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首页> 外文期刊>Human vaccines & immunotherapeutics. >Screening of primary gp120 immunogens to formulate the next generation polyvalent DNA prime-protein boost HIV-1 vaccines
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Screening of primary gp120 immunogens to formulate the next generation polyvalent DNA prime-protein boost HIV-1 vaccines

机译:筛选初级GP120免疫原制备下一代多元化DNA蛋白增强HIV-1疫苗

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摘要

Our previous preclinical studies and a Phase I clinical trial DP6-001 have indicated that a polyvalent Env formulation was able to elicit broadly reactive antibody responses including low titer neutralizing antibody responses against viral isolates of subtypes A, B, C and AE. In the current report, a panel of 62 gp120 immunogens were screened in a rabbit model to identify gp120 immunogens that can elicit improved binding and neutralizing antibody responses and some of them can be included in the next polyvalent formulation. Only about 19% of gp120 immunogens in this panel were able to elicit neutralizing antibodies against greater than 50% of the viruses included in a high throughput PhenoSense neutralization assay when these immuongens were tested as a DNA prime followed by a fixed 5-valent gp120 protein vaccine boost. The new polyvalent formulation, using five gp120 immunogens selected from this subgroup, elicited improved quality of antibody responses in rabbits than the previous DP6-001 formulation. More significantly, this new polyvalent formulation elicited higher antibody responses against a panel of gp70V1/V2 antigens expressing V1/V2 sequences from diverse subtypes. Bioinformatics analysis supports the design of a 4-valent or 5-valent formulation using gp120 immunogens from this screening study to achieve a broad coverage against 16 HIV-1 subtypes.
机译:我们以前的临床前研究和I阶段临床试验DP6-001表明,多价Env配方能够引发广泛的反应性抗体应答,包括对亚型A,B,C和AE的病毒分离株的低滴度中和抗体反应。在当前报告中,在兔模型中筛选62个GP120免疫原的小组,以鉴定可以引发改善的结合和中和抗体反应的GP120免疫原,并且其中一些可以包括在下一个多价制剂中。当这些免疫转移作为DNA Prime后,该小组中只有约19%的GP120免疫蛋白在该小组中,能够引发抗体的中和抗体,其在高通量比例中和中和中和在高通吞吐量中和中和中和中加入的病毒中包含的病毒。随后是固定的5价GP120蛋白疫苗提升。新的多价制剂,使用选自该亚组的五种GP120免疫原,引发了兔子中的抗体反应的提高质量,而不是先前的DP6-001配方。更重要的是,这种新的多价制剂引发了与来自不同亚型的V1 / V2序列的GP70V1 / V2抗原面板引发了更高的抗体反应。生物信息学分析支持使用来自该筛查研究的GP120免疫原的4价或5价配方的设计,以实现针对16个HIV-1亚型的广泛覆盖范围。

著录项

  • 来源
    《Human vaccines & immunotherapeutics.》 |2017年第12期|共14页
  • 作者单位

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

    Univ Massachusetts Sch Med Dept Mol Med Worcester MA USA;

    NIAID Immunopathogenesis Sect NIH 9000 Rockville Pike Bethesda MD 20892 USA;

    Duke Univ Sch Med Dept Surg Durham NC USA;

    Univ Massachusetts Sch Med Dept Med Lab Nucle Acid Vaccines Worcester MA 01605 USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 医学免疫学;
  • 关键词

    antibody; DNA vaccine; envelope glycoprotein; heterologous prime - boost; HIV-1; polyvalent; protein vaccine; vaccine;

    机译:抗体;DNA疫苗;包膜糖蛋白;异源素 - 升压;HIV-1;多价;蛋白质疫苗;疫苗;

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