基的流感疫苗的发展产生重要影响。

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Wang, Shixia; Taaffe, Jessica; Parker, Christopher S.; Solorzano, Alicia; Cao, Hong; Garcia-Sastre, Adolfo; Lu, Shan;
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专利

1. Heterologous HA DNA vaccine prime-inactivated influenza vaccine boost is more effective than using DNA or inactivated vaccine alone in eliciting antibody responses against H1 or H3 serotype influenza viruses. [J] . Wang S, Parker C, Taaffe J, Vaccine . 2008,第29a30期

机译：在引发针对H1或H3血清型流感病毒的抗体应答中，异源HA DNA疫苗初免灭活的流感疫苗加强效果比单独使用DNA或灭活疫苗更有效。
2. Influenza bivalent vaccine comprising recombinant H3 hemagglutinin (HA) and H1 HA containing replaced H3 hemagglutinin transmembrane domain exhibited improved heterosubtypic protection immunity in mice [J] . Liu Qiliang, Xue Chunyi, Zheng Jing, Vaccine . 2015,第32期

机译：包含重组H3血凝素（HA）和含有H3血凝素跨膜结构域的H1 HA的流感二价疫苗在小鼠中表现出改善的异型保护免疫
3. Comparative immunogenicity of recombinant adenovirus-vectored vaccines expressing different forms of hemagglutinin (HA) proteins from the H5 serotype of influenza A viruses in mice. [J] . Hu X, Meng W, Dong Z, Virus Research: An International Journal of Molecular and Cellular Virology . 2011,第1期

机译：重组腺病毒载体疫苗在小鼠中表现出不同形式的免疫原性，该疫苗表达不同形式的A型流感病毒H5血清型血凝素（HA）蛋白。
4. Antibody Cross-Reactivity to Hemagglutinin Protein Antigens Demonstrates Feasibility for Development of a "Universal" Influenza A Synthetic Peptide Vaccine [C] . Ziqing Jiang, Lajos Gera, Colin T. Mant American Peptide Symposium . 2015

机译：血凝素蛋白抗原的抗体交叉反应性表明了一种“通用”流感的开发合成肽疫苗的可行性
5. Hemagglutinin (HA) Proteins from H1 and H3 Serotypes of Influenza A Viruses Require Different Antigen Designs for the Induction of Optimal Protective Antibody Responses as Studied by Codon-Optimized HA DNA Vaccines [O] . Shixia Wang, Jessica Taaffe, Christopher Parker, 2006

机译：甲型流感病毒H1和H3血清型的血凝素（HA）蛋白需要不同的抗原设计才能诱导最佳保护性抗体反应如密码子优化的HA DNA疫苗研究
6. Hemagglutinin (HA) Proteins from H1 and H3 Serotypes of Influenza A Viruses Require Different Antigen Designs for the Induction of Optimal Protective Antibody Responses as Studied by Codon-Optimized HA DNA Vaccines▿ [O] . Wang, Shixia, Taaffe, Jessica, Parker, Christopher, 2006

机译：甲型流感病毒H1和H3血清型的血凝素（HA）蛋白需要不同的抗原设计才能诱导最佳保护性抗体反应，如密码子优化的HA DNA疫苗研究▿

Hemagglutinin (HA) proteins from H1 and H3 serotypes of influenza A viruses require different antigen designs for the induction of optimal protective antibody responses as studied by codon-optimized HA DNA vaccines

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