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Chimpanzee/human mAbs to vaccinia virus B5 protein neutralize vaccinia and smallpox viruses and protect mice against vaccinia virus

机译:黑猩猩/人单克隆抗体对牛痘病毒B5蛋白的作用可中和牛痘和天花病毒,并保护小鼠免受牛痘病毒

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摘要

Chimpanzee Fabs against the B5 envelope glycoprotein of vaccinia virus were isolated and converted into complete mAbs with human γ1 heavy chain constant regions. The two mAbs (8AH8AL and 8AH7AL) displayed high binding affinities to B5 (Kd of 0.2 and 0.7 nM). The mAb 8AH8AL inhibited the spread of vaccinia virus as well as variola virus (the causative agent of smallpox) in vitro, protected mice from subsequent intranasal challenge with virulent vaccinia virus, protected mice when administered 2 days after challenge, and provided significantly greater protection than that afforded by a previously isolated rat anti-B5 mAb (19C2) or by vaccinia immune globulin. The mAb bound to a conformational epitope between amino acids 20 and 130 of B5. These chimpanzee/human anti-B5 mAbs may be useful in the prevention and treatment of vaccinia virus-induced complications of vaccination against smallpox and may also be effective in the immunoprophylaxis and immunotherapy of smallpox.
机译:分离出针对痘苗病毒B5包膜糖蛋白的黑猩猩Fab,并将其转化为具有人γ1重链恒定区的完整mAb。这两个mAb(8AH8AL和8AH7AL)显示出与B5的高结合亲和力(Kd为0.2和0.7 nM)。 mAb 8AH8AL在体外抑制牛痘病毒和天花病毒(天花的病原体)的传播,用强力牛痘病毒保护小鼠免于随后的鼻内攻击,在攻击后2天给药时保护小鼠,并且提供的保护作用远大于由先前分离出的大鼠抗B5 mAb(19C2)或牛痘免疫球蛋白提供的抗体。该mAb结合至B5的氨基酸20和130之间的构象表位。这些黑猩猩/人抗B5单抗可用于预防和治疗牛痘病毒诱导的针对天花的疫苗接种并发症,也可有效预防和预防天花。

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