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一种腺病毒5型初免-安卡拉改良痘苗病毒加强的亚单位疫苗对犊牛抗副结核分枝杆菌感染的免疫、安全性及保护作用

Immunity, safety and protection of an Adenovirus 5 prime--Modified Vaccinia virus Ankara boost subunit vaccine against Mycobacterium avium subspecies paratuberculosis infection in calves.

作者信息

Bull Tim J, Vrettou Christina, Linedale Richard, McGuinnes Catherine, Strain Sam, McNair Jim, Gilbert Sarah C, Hope Jayne C

机构信息

Institute of Infection and Immunity, St, George's University of London, Cranmer Terrace, London SW17 0RE, UK.

出版信息

Vet Res. 2014 Oct 29;45(1):112. doi: 10.1186/s13567-014-0112-9.

Abstract

Vaccination is the most cost effective control measure for Johne's disease caused by Mycobacterium avium subspecies paratuberculosis (MAP) but currently available whole cell killed formulations have limited efficacy and are incompatible with the diagnosis of bovine tuberculosis by tuberculin skin test. We have evaluated the utility of a viral delivery regimen of non-replicative human Adenovirus 5 and Modified Vaccinia virus Ankara recombinant for early entry MAP specific antigens (HAV) to show protection against challenge in a calf model and extensively screened for differential immunological markers associated with protection. We have shown that HAV vaccination was well tolerated, could be detected using a differentiation of infected and vaccinated animals (DIVA) test, showed no cross-reactivity with tuberculin and provided a degree of protection against challenge evidenced by a lack of faecal shedding in vaccinated animals that persisted throughout the 7 month infection period. Calves given HAV vaccination had significant priming and boosting of MAP derived antigen (PPD-J) specific CD4+, CD8+ IFN-γ producing T-cell populations and, upon challenge, developed early specific Th17 related immune responses, enhanced IFN-γ responses and retained a high MAP killing capacity in blood. During later phases post MAP challenge, PPD-J antigen specific IFN-γ and Th17 responses in HAV vaccinated animals corresponded with improvements in peripheral bacteraemia. By contrast a lack of IFN-γ, induction of FoxP3+ T cells and increased IL-1β and IL-10 secretion were indicative of progressive infection in Sham vaccinated animals. We conclude that HAV vaccination shows excellent promise as a new tool for improving control of MAP infection in cattle.

摘要

疫苗接种是控制由副结核分枝杆菌(MAP)引起的副结核病最具成本效益的措施,但目前可用的全细胞灭活制剂疗效有限,并且与结核菌素皮肤试验诊断牛结核病不兼容。我们评估了非复制型人腺病毒5和改良痘苗病毒安卡拉重组体的病毒递送方案用于早期递送MAP特异性抗原(HAV)在犊牛模型中显示对攻毒的保护作用,并广泛筛选与保护相关的差异免疫标志物。我们已经表明,HAV疫苗接种耐受性良好,可以使用感染动物和接种疫苗动物的鉴别(DIVA)试验进行检测,与结核菌素无交叉反应,并提供了一定程度的保护以抵御攻毒,这表现为接种疫苗的动物在整个7个月的感染期内粪便中均未排出病原体。接种HAV疫苗的犊牛对MAP衍生抗原(PPD-J)特异性CD4 +、CD8 + IFN-γ产生T细胞群体有显著的启动和增强作用,并且在攻毒后,出现早期特异性Th-17相关免疫反应,增强的IFN-γ反应,并在血液中保持高MAP杀伤能力。在MAP攻毒后的后期阶段,接种HAV疫苗的动物中PPD-J抗原特异性IFN-γ和Th-17反应与外周菌血症的改善相对应。相比之下,缺乏IFN-γ、诱导FoxP3 + T细胞以及增加IL-1β和IL-10分泌表明假接种动物中存在进行性感染。我们得出结论,HAV疫苗接种作为改善牛群中MAP感染控制的新工具显示出极好的前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c13/4258034/b2d91da1e305/13567_2014_112_Fig2_HTML.jpg

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