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基于 GI-23 谱系的不同批次传染性支气管炎病毒 (IBV) 疫苗中的病毒亚群变异性:对现场的影响。

Viral subpopulation variability in different batches of Infectious bronchitis virus (IBV) vaccines based on GI-23 lineage: Implications for the field.

机构信息

Department of Animal Medicine, Production and Health, University of Padova, Legnaro, PD, Italy.

Ceva Phylaxia, Szállás u. 5., 1107 Budapest, Hungary.

出版信息

Virus Res. 2022 Oct 2;319:198877. doi: 10.1016/j.virusres.2022.198877. Epub 2022 Jul 22.

Abstract

The control of infectious bronchitis (IB) is largely based on routine vaccine administration, often using live-attenuated vaccines. However, their capability to replicate and be transmitted among animals and farms implies significant risks. The detection of strains genetically related to vaccines complicates the diagnostic process and understanding of the viral molecular epidemiology. Moreover, reversion to virulence and associated clinical outbreaks can occur although the underlying mechanism are often unknown. In the present study, three vaccine vials, based on IBV GI-23 lineage (also known as Variant2) were deep sequenced through Next Generation Sequencing (NGS) to investigate the presence and features of viral subpopulations. To elucidate the consequences in the field and identify potential markers suitable for a DIVA strategy, the S1 sequences of strains originating from farms in different countries were sequenced and classified based on the knowledge of their vaccination history and similarity with the applied vaccine. Although all considered vaccine batches shared the same consensus sequence, different subpopulations were identified suggesting independent and poorly constrained evolutionary processes. When compared with strains sampled from farms, the vaccine consensus sequences and the respective subpopulations clustered with vaccine strains and no genetic features were consistently shared with field strains. Therefore, if vaccine-induced outbreaks occur, they are more likely to originate from in vivo evolution rather than selection of already present subpopulations. Although some amino acid residues were most commonly detected in field or vaccine strains, no consistent marker could be identified. The occurrence of subpopulations within IBV GI-23-based vaccines and variability featuring different production batches was demonstrated. Being such a phenomenon apparently driven by random genetic drift rather than directional selection, the differentiation between field and vaccine-derived strains appears extremely challenging based on sequence analysis alone. The knowledge of farm management and vaccination history should thus be considered for a proper epidemiological investigation.

摘要

传染性支气管炎(IB)的控制主要基于常规疫苗接种,通常使用活疫苗。然而,它们在动物和农场之间复制和传播的能力意味着存在重大风险。疫苗相关遗传株的检测使诊断过程复杂化,并增加了对病毒分子流行病学的理解难度。此外,尽管潜在机制通常未知,但毒力恢复和相关临床暴发仍可能发生。在本研究中,通过下一代测序(NGS)对基于 IBV GI-23 谱系(也称为 Variant2)的三瓶疫苗进行了深度测序,以研究病毒亚群的存在和特征。为了阐明田间的后果并确定适合 DIVA 策略的潜在标志物,对源自不同国家农场的菌株的 S1 序列进行了测序和分类,依据其接种史和与应用疫苗的相似性。尽管所有考虑的疫苗批次都具有相同的共识序列,但仍鉴定出不同的亚群,表明存在独立且受限制较少的进化过程。与从农场采样的菌株相比,疫苗共识序列及其各自的亚群与疫苗株聚类,与田间菌株没有一致的遗传特征共享。因此,如果发生疫苗引起的暴发,它们更可能源于体内进化,而不是选择已存在的亚群。尽管在田间或疫苗株中最常检测到某些氨基酸残基,但没有一致的标志物可以确定。证明了基于 IBV GI-23 的疫苗中存在亚群和不同生产批次的变异性。由于这种现象显然是由随机遗传漂变驱动,而不是定向选择,因此仅基于序列分析,区分田间和疫苗衍生株似乎极具挑战性。因此,应考虑农场管理和疫苗接种史的知识,以进行适当的流行病学调查。

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