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Evaluation of protection induced by immunisation of domestic pigs with deletion mutant African swine fever virus BeninΔMGF by different doses and routes

机译:不同剂量和途径用缺失突变型非洲猪瘟病毒贝宁ΔMGF免疫家猪的保护性评价

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摘要

A live attenuated African swine fever virus (ASFV) vaccine candidate, produced by deletion of several genes belonging to multi-gene families MGF360 and 505 from virulent Benin 97/1 strain (BeninΔMGF), induces protection in pigs against parental virulent strain. In order to better define the safety and efficacy of this attenuated vaccine candidate and to understand protective mechanisms, we extended previous studies by intramuscular immunisation of pigs with the deletion mutant BeninΔMFG at different doses (102, 103, 104 TCID50), together with intranasal immunisation at the 103 dose. Results demonstrated a strong correlation between both doses and routes of immunisation of BeninΔMFG and the percentage of protection achieved, the onset of clinical signs, the viremia levels reached and the onset of death in non-protected pigs. The results show that the intramuscular route using high doses (104 TCID50) is the best option for immunisation. Only transient increase in temperature associated with a peak of virus genome levels was observed in most pigs after immunisation. Then, virus genome levels progressively decreased throughout the experiment until reaching low or undetectable levels in those protected pigs that survived after challenge. The IgM antibody responses following immunisation were detected between day 7–10 post-immunisation and remained at elevated levels for 10–18 days in most pigs before dropping. IgG was detected from day 15 to 21 post-immunisation and maintained at increased levels for the remainder of the experiment in most pigs. Induction of IFNγ and IL-10 was detected by ELISA in sera from some pigs immunised with 103 TCID50 by intramuscular or intranasal route at early times post-immunisation. IL-10 was also detected in serum from some non-protected pigs included in these groups after challenge.
机译:通过从强毒贝宁97/1品系(BeninΔMGF)中删除多个属于多基因家族MGF360和505的基因产生的减毒非洲猪瘟活疫苗(ASFV)候选疫苗,可诱导猪对亲本强毒株的保护。为了更好地确定这种减毒候选疫苗的安全性和有效性并了解保护机制,我们通过用不同剂量(10 2 ,10 < sup> 3 ,10 4 TCID50)以及10 3 剂量的鼻内免疫。结果表明,贝宁ΔMFG的剂量和免疫途径与获得保护的百分比,临床体征的发作,达到的病毒血症水平和未受保护的猪的死亡之间都具有很强的相关性。结果表明,高剂量(10 4 TCID50)的肌内途径是免疫的最佳选择。免疫后大多数猪只观察到与病毒基因组水平峰值相关的温度的短暂升高。然后,病毒基因组水平在整个实验过程中逐渐降低,直到在攻击后存活的受保护猪中达到低水平或无法检测到。在免疫后7-10天之间检测到免疫后的IgM抗体反应,并且在下降之前,大多数猪的IgM抗体水平在升高的水平下保持10-18天。从免疫后第15天到第21天检测到IgG,在其余实验中,大多数猪的IgG保持在升高的水平。在免疫后早期,通过肌内或鼻内途径用10 3 TCID50免疫的一些猪的血清中通过ELISA检测了IFNγ和IL-10的诱导。攻击后,在这些组中包括的一些未保护的猪的血清中也检测到IL-10。

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