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Genetic characterization of the cell-adapted PanAsia strain of foot-and-mouth disease virus O/Fujian/CHA/5/99 isolated from swine

机译:分离自猪的口蹄疫病毒O / Fujian / CHA / 5/99的适应细胞的泛亚株的遗传特征

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Background According to Office International Des Epizooties (OIE) Bulletin, the PanAsia strain of Foot-and-Mouth Disease Virus (FMDV) was invaded into the People's Republic of China in May 1999. It was confirmed that the outbreaks occurred in Tibet, Hainan and Fujian provinces. In total, 1280 susceptible animals (68 cattle, 1212 swine) were destroyed for the epidemic control. To investigate the distinct biological properties, we performed plaque assay, estimated the pathogenicity in suckling mice and determined the complete genomic sequence of FMDV swine-isolated O/Fujian/CHA/5/99 strain. In addition, a molecular modeling was carried out with the external capsid proteins. Results The pathogenicity study showed that O/Fujian/CHA/5/99 had high virulence with respect to infection in 3-day-old suckling-mice (LD50 = 10-8.3), compared to O/Tibet/CHA/1/99 (LD50 = 10-7.0) which isolated from bovine. The plaque assay was distinguishable between O/Fujian/CHA/5/99 and O/Tibet/CHA/1/99 by their plaque phenotypes. O/Fujian/CHA/5/99 formed large plaque while O/Tibet/CHA/1/99 formed small plaque. The 8,172 nucleotides (nt) of O/Fujian/CHA/5/99 was sequenced, and a phylogenetic tree was generated from the complete nucleotide sequences of VP1 compared with other FMDV reference strains. The identity data showed that O/Fujian/CHA/5/99 is closely related to O/AS/SKR/2002 (94.1% similarity). Based on multiple sequence alignments, comparison of sequences showed that the characteristic nucleotide/amino acid mutations were found in the whole genome of O/Fujian/CHA/5/99. Conclusion Our finding suggested that C275T substitution in IRES of O/Fujian/CHA/5/99 may induce the stability of domain 3 for the whole element function. The structure prediction indicated that most of 14 amino acid substitutions are fixed in the capsid of O/Fujian/CHA/5/99 around B-C loop and E-F loop of VP2 (antigenic site 2), and G-H loop of VP1 (antigenic site 1), respectively. These results implicated that these substitutions close to heparin binding sites (E136G in VP2, A174 S in VP3) and at antigenic site 1 (T142A, A152T and Q153P in VP1) may influence plaque size and the pathogenicity to suckling mice. The potential of genetic characterization would be useful for microevolution and viral pathogenesis of FMDV in the further study.
机译:背景信息根据国际兽疫局(OIE)公告,1999年5月,泛亚株口蹄疫病毒(FMDV)入侵了中华人民共和国。已确认该暴发发生在西藏,海南和中国。福建省。为了控制流行,总共销毁了1280只易感动物(68头牛,1212头猪)。为了研究独特的生物学特性,我们进行了噬菌斑测定,评估了乳鼠的致病性并确定了FMDV猪分离的O / Fujian / CHA / 5/99菌株的完整基因组序列。另外,用外部衣壳蛋白进行了分子建模。结果致病性研究表明,O / Fujian / CHA / 5/99对3天大的乳鼠(LD 50 = 10 -8.3 ),与从牛中分离出的O / Tibet / CHA / 1/99(LD50 = 10 -7.0 )相比。通过噬菌斑表型,噬菌斑试验在O / Fujian / CHA / 5/99和O / Tibet / CHA / 1/99之间是可区分的。 O / Fujian / CHA / 5/99形成大斑块,而O / Tibet / CHA / 1/99形成小斑块。对O / Fujian / CHA / 5/99的8,172个核苷酸(nt)进行了测序,与其他FMDV参考菌株相比,从VP1的完整核苷酸序列生成了系统树。身份数据表明,O / Fujian / CHA / 5/99与O / AS / SKR / 2002密切相关(相似性为94.1%)。基于多个序列比对,序列比较表明在O / Fujian / CHA / 5/99的整个基因组中发现了特征性核苷酸/氨基酸突变。结论我们的发现表明O / Fujian / CHA / 5/99的IRES中的C275T取代可能诱导结构域3整个元素功能的稳定性。结构预测表明,在VP2的BC环和EF环(抗原位点2)和VP1的GH环(抗原位点1)周围,O / Fujian / CHA / 5/99的衣壳中固定了14个氨基酸的大部分。 , 分别。这些结果暗示,这些置换靠近肝素结合位点(VP2中为E136G,VP3中为A174 S)和抗原性位点1(VP1中为T142A,A152T和Q153P)可能影响菌斑大小和对乳鼠的致病性。遗传表征的潜力将对进一步研究FMDV的微进化和病毒发病机制有用。

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