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南非SAT3型口蹄疫病毒抗原变异的遗传基础

Genetic Basis of Antigenic Variation of SAT3 Foot-And-Mouth Disease Viruses in Southern Africa.

作者信息

Maake Lorens, Harvey William T, Rotherham Lia, Opperman Pamela, Theron Jacques, Reeve Richard, Maree Francois F

机构信息

Vaccine and Diagnostic Development Programme, Onderstepoort Veterinary Institute, Agricultural Research Council, Pretoria, South Africa.

Department of Biochemistry, Genetics and Microbiology, Faculty of Agricultural and Natural Sciences, University of Pretoria, Pretoria, South Africa.

出版信息

Front Vet Sci. 2020 Sep 8;7:568. doi: 10.3389/fvets.2020.00568. eCollection 2020.

Abstract

Foot-and-mouth disease (FMD) continues to be a major burden for livestock owners in endemic countries and a continuous threat to FMD-free countries. The epidemiology and control of FMD in Africa is complicated by the presence of five clinically indistinguishable serotypes. Of these the Southern African Territories (SAT) type 3 has received limited attention, likely due to its restricted distribution and it being less frequently detected. We investigated the intratypic genetic variation of the complete P1 capsid-coding region of 22 SAT3 viruses and confirmed the geographical distribution of five of the six SAT3 topotypes. The antigenic cross-reactivity of 12 SAT3 viruses against reference antisera was assessed by performing virus neutralization assays and calculating the r-values, which is a ratio of the heterologous neutralizing titer to the homologous neutralizing titer. Interestingly, cross-reactivity between the SAT3 reference antisera and many SAT3 viruses was notably high (r-values >0.3). Moreover, some of the SAT3 viruses reacted more strongly to the reference sera compared to the homologous virus (r-values >1). An increase in the avidity of the reference antisera to the heterologous viruses could explain some of the higher neutralization titers observed. Subsequently, we used the antigenic variability data and corresponding genetic and structural data to predict naturally occurring amino acid positions that correlate with antigenic changes. We identified four unique residues within the VP1, VP2, and VP3 proteins, associated with a change in cross-reactivity, with two sites that change simultaneously. The analysis of antigenic variation in the context of sequence differences is critical for both surveillance-informed selection of effective vaccines and the rational design of vaccine antigens tailored for specific geographic localities, using reverse genetics.

摘要

口蹄疫(FMD)仍然是流行国家牲畜养殖户的主要负担,也是对口蹄疫无疫国家的持续威胁。非洲口蹄疫的流行病学和防控因存在五种临床无法区分的血清型而变得复杂。其中,南非领土(SAT)3型受到的关注有限,这可能是由于其分布受限且检测频率较低。我们研究了22株SAT3病毒完整P1衣壳编码区的型内基因变异,并确认了六种SAT3拓扑型中五种的地理分布。通过进行病毒中和试验并计算r值(即异源中和滴度与同源中和滴度之比),评估了12株SAT3病毒与参考抗血清的抗原交叉反应性。有趣的是,SAT3参考抗血清与许多SAT3病毒之间的交叉反应性显著较高(r值>0.3)。此外,一些SAT3病毒与同源病毒相比,对参考血清的反应更强(r值>1)。参考抗血清对异源病毒亲和力的增加可以解释观察到的一些较高中和滴度。随后,我们利用抗原变异性数据以及相应的遗传和结构数据来预测与抗原变化相关的天然氨基酸位置。我们在VP1、VP2和VP3蛋白中鉴定出四个独特的残基,它们与交叉反应性的变化相关,其中两个位点同时发生变化。在序列差异背景下分析抗原变异对于基于监测选择有效的疫苗以及利用反向遗传学为特定地理区域量身定制疫苗抗原的合理设计都至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/909d/7506032/e44792b432a9/fvets-07-00568-g0001.jpg

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