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Humanized antibodies with broad-spectrum neutralization to avian influenza virus H5N1.

机译:对禽流感病毒H5N1具有广谱中和的人源化抗体。

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Hemagglutinin (HA), the major antigen on the surface of influenza viruses, is the primary target for neutralizing antibodies and vaccine design. However, frequent mutations in this gene allow the virus to evade host immune responses and conventional prophylaxis and treatment. In this report, we humanized 4D1 and 10F7 mouse monoclonal antibodies (mAbs) that, we had previously shown to display broad-spectrum neutralization to avian H5N1 virus. The genes of variable (V) regions of 4D1 and 10F7 mAbs were combined with constant region of human antibody to construct the chimeric antibodies (cAbs). The results of hemagglutinin inhibition (HI) and neutralization assays showed that 4D1 and 10F7 cAbs were functional and retained broad-spectrum reactivity. Antibody competitive ELISA and affinity tests indicated that the cAbs recognized the same epitope as the parent mAbs with similar affinity. In animal experiments, the 10F7 cAb showed full protection against lethal challenge of highly virulent avian H5N1 virus, A/BH Goose/QH/15C/2005, in all infected mice. These humanized broad-spectrum antibodies may be potentially important for the control of both current and future antigenic variants of H5N1 virus.
机译:血凝素(HA)是流感病毒表面的主要抗原,是中和抗体和疫苗设计的主要目标。但是,该基因的频繁突变使病毒能够逃避宿主的免疫反应以及常规的预防和治疗。在本报告中,我们将以前显示对禽类H5N1病毒显示广谱中和的4D1和10F7小鼠单克隆抗体(mAbs)人源化。将4D1和10F7 mAb的可变(V)区基因与人抗体的恒定区结合,以构建嵌合抗体(cAb)。血凝素抑制(HI)和中和测定的结果表明4D1和10F7 cAb具有功能并保留了广谱反应性。抗体竞争性ELISA和亲和力测试表明,cAb与亲本mAb识别具有相同亲和力的相同表位。在动物实验中,10F7 cAb在所有感染的小鼠中均显示出对高毒性禽H5N1病毒A / BH Goose / QH / 15C / 2005的致命攻击的全面保护。这些人源化的广谱抗体对于控制H5N1病毒的当前和未来抗原变体都可能潜在重要。

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