首页> 美国卫生研究院文献>Journal of Virology >Biology of Attenuated Modified Vaccinia Virus Ankara Recombinant Vector in Mice: Virus Fate and Activation of B- and T-Cell Immune Responses in Comparison with the Western Reserve Strain and Advantages as a Vaccine
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Biology of Attenuated Modified Vaccinia Virus Ankara Recombinant Vector in Mice: Virus Fate and Activation of B- and T-Cell Immune Responses in Comparison with the Western Reserve Strain and Advantages as a Vaccine

机译:减毒的牛痘病毒安卡拉重组载体在小鼠中的生物学:病毒的命运以及B和T细胞免疫应答的活化与西方储备菌株的比较和作为疫苗的优势

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摘要

The modified vaccinia virus Ankara (MVA) strain is a candidate vector for vaccination against pathogens and tumors, due to safety concerns and the proven ability of recombinants based on this vector to trigger protection against pathogens in animals. In this study we addressed the fate of the MVA vector in BALB/c mice after intraperitoneal inoculation in comparison with that of the replication-competent Western Reserve (WR) strain by measuring levels of expression of the reporter luciferase gene, the capability to infect target tissues from the site of inoculation, and the length of time of virus persistence. We evaluated the extent of humoral and cellular immune responses induced against the virus antigens and a recombinant product (β-galactosidase). We found that MVA infects the same target tissues as the WR strain; surprisingly, within 6 h postinoculation the levels of expression of antigens were higher in tissues from MVA-infected mice than in tissues from mice infected with wild-type virus but at later times postinoculation were 2 to 4 log units higher in tissues from WR-infected mice. In spite of this, antibodies and cellular immune responses to viral vector antigens were considerably lower in MVA-inoculated mice than in WR virus-inoculated mice. In contrast, the cellular immune response to a foreign antigen expressed from MVA was similar to and even higher than that triggered by the recombinant WR virus. MVA elicited a Th1 type of immune response, and the main proinflammatory cytokines induced were interleukin-6 and tumor necrosis factor alpha. Our findings have defined the biological characteristics of MVA infection in tissues and the immune parameters activated in the course of virus infection. These results are of significance with respect to optimal use of MVA as a vaccine.
机译:修饰的牛痘病毒安卡拉(MVA)菌株是候选疫苗,可用于接种病原体和肿瘤,这是出于安全方面的考虑,并且基于该载体的重组体已被证明具有触发动物病原体保护的能力。在这项研究中,我们通过测量报告荧光素酶基因的表达水平,感染靶点的能力,探讨了腹腔接种BALB / c小鼠中MVA载体与具有复制能力的Western Reserve(WR)菌株相比的命运。组织从接种部位开始,以及病毒持续时间的长短。我们评估了针对病毒抗原和重组产物(β-半乳糖苷酶)诱导的体液和细胞免疫应答的程度。我们发现,MVA感染与WR菌株相同的靶组织。令人惊讶地,在接种后6小时内,来自MVA感染的小鼠的组织中的抗原表达水平高于被野生型病毒感染的小鼠的组织中的抗原表达水平,但是在随后的时间,在接种由WR感染的组织中,接种后的抗原表达水平高2-4个log单位。老鼠。尽管如此,在MVA接种的小鼠中对病毒载体抗原的抗体和细胞免疫应答比在WR病毒接种的小鼠中要低得多。相反,对由MVA表达的外源抗原的细胞免疫应答与重组WR病毒触发的相似,甚至更高。 MVA引发Th1型免疫反应,诱导的主要促炎细胞因子为白介素6和肿瘤坏死因子α。我们的发现定义了组织中MVA感染的生物学特征以及在病毒感染过程中激活的免疫参数。这些结果对于最佳使用MVA作为疫苗具有重要意义。

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