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首页> 外文期刊>Clinical and vaccine immunology: CVI >Monoclonal antibodies that bind to common epitopes on the dengue virus type 2 nonstructural-1 and envelope glycoproteins display weak neutralizing activity and differentiated responses to virulent strains: implications for pathogenesis and vaccines.
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Monoclonal antibodies that bind to common epitopes on the dengue virus type 2 nonstructural-1 and envelope glycoproteins display weak neutralizing activity and differentiated responses to virulent strains: implications for pathogenesis and vaccines.

机译:单克隆抗体结合常见的抗原表位登革病毒2型nonstructural-1和包膜糖蛋白显示弱的中和活动和差异化的毒性反应对发病机理和特性:影响疫苗。

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The abilities of monoclonal antibodies (MAbs) that bind to defined sequential epitopes on the dengue virus (DENV) nonstructural-1 (NS1) glycoproteins to cross-react with epitopes on the DENV envelope (E) glycoproteins were investigated. In this study, some of these MAbs cross-reacted with the DENV type 2 (DENV-2) E glycoprotein and with synthetic peptides representing X-ray crystallographically confirmed surface-exposed regions on this glycoprotein. MAb 1G5.3 cross-reacted with the flavivirus-conserved 101-WGNGCGLFG-109 fusion sequence, the 273-SSGNL-277 DENV-2 hinge region sequence, and the 156-GKHGKEIKIT-165 sequence of virulent DENV-2 strains. MAb 1G5.4-A1-C3 cross-reacted with the 67-NTTTESRCPT-76 and 156-GKHGKEIKIT-165 sequences of virulent DENV-2 strains, the 338-EIMDLDNRHV-347 sequence from a highly virulent DENV-2 (M2) strain, and two epitopes on a virulent DENV-3 strain (288-KMDKLELKG-296 and 323-RVEYRGEDAP-332), which all contained target ELK/KLE-type motifs (underlined). These MAbs showed reduced cross-reactions with the corresponding sequences from weakly pathogenic strains of all four DENV serotypes and had either no (MAb 1G5.4-A1-C3) or weak (MAb 1G5.3) neutralizing activity against them. MAb 1G5.3 more strongly neutralized DENV-2 strains with higher pathogenic capacities, while MAb 1G5.4-A1-C3 showed increasing neutralizing titers against the virulent DENV-3 strain and the moderately virulent and highly virulent (M2) DENV-2 strains. These cross-reactions with the E glycoprotein accord with the observation that MAb 1G5.3 caused dramatic and lethal antibody-enhanced replication (AER) of a DENV-2 strain in vivo. Together with in vivo AER studies of these DENV strains using MAb 1G5.4-A1-C3, these results may account for the increased pathogenic capacities of such strains, which is likely to have important implications for pathogenesis and vaccines.
机译:单克隆抗体(mab)的能力绑定到登革热的定义顺序表位病毒(DENV) nonstructural-1 (NS1)糖蛋白DENV信封和抗原表位交叉反应(E)糖蛋白。研究中,其中一些马伯的交叉作用DENV 2型(DENV-2) E糖蛋白和合成肽代表x射线结晶学证实surface-exposed地区的糖蛋白。与flavivirus-conserved交叉作用101 - wgngcglfg - 109融合序列,273 - ssgnl - 277 DENV-2铰链区序列,和156 - gkhgkeikit - 165序列的强DENV-2菌株。67 - ntttesrcpt - 76和156 - gkhgkeikit - 165毒性DENV-2菌株的序列从一个高度338 - eimdldnrhv - 347序列毒性DENV-2 (M2),和两个抗原表位一个致命DENV-3应变(288 - kmdklelkg - 296和323 - rveyrgedap - 332),它包含所有的目标麋鹿/ KLE-type图案(下划线)。显示减少的交叉反应对应的序列从弱致病性所有四个DENV菌株血清型,要么没有(MAb 1 g5.4-a1-c3)或弱(MAb 1 g5.3)中和活动。更强烈中和DENV-2菌株更高的致病能力,而马伯1 g5.4-a1-c3显示增加中和滴度对毒性和DENV-3压力适度的毒性和高毒性(M2)DENV-2菌株。糖蛋白符合马伯的观察1 g5.3造成戏剧性的和致命的DENV-2 antibody-enhanced复制(AER)体内。这些使用马伯1 g5.4-a1-c3 DENV菌株,这些结果可能占增加致病能力的菌株,可能有重要的意义发病机理和疫苗。

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