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Effect of emergency FMD vaccine antigen payload on protection, sub-clinical infection and persistence following direct contact challenge of cattle

机译:紧急口蹄疫疫苗抗原有效载荷对牛直接接触攻击后保护,亚临床感染和持久性的影响

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摘要

Previous work, in sheep vaccinated with emergency foot-and-mouth disease (FMD) vaccine, indicated the benefit of increasing the antigen payload in inhibiting local virus replication and consequently persistence following an indirect aerosol challenge with a virus homologous to the vaccine strain. The work presented here investigates this possibility further using cattle and a more severe semi-heterologous direct contact challenge. The quantitative dynamics of virus replication and excretion in both vaccinated and non-vaccinated cattle following challenge are examined. Two experiments were carried out each involving 20 vaccinated and 5 non-vaccinated cattle. An O(1) Manisa vaccine (18 PD(50)) was used for the first, previously reported experiment [Cox SJ, Voyce C, Parida S, Reid SM, Hamblin PA, Paton DJ, et al. Protection against direct contact challenge following emergency FMD vaccination of cattle and the effect on virus excretion from the oropharynx. Vaccine 2005;23:1106-13]. The same vaccine was used for the second experiment described in this paper except the antigen payload was increased 10-fold per bovine dose, resulting in significantly higher FMD virus neutralising antibody titres prior to challenge. Twenty-one days post-vaccination the cattle received a 5-day direct contact challenge with FMD virus from five further non-vaccinated cattle infected 24h earlier with O UKG 34/2001. All vaccinated cattle regardless of antigen payload were protected against clinical disease. Sub-clinical oropharyngeal infection was detected in animals from both experiments but the level of virus replication shortly after direct contact challenge was significantly reduced in vaccinated animals. Cattle immunised with the 10-fold antigen payload cleared the virus more readily and consequently at 28 days post-challenge fewer animals were persistently infected compared to the single strength vaccine. Following a severe challenge, the results from both experiments show that use of emergency vaccine can prevent or decrease local virus replication and thereby dramatically reduce the amount of virus released into the environment, particularly during the early post-exposure period. Additionally, increasing the antigen payload of the vaccine may reduce sub-clinical infection, leading to fewer persistently infected virus carrier animals.
机译:先前的工作是在用紧急口蹄疫(FMD)疫苗接种的绵羊中进行的,表明增加抗原有效载荷的作用在于抑制局部病毒复制,从而在与疫苗株同源的病毒进行间接气雾攻击后具有持久性。本文介绍的工作进一步调查了使用牛和更严重的半异源直接接触挑战的可能性。检查了接种后和未接种牛中病毒复制和排泄的定量动力学。进行了两个实验,每个实验涉及20只疫苗接种的牛和5只未接种疫苗的牛。 O(1)Manisa疫苗(18 PD(50))用于第一个先前报道的实验[Cox SJ,Voyce C,Parida S,Reid SM,Hamblin PA,Paton DJ等。预防牛口蹄疫紧急接种后的直接接触挑战以及对口咽病毒排泄的影响。疫苗2005; 23:1106-13]。相同的疫苗用于本文所述的第二个实验,只是抗原有效载荷每牛剂量增加了10倍,从而在攻击前显着提高了FMD病毒中和抗体的效价。疫苗接种后二十一天,牛从24小时前被O UKG 34/2001感染的另外五只未接种牛中接受了5天与口蹄疫病毒的直接接触攻击。不论抗原有效载荷如何,所有接种牛都可以预防临床疾病。在两个实验中均在动物中检测到亚临床的口咽感染,但是在直接接触攻击后不久,接种疫苗的动物中病毒复制的水平显着降低。用10倍抗原有效载荷免疫的牛更容易清除病毒,因此,与单强度疫苗相比,攻击后28天持续感染的动物更少。经过严峻的挑战,两个实验的结果表明,使用应急疫苗可以预防或减少局部病毒复制,从而显着减少释放到环境中的病毒数量,尤其是在暴露后初期。另外,增加疫苗的抗原有效载荷可以减少亚临床感染,从而导致更少的持续感染的病毒携带动物。

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