首页> 外文OA文献 >A Recombinant La Sota Vaccine Strain Expressing Multiple Epitopes of Infectious Bronchitis Virus (IBV) Protects Specific Pathogen-Free (SPF) Chickens against IBV and NDV Challenges
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A Recombinant La Sota Vaccine Strain Expressing Multiple Epitopes of Infectious Bronchitis Virus (IBV) Protects Specific Pathogen-Free (SPF) Chickens against IBV and NDV Challenges

机译:表达传染性支气管炎病毒(IBV)多个表位的重组LA SOTA疫苗菌株保护针对IBV和NDV挑战的特异性无病原体(SPF)鸡

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摘要

Infectious bronchitis (IB) and Newcastle disease (ND) are two major infectious diseases that are a threat to the domestic poultry industry. In this study, we successfully generated a recombinant LaSota candidate vaccine strain, rNDV-IBV-T/B, which expresses a short, synthetic, previously identified IBV S1 multi-epitope cassette using the reverse genetic system. The recombinant virus was propagated in nine-day-old embryonated chicken eggs for 20 passages and genetic stability was confirmed by whole genome DNA sequencing. The recombinant virus had a hemagglutination (HA) titer of 210, mean death time (MDT) of 118 hours, and intracerebral pathogenicity index (ICPI) of 0.05. None of these were significantly different from the parental Newcastle disease virus (NDV) LaSota strain (p > 0.05). Vaccination of white leghorn chickens at one day of age with 106 EID50 rNDV-IBV-T/B provided 90% protection against virulent IBV M41 challenge at three weeks of age, which was significantly higher than the protection of the control group vaccinated with phosphate-buffered saline (PBS) (p < 0.05). The ciliostasis scores of rNDV-IBV-T/B-vaccinated and LaSota-vaccinated groups were 4.2 and 37.6, respectively, which indicated that rNDV-IBV-T/B vaccination reduced the pathogenicity of IBV toward the trachea. Furthermore, real-time RT-PCR assay showed that the rNDV-IBV-T/B vaccination resulted in low levels of viral load (647.80 ± 49.65 RNA copies) in the trachea four days post-challenge, which is significantly lower than groups vaccinated with PBS (8591.25 ± 311.10 RNA copies) or LaSota (7742.60 ± 298.50 RNA copies) (p < 0.05). Meanwhile, the same dose of rNDV-IBV-T/B vaccination provided complete protection against velogenic NDV F48E9 challenge. These results demonstrate that the rNDV-IBV-T/B strain is a promising vaccine candidate to control both IB and ND simultaneously. Furthermore, epitope-based live vector vaccines provide an alternative strategy for the development of cost-effective and, broadly, cross-protective vaccines.
机译:感染性支气管炎(IB)和新城疫(ND)是两种主要传染病,这是对家禽业的威胁。在这项研究中,我们成功地生成了使用反向遗传系统表达短,合成的先前鉴定的IBV S1多表位盒的重组型溶液候选疫苗菌株,RNDV-IBV-T / B.重组病毒在九天血液胚胎卵中繁殖,以20个通道,通过全基因组DNA测序确认遗传稳定性。重组病毒具有210的血凝(HA)滴度,平均死亡时间(MDT)为118小时,脑致病性指数(ICPI)为0.05。这些都没有与祖父疾病病毒(NDV)Lasota菌株的显着不同(P> 0.05)。 White Lehghorn鸡的疫苗接种在1天的时候,用106 EID50 RNDV-IBV-T / B提供了90%的保护,针对毒力IBV M41挑战在三周的年龄上进行了挑战,显着高于用磷疫苗接种的对照组的保护 - 缓冲盐水(PBS)(P <0.05)。 RNDV-IBV-T / B接种疫苗和漂移分数分别为4.2和37.6分别为4.2和37.6,表明RNDV-IBV-T / B疫苗接种疫苗接种促进IBV朝向气管的致病性。此外,实时RT-PCR测定显示RNDV-IBV-T / B疫苗接种导致气管中的病毒载量(647.80±49.65 rna拷贝)在攻击后四天,这显着低于疫苗的基团PBS(8591.25±311.10拷贝)或漂移(7742.60±298.50 rna拷贝)(P <0.05)。同时,相同剂量的RNDV-IBV-T / B疫苗接种疫苗提供了完全保护,免受麝配醋栗NDV F48E9挑战。这些结果表明,RNDV-IBV-T / B菌株是一种有前途的疫苗候选者,用于同时控制IB和ND。此外,基于EPITOPE的现场矢量疫苗提供了用于开发成本效益和,广泛,交叉保护疫苗的替代策略。

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