首页> 美国卫生研究院文献>Journal of Virology >A multivalent minigene vaccine containing B-cell cytotoxic T-lymphocyte and Th epitopes from several microbes induces appropriate responses in vivo and confers protection against more than one pathogen.
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A multivalent minigene vaccine containing B-cell cytotoxic T-lymphocyte and Th epitopes from several microbes induces appropriate responses in vivo and confers protection against more than one pathogen.

机译:一种多价小基因疫苗其中包含来自几种微生物的B细胞细胞毒性T淋巴细胞和Th表位可在体内诱导适当的反应并提供针对多种病原体的保护。

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摘要

The development of safe and effective vaccines remains a major goal in the prevention, and perhaps treatment, of infectious diseases. Ideally, a single vaccine would confer protection against several pathogens and would induce both cellular and humoral arms of the immune response. We originally demonstrated that two virus-specific cytotoxic T-lymphocyte (CTL) epitopes, from the same virus but presented by different major histocompatibility complex alleles, when linked in tandem as minigenes in a recombinant vaccinia virus, could confer complete protection against subsequent viral challenge. In the study, we extended this approach, which we termed string of beads, expanding the immunogenic scope in two ways: first, by introduction of T helper (Th) and B-cell (antibody) epitopes alongside CTL epitopes and second, by including immunogenic sequences from a variety of infectious agents, five viruses and one bacterium. The vaccine (VV-sv) comprises CTL epitopes from Sendai virus, respiratory syncytial virus, and lymphocytic choriomeningitis virus (LCMV); Th epitopes from vesicular stomatitis virus and Mycobacterium tuberculosis; and an antibody epitope from mengovirus. The construct contains a single start codon, and the epitopes are linked directly, without intervening spacer amino acids. There was some concern that the combination of several normally immunodominant epitopes might result in a new hierarchy of dominance, in which certain epitopes predominated and others exhibited reduced immunogenicity. However we show that when analyzed in tissue culture and in vivo, all six epitopes are expressed. CTL and Th cells are induced in vivo, along with neutralizing antibody. The induced immunity is biologically relevant: after VV-sv immunization, the antimengovirus antibody confers protection against mengovirus challenge. Similarly, CTL induced by the LCMV epitope protected mice against challenge with this agent. Thus, a polyvalent, minigene-based vaccine can simultaneously induce several classes of immune response and thereby can confer protection against diverse pathogens.
机译:开发安全有效的疫苗仍然是预防或可能治疗传染病的主要目标。理想情况下,单一疫苗可针对几种病原体提供保护,并诱导免疫反应的细胞和体液。我们最初证明,来自同一病毒但由不同主要组织相容性复杂等位基因呈现的两个病毒特异性细胞毒性T淋巴细胞(CTL)表位,在重组痘苗病毒中作为小基因串联时,可以赋予针对后续病毒攻击的完整保护。在研究中,我们扩展了这种方法,我们称其为“珠串”,以两种方式扩展了免疫原性的范围:首先,通过引入T辅助(Th)和B细胞(抗体)表位以及CTL表位,其次,包括来自多种传染原,五种病毒和一种细菌的免疫原性序列。疫苗(VV-sv)包含仙台病毒,呼吸道合胞病毒和淋巴细胞性脉络膜脑膜炎病毒(LCMV)的CTL表位;水泡性口炎病毒和结核分枝杆菌的Th表位;以及来自芒果病毒的抗体表位。该构建体包含单个起始密码子,并且表位直接连接,而无需插入间隔氨基酸。令人担忧的是,几种通常具有免疫优势的抗原决定簇的结合可能会导致新的优势等级,其中某些抗原决定簇占主导,而其他抗原决定簇则具有降低的免疫原性。但是,我们显示,在组织培养和体内进行分析时,所有六个表位均表达。与中和抗体一起在体内诱导CTL和Th细胞。诱导的免疫是生物学相关的:在VV-sv免疫后,抗芒果病毒抗体可提供抵抗芒果病毒攻击的保护作用。类似地,由LCMV表位诱导的CTL使小鼠免受该试剂的攻击。因此,基于小基因的多价疫苗可同时诱导几种类型的免疫反应,从而可针对多种病原体提供保护。

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