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Priming with a DNA vaccine and boosting with an inactivated vaccine enhance the immune response against infectious bronchitis virus

机译:用DNA疫苗引发和灭活疫苗加强免疫可增强针对传染性支气管炎病毒的免疫反应

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摘要

The methods of repeated immunization with inactivated vaccines have been used widely to increase antibody protection against infectious bronchitis virus (IBV). However, compared with DNA vaccines, these methods usually induce poor cellular responses. In the present study, specific pathogen-free (SPF) chickens were immunized intramuscularly with a DNA vaccine carrying the main IBV structural genes (pVAX1-S1, pVAX1-M, and pVAX1-N, respectively) and boosted with the IBV M41 strain inactivated vaccine to assess whether such a new strategy could enhance the immune responses against IBV. The protection efficacy of the DNA vaccine carrying different structural genes for priming was evaluated further. The chickens were immunized primely on day 7 and boosted 2 weeks later. After that, distribution of the DNA vaccine , the percentage of CD4+CD3+ and CD8+CD3+ subgroups of peripheral blood T-lymphocytes, and the specific IgG and virus neutralizing antibodies were measured. Chickens were then challenged by the nasal–ocular route with the IBV M41 strain 4 weeks after booster immunization. The results demonstrated that priming with a DNA vaccine encoding nucleocapsid protein (pVAX1-N) and boosting with the inactivated IBV vaccine led to the dramatic augmentation of humoral and cellular responses, and provided up to 86.7% rate of immune protection, providing an effective approach to protect chickens from IBV.
机译:用灭活疫苗重复免疫的方法已被广泛用于增强针对传染性支气管炎病毒(IBV)的抗体保护。但是,与DNA疫苗相比,这些方法通常会引起较差的细胞反应。在本研究中,使用携带主要IBV结构基因(分别为pVAX1-S1,pVAX1-M和pVAX1-N)的DNA疫苗肌肉注射特定无病原体(SPF)的鸡,并用灭活的IBV M41株加强免疫疫苗以评估这种新策略是否可以增强针对IBV的免疫反应。进一步评估了携带不同结构基因的DNA疫苗的保护效果。在第7天对鸡进行免疫接种,并在2周后加强免疫。之后,测量DNA疫苗的分布,外周血T淋巴细胞的CD4 + CD3 +和CD8 + CD3 +亚群的百分比,以及特异性IgG和病毒中和抗体。加强免疫4周后,用IBV M41毒株通过鼻-眼途径攻击鸡。结果表明,用编码核衣壳蛋白(pVAX1-N)的DNA疫苗引发和用灭活的IBV疫苗加强免疫可显着增强体液和细胞应答,并提供高达86.7%的免疫保护率,提供了一种有效的方法保护鸡免受IBV感染。

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