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用猪繁殖与呼吸综合征病毒样颗粒加2',3'-环鸟苷酸VacciGrade™佐剂对猪进行鼻内免疫会在病毒攻击后加重病毒血症。

Intranasal immunization of pigs with porcine reproductive and respiratory syndrome virus-like particles plus 2', 3'-cGAMP VacciGrade™ adjuvant exacerbates viremia after virus challenge.

作者信息

Van Noort Alexandria, Nelsen April, Pillatzki Angela E, Diel Diego G, Li Feng, Nelson Eric, Wang Xiuqing

机构信息

Department of Biology and Microbiology, South Dakota State University, Brookings, SD, 57007, USA.

Department of Veterinary and Biomedical Sciences, South Dakota State University, Brookings, SD, 57007, USA.

出版信息

Virol J. 2017 Apr 12;14(1):76. doi: 10.1186/s12985-017-0746-0.

Abstract

BACKGROUND

Porcine reproductive and respiratory syndrome virus (PRRSV) causes reproductive failure in pregnant sows and acute respiratory disease in young pigs. It is a leading infectious agent of swine respiratory complex, which has significant negative economic impact on the swine industry. Commercial markets currently offer both live attenuated and killed vaccines; however, increasing controversy exists about their efficacy providing complete protection. Virus-like particles (VLPs) possess many desirable features of a potent vaccine candidate and have been proven to be highly immunogenic and protective against virus infections. Here we explored the efficacy of PRRSV VLPs together with the use of a novel 2', 3'-cGAMP VacciGrade™ adjuvant.

METHODS

Animals were immunized twice intranasally with phosphate buffered saline (PBS), PRRSV VLPs, or PRRSV VLPs plus 2', 3'-cGAMP VacciGrade™ at 2 weeks apart. Animals were challenged with PRRSV-23983 at 2 weeks post the second immunization. PRRSV specific antibody response and cytokines were measured. Viremia, clinical signs, and histological lesions were evaluated.

RESULTS

PRRSV N protein specific antibody was detected in all animals at day 10 after challenge, but no significant difference was observed among the vaccinated and control groups. Surprisingly, a significantly higher viremia was observed in the VLPs and VLPs plus the adjuvant groups compared to the control group. The increased viremia is correlated with a higher interferon-α induction in the serum of the VLPs and the VLPs plus the adjuvant groups.

CONCLUSIONS

Intranasal immunizations of pigs with PRRSV VLPs and VLPs plus the 2', 3'-cGAMP VacciGrade™ adjuvant exacerbates viremia. A higher level of interferon-α production, but not interferon-γ and IL-10, is correlated with enhanced virus replication. Overall, PRRSV VLPs and PRRSV VLPs plus the adjuvant fail to provide protection against PRRSV challenge. Different dose of VLPs and alternative route of vaccination such as intramuscular injection should be explored in the future studies to fully assess the feasibility of such a vaccine platform for PRRSV control and prevention.

摘要

背景

猪繁殖与呼吸综合征病毒(PRRSV)可导致怀孕母猪繁殖失败及仔猪急性呼吸道疾病。它是猪呼吸道疾病综合征的主要病原体,对养猪业造成重大负面经济影响。目前商业市场上有减毒活疫苗和灭活疫苗;然而,关于它们提供完全保护的效果存在越来越多的争议。病毒样颗粒(VLP)具备作为一种高效疫苗候选物的许多理想特性,并且已被证明具有高度免疫原性且能抵御病毒感染。在此,我们探究了PRRSV VLP与新型2', 3'-cGAMP VacciGrade™佐剂联合使用的效果。

方法

动物每隔2周经鼻内免疫两次,分别给予磷酸盐缓冲盐水(PBS)、PRRSV VLP或PRRSV VLP加2', 3'-cGAMP VacciGrade™。在第二次免疫后2周,用PRRSV - 23983对动物进行攻毒。检测PRRSV特异性抗体反应和细胞因子。评估病毒血症、临床症状和组织学病变。

结果

攻毒后第10天,在所有动物中均检测到PRRSV N蛋白特异性抗体,但接种组和对照组之间未观察到显著差异。令人惊讶的是,与对照组相比,VLP组和VLP加佐剂组观察到显著更高的病毒血症。病毒血症增加与VLP组和VLP加佐剂组血清中更高的α干扰素诱导相关。

结论

用PRRSV VLP和VLP加2', 3'-cGAMP VacciGrade™佐剂经鼻内免疫猪会加剧病毒血症。更高水平的α干扰素产生,但不是γ干扰素和白细胞介素-10,与病毒复制增强相关。总体而言,PRRSV VLP和PRRSV VLP加佐剂未能提供抵御PRRSV攻毒的保护。未来研究应探索不同剂量的VLP和替代接种途径,如肌肉注射,以全面评估这种疫苗平台用于控制和预防PRRSV的可行性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/deda/5389191/214da414c3b8/12985_2017_746_Fig1_HTML.jpg

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