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首页> 外文期刊>The Journal of Biochemistry >Characterization of human single-chain antibodies against highly pathogenic avian influenza H5N1 viruses: mimotope and neutralizing activity.
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Characterization of human single-chain antibodies against highly pathogenic avian influenza H5N1 viruses: mimotope and neutralizing activity.

机译:针对高致病性禽流感H5N1病毒的人单链抗体的表征:模拟表位和中和活性。

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The development of new therapeutic targets and strategies to control highly pathogenic avian influenza (HPAI) H5N1 virus infection in humans is urgently needed. Neutralizing recombinant human antibodies would provide important agents for immunotherapy on human H5N1 virus infection and definition of the critical mimotope for vaccine development. In this study, we have characterized an anti-H5-specific scFv clone, 3D1 from the human-scFv-displaying phage library. 3D1 blocked the binding of H5-Fc to MDCK cells in flow cytometry and neutralized H5N1 subtype influenza A viruses in a microneutralization assay. Employing a peptide-displaying phage library, Ph.D-12, the mimotope was determined to be at #128-131 and #204-211 of H5, which are silic acid-binding regions. In consistency with this result, 3D1 binds the recombinant sugar-binding domain (#50G-#272E) produced by a baculovirus vector. The 3D1 antibody employs the germline gene VH1-23. As this antibody is the first human anti-H5 scFv clearly defined on the sugar-binding epitope, it allows us to investigate the influence of amino acid substitutions in this region on the determination of the binding specificity to either sialic acid alpha2,6-galactose (SA alpha2,6Gal) or sialic acid alpha2,3-galactose (SA alpha2,3Gal) providing new insight for the development of effective H5N1 pandemic vaccines.
机译:迫切需要开发新的治疗靶标和控制人类高致病性禽流感(HPAI)H5N1病毒感染的策略。中和重组人抗体将为人H5N1病毒感染的免疫治疗提供重要试剂,并为疫苗开发确定关键的模拟表位。在这项研究中,我们已经从展示人scFv的噬菌体文库中表征了抗H5特异性的scFv克隆3D1。 3D1在流式细胞仪中阻断了H5-Fc与MDCK细胞的结合,并在微中和试验中中和了H5N1亚型甲型流感病毒。利用展示肽的噬菌体文库Ph.D-12,确定模拟表位位于H5的#128-131和#204-211,它们是硅酸结合区。与该结果一致,3D1结合杆状病毒载体产生的重组糖结合结构域(#50G-#272E)。 3D1抗体使用种系基因VH1-23。由于该抗体是在糖结合表位上明确定义的首个人类抗H5 scFv抗体,因此它使我们能够研究该区域氨基酸取代对唾液酸α2,6-半乳糖结合特异性测定的影响(SA alpha2,6Gal)或唾液酸alpha2,3-半乳糖(SA alpha2,3Gal)为开发有效的H5N1大流行疫苗提供了新的见识。

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