首页> 外文期刊>Antiviral Research >A humanised murine monoclonal antibody with broad serogroup specificity protects mice from challenge with Venezuelan equine encephalitis virus.
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A humanised murine monoclonal antibody with broad serogroup specificity protects mice from challenge with Venezuelan equine encephalitis virus.

机译:具有广泛血清群特异性的人源化鼠类单克隆抗体可以保护小鼠免受委内瑞拉马脑炎病毒的攻击。

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In murine models of Venezuelan equine encephalitis virus (VEEV) infection, the neutralising monoclonal antibody 1A3B-7 has been shown to be effective in passive protection from challenge by the aerosol route with serogroups I, II and Mucambo virus (formally VEE complex subtype IIIA). This antibody is able to bind to all serogroups of the VEEV complex when used in ELISA and therefore is an excellent candidate for protein engineering in order to derive a humanised molecule suitable for therapeutic use in humans. A Complementarity Determining Region (CDR) grafting approach using human germline IgG frameworks was used to produce a panel of humanised variants of 1A3B-7, from which a single candidate molecule with retained binding specificity was identified. Evaluation of humanised 1A3B-7 (Hu1A3B-7) in in vitro studies indicated that Hu1A3B-7 retained both broad specificity and neutralising activity. Furthermore, in vivo experiments showed that Hu1A3B-7 successfully protected mice against lethal subcutaneous and aerosol challenges with VEEV strain TrD (serogroup I). Hu1A3B-7 is therefore a promising candidate for the future development of a broad-spectrum antiviral therapy to treat VEEV disease in humans.
机译:在委内瑞拉马脑炎病毒(VEEV)的鼠科动物模型中,中和性单克隆抗体1A3B-7已显示在被动保护中有效抵抗血清群I,II和Mucambo病毒(正式为VEE复合体IIIA型)的气溶胶途径攻击。当用于ELISA中时,该抗体能够结合VEEV复合物的所有血清群,因此是蛋白质工程化的极佳候选者,以衍生出适用于人类的治疗用途的人源化分子。使用人类种系IgG框架的互补决定区(CDR)嫁接方法用于生产1A3B-7人源化变体,从中鉴定出具有保留的结合特异性的单个候选分子。在体外研究中对人源化1A3B-7(Hu1A3B-7)的评估表明,Hu1A3B-7保留了广泛的特异性和中和活性。此外,体内实验表明,Hu1A3B-7成功地保护了小鼠免受VEEV株TrD(血清群I)的致死性皮下和气溶胶攻击。因此,Hu1A3B-7是治疗人类VEEV疾病的广谱抗病毒疗法未来发展的有希望的候选者。

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