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传染性支气管炎病毒种群结构决定免疫反应和保护作用。

Infectious Bronchitis Virus Population Structure Defines Immune Response and Protection.

作者信息

Zegpi R A, Joiner K S, van Santen V L, Toro H

机构信息

Department of Pathobiology, Auburn University College of Veterinary Medicine, Auburn, AL 36830.

Department of Pathobiology, Auburn University College of Veterinary Medicine, Auburn, AL 36830,

出版信息

Avian Dis. 2020 Mar;64(1):60-68. doi: 10.1637/0005-2086-64.1.60.

Abstract

A commercial Arkansas (Ark) Delmarva Poultry Industry (DPI)-type vaccine and a more homogeneous population of that vaccine obtained previously through adaptation to chicken embryo kidney (CEK) cells (CEK-ArkDPI) were used as a model to further understand the impact of population genetic structure on generation of immune responses and protection. In a first experiment, vaccinated chickens were challenged with an IBV Ark99-type virulent strain (AL/4614/98). Despite extensive sequence similarity between the vaccines, the more heterogeneous commercial ArkDPI was more efficient at reducing viral loads in challenged chickens, while respiratory signs and tracheal lesions were reduced similarly by either vaccine. A distinct subpopulation of the Ark challenge virus showing asparagine at S1 position 56 was consistently negatively selected by immune pressure originating from vaccination with either vaccine. Antibody levels and antibody avidity to Ark-type S1 protein were greater in CEK-ArkDPI-vaccinated chickens compared to chickens vaccinated with the more diverse commercial ArkDPI vaccine. Synchronous replication of a homogeneous virus population likely elicits clonal expansion and affinity maturation of a greater number of responding B cells compared to a diverse virus population continuously changing its proportion of phenotypes during replication. The results of a second experiment showed that during initial vaccine virus replication (24 and 48 hr postvaccination), the virus population showing increased diversity (commercial ArkDPI) achieved higher concentrations of IBV RNA in the trachea compared to the more homogenous virus. mRNA expression of genes associated with innate immune responses in the trachea 48 hr postvaccination generally showed greater upregulation in chickens vaccinated with the heterogeneous commercial ArkDPI vaccine compared to the CEK-adapted virus. The greater upregulation of these genes is likely associated with higher virus replication achieved by the heterogeneous commercial vaccine. Thus, while the adaptive antibody response was favored by the more homogenous structure of the CEK-ArkDPI vaccine population (higher antibody levels and antibody avidity), the innate immune response was favored by the more diverse viral population of the commercial ArkDPI. We confirmed previous results that distinct subpopulations in wild Ark challenge virus become selected by immune pressure originating from vaccination, and we concluded that the population structure of IBV vaccines impacts innate immune response, antibody avidity, and protection.

摘要

使用一种商业化的阿肯色州(Ark)德尔马瓦家禽业(DPI)型疫苗以及先前通过适应鸡胚肾(CEK)细胞获得的该疫苗的更均匀群体(CEK-ArkDPI)作为模型,以进一步了解群体遗传结构对免疫反应产生和保护的影响。在第一个实验中,给接种疫苗的鸡用传染性支气管炎病毒(IBV)Ark99型强毒株(AL/4614/98)进行攻毒。尽管两种疫苗之间存在广泛的序列相似性,但更具异质性的商业化ArkDPI在降低攻毒鸡的病毒载量方面更有效,而两种疫苗对呼吸道症状和气管损伤的减轻效果相似。Ark攻毒病毒中在S1蛋白第56位显示天冬酰胺的一个独特亚群始终受到来自任何一种疫苗接种产生的免疫压力的负选择。与接种更具多样性的商业化ArkDPI疫苗的鸡相比,接种CEK-ArkDPI疫苗的鸡对Ark型S1蛋白的抗体水平和抗体亲和力更高。与在复制过程中不断改变其表型比例的多样化病毒群体相比,均匀病毒群体的同步复制可能引发更多应答B细胞的克隆扩增和亲和力成熟。第二个实验的结果表明,在疫苗病毒初始复制期间(接种后24小时和48小时),与更均匀的病毒相比,显示出多样性增加的病毒群体(商业化ArkDPI)在气管中实现了更高浓度的IBV RNA。接种后48小时,气管中与先天免疫反应相关基因的mRNA表达通常在接种异质性商业化ArkDPI疫苗的鸡中比接种CEK适应病毒的鸡表现出更大的上调。这些基因的更大上调可能与异质性商业化疫苗实现的更高病毒复制有关。因此,虽然适应性抗体反应受到CEK-ArkDPI疫苗群体更均匀结构的青睐(更高的抗体水平和抗体亲和力),但先天免疫反应受到商业化ArkDPI更多样化病毒群体的青睐。我们证实了先前的结果,即野生Ark攻毒病毒中的独特亚群会受到疫苗接种产生的免疫压力的选择,并且我们得出结论,IBV疫苗的群体结构会影响先天免疫反应、抗体亲和力和保护作用。

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