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Molecular basis for dengue virus broad cross-neutralization by humanized monoclonal antibody 513

机译:Dengue病毒的分子基础通过人源化单克隆抗体的繁体交叉中和513

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Dengue is a widespread viral disease with 3.6 billion people at risk worldwide. Humanized monoclonal antibody (mAb) 513, currently undergoing clinical trials in Singapore, targets an epitope on the envelope protein domain III exposed at the surface of the viral particle. This antibody potently neutralizes all four dengue virus serotypes in a humanized mouse model that recapitulates human dengue infection, without signs of antibody-mediated enhancement of the disease. The crystal structure of single-chain variable fragment (scFv) 513 bound to the envelope protein domain III from dengue virus serotype 4 was used as a template to explore the molecular origins of the broader cross-reactivity and increased in vivo potency of mAb 513, compared to the parent murine mAb 4E11, using molecular dynamics simulations and network analyses. These two methods are a powerful complement to existing structural and binding data and detail specific interactions that underpin the differential binding of the two antibodies. We found that a Glu at position H55 (GluH55) from the second Complementarity Determining Region of the Heavy chain (CDR-H2) which corresponds to Ala in 4E11, is a major contributor to the enhancement in the interactions of mAb 513 compared to 4E11. Importantly, we also validate the importance of GluH55 using site-directed mutagenesis followed by isothermal titration calorimetry measurements.
机译:登革热是一种普遍的病毒疾病,全球风险36亿人。人类源化单克隆抗体(MAB)513,目前正在进行新加坡的临床试验,靶向在病毒颗粒表面暴露在曝光的包膜蛋白结构域III上。该抗体在人源化的小鼠模型中易于中和所有四种登革热病毒血清型,旨在概括人类登革症感染,而无需抗体介导的疾病的增强。用登革热病毒血清型4与包络蛋白结构域III结合的单链可变片段(SCFV)513的晶体结构用作模板,以探讨更广泛的交叉反应性的分子起源,促进MAB 513的体内效力增加,与父鼠MAB 4E11相比,使用分子动力学模拟和网络分析。这两种方法是对现有结构和结合数据的强大补充和细节,使得支撑两种抗体的差异结合。我们发现,来自对应于4E11中的ALA的重链(CDR-H2)的第二互补确定区域的位置H55(GLUH55)的GLU是MAb 513相互作用的增强的主要因素与4E11相比。重要的是,我们还验证了GLUH55使用现场定向诱变的重要性,然后是等温滴定热量测量测量。

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