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Evaluation of an African swine fever (ASF) vaccine strategy incorporating priming with an alphavirus-expressed antigen followed by boosting with attenuated ASF virus

机译:评估非洲猪瘟(ASF)疫苗策略,其掺入与alphavirous表达的抗原引起的,然后用减毒ASF病毒提升

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In this study, an alphavirus vector platform was used to deliver replicon particles (RPs) expressing African swine fever virus (ASFV) antigens to swine. Alphavirus RPs expressing ASFV p30 (RP-30), p54 (RP-54) or pHA-72 (RP-sHA-p72) antigens were constructed and tested for expression in Vero cells and for immunogenicity in pigs. RP-30 showed the highest expression in Vero cells and was the most immunogenic in pigs, followed by RP-54 and RP-sHA-p72. Pigs primed with two doses of the RP-30 construct were then boosted with a naturally attenuated ASFV isolate, OURT88/3. Mapping of p30 identified an immunodominant region within the amino acid residues 111-130. However, the principal effect of the prime-boost was enhanced recognition of an epitope covered by the peptide sequence 61-110. The results suggest that a strategy incorporating priming with a vector-expressed antigen followed by boosting with an attenuated live virus may broaden the recognition of ASFV epitopes.
机译:在本研究中,使用alphavirus载体平台将表达非洲猪瘟病毒(ASFV)抗原的复制子颗粒(RPS)递送至猪。 构建并测试表达ASFV P30(RP-30),P54(RP-54)或PHA-72(RP-SHA-P72)抗原的alphavirus rps,并在VERO细胞中表达和用于猪的免疫原性。 RP-30显示了Vero细胞中最高的表达,并且是猪中最免疫原性的,其次是RP-54和RP-SHA-P72。 然后用两种剂量的RP-30构建体引入猪,用天然衰减的ASFV分离物,OUT88 / 3升高。 P30的映射鉴定了氨基酸残基111-130内的免疫肿块区域。 然而,Prime-Boost的主要效果增强了肽序列61-110覆盖的表位的识别。 结果表明,用载体表达的抗原引入引发的策略,然后用减毒的活病毒提升,可以扩大ASFV表位的识别。

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