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Resistance analysis of an antibody that selectively inhibits dengue virus serotype-1

机译:选择性抑制登革热病毒血清型1的抗体的耐药性分析

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The four serotypes of dengue virus (DENV) are the causative agents of the most prevalent mosquito-borne viral disease in human. No clinically approved antiviral therapy is currently available. Therapeutic antibodies represent a viable approach for potential treatment of DENV infection. We recently isolated a human monoclonal antibody (HM14c10) that selectively neutralizes DENV serotype 1 (DENV-1), but not serotypes 2, 3, and 4. Here we report the resistance profile of DENV-1 against HM14c10 in cell culture. Escape mutant viruses readily emerged by culturing wild-type DENV-1 in the presence of the HM14c10 antibody. Sequencing of resistant viruses revealed a single T51K substitution in the domain I/II hinge region of the viral envelope protein. Residue T51 is located within the HM14c10 epitope and is highly conserved among various DENV-1 isolates. Recombinant DENV-1 containing the T51K mutation could not be neutralized by HM14c10 in vitro or in vivo. Biochemical assay revealed that the T51K mutation completely abolished the antibody binding to the DENV-1 virion. Collectively, the results demonstrate that a single amino acid change in DENV envelope protein can confer resistance to a potent antibody through abolishing the antibody-virus interaction.
机译:登革热病毒(DENV)的四种血清型是人类中最普遍的蚊媒病毒性疾病的病原体。当前没有临床批准的抗病毒治疗。治疗性抗体代表了潜在治疗DENV感染的可行方法。我们最近分离了人单克隆抗体(HM14c10),该抗体选择性中和DENV血清型1(DENV-1),但不中和血清型2、3和4。在这里,我们报道DENV-1在细胞培养物中对HM14c10的耐药性。通过在HM14c10抗体的存在下培养野生型DENV-1,很容易出现逃脱突变病毒。抗性病毒的测序表明,在病毒被膜蛋白的结构域I / II铰链区中存在单个T51K取代。 T51残基位于HM14c10表位内,在各种DENV-1分离株中高度保守。 HM14c10无法在体内或体外中和含有T51K突变的重组DENV-1。生化分析表明,T51K突变完全消除了与DENV-1病毒体结合的抗体。总体而言,结果表明,DENV包膜蛋白中的单个氨基酸变化可通过消除抗体与病毒的相互作用而赋予对有效抗体的抗性。

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