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与H蛋白的胱氨酸环结构域结合的单克隆抗体对麻疹病毒脑炎具有保护作用,该结构域由母体抗体无法识别的肽模拟。

Protection against measles virus encephalitis by monoclonal antibodies binding to a cystine loop domain of the H protein mimicked by peptides which are not recognized by maternal antibodies.

作者信息

Ziegler D, Fournier P, Berbers G A, Steuer H, Wiesmüller K H, Fleckenstein B, Schneider F, Jung G, King C C, Muller C P

机构信息

Laboratoire National de Santé, Luxembourg.

出版信息

J Gen Virol. 1996 Oct;77 ( Pt 10):2479-89. doi: 10.1099/0022-1317-77-10-2479.

DOI:10.1099/0022-1317-77-10-2479
PMID:8887481
Abstract

After immunization with measles virus (MV) several monoclonal antibodies (MAbs) were obtained, which reacted with peptides corresponding to the amino acids 361-410 of the haemagglutinin protein (MV-H). Three of these MAbs (BH6, BH21 and BH216) inhibited haemagglutination, neutralized MV in vitro and protected animals from a lethal challenge of rodent-adapted neurotropic MV. These MAbs reacted with the 15-mer peptides H381 and H386 defining their overlapping region 386-395 as a sequential neutralizing and protective epitope, which can be imitated by a short peptide. H381 and H386 share two Cys residues (C(386)KGKIQALC(394)ENPEWA) and for optimal MAb binding of peptide (or MV) disulphide bonds were required in addition to a linear C-terminal extension. Other MAbs bound to peptides C- (BH147, BH195) and N-terminally (BH 168, BH 171) adjacent to the loop but did not neutralize or protect. When sera from measles patients or from women of child-bearing age were tested with the peptides corresponding to this haemagglutinating and neutralizing epitope (HNE), none of the sera recognized the 15-mer peptides of this region, while some reactivity was found to 30-mers homologous to different wild-type mutants. Its lack of recognition by maternal antibodies and its high degree of conservation would make the HNE loop an attractive candidate to include into a subunit vaccine, which could be administered during early childhood, independent of immune status.

摘要

用麻疹病毒(MV)免疫后,获得了几种单克隆抗体(MAb),它们与血凝素蛋白(MV-H)氨基酸361-410对应的肽段发生反应。其中三种单克隆抗体(BH6、BH21和BH216)抑制血凝,在体外中和MV,并保护动物免受啮齿动物适应的嗜神经MV的致死性攻击。这些单克隆抗体与15肽H381和H386发生反应,将其重叠区域386-395定义为连续的中和及保护性表位,该表位可被短肽模拟。H381和H386共有两个半胱氨酸残基(C(386)KGKIQALC(394)ENPEWA),除线性C末端延伸外,肽段(或MV)的最佳单克隆抗体结合还需要二硫键。其他单克隆抗体与环相邻的C末端(BH147、BH195)和N末端(BH168、BH171)肽段结合,但不具有中和或保护作用。当用与该血凝和中和表位(HNE)对应的肽段检测麻疹患者或育龄妇女的血清时,没有一种血清能识别该区域的15肽,而对与不同野生型突变体同源的30肽有一些反应性。母体抗体对其缺乏识别以及其高度保守性,将使HNE环成为纳入亚单位疫苗的有吸引力的候选者,该疫苗可在幼儿期接种,与免疫状态无关。

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