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一种源自人非免疫噬菌体文库的单克隆Fab片段揭示了gp41上的一个新表位,并能中和多种1型人类免疫缺陷病毒毒株。

A monoclonal Fab derived from a human nonimmune phage library reveals a new epitope on gp41 and neutralizes diverse human immunodeficiency virus type 1 strains.

作者信息

Gustchina Elena, Louis John M, Lam Son N, Bewley Carole A, Clore G Marius

机构信息

Laboratory of Chemical Physics, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892-0820, USA.

出版信息

J Virol. 2007 Dec;81(23):12946-53. doi: 10.1128/JVI.01260-07. Epub 2007 Sep 26.

Abstract

A monoclonal Fab (Fab 3674) selected from a human nonimmune phage library by panning against the chimeric construct N(CCG)-gp41 (which comprises an exposed coiled-coil trimer of gp41 N helices fused in the helical phase onto the minimal thermostable ectodomain of gp41) is described. Fab 3674 is shown to neutralize diverse laboratory-adapted B strains of human immunodeficiency virus type 1 (HIV-1) and primary isolates of subtypes A, B, and C in an Env-pseudotyped-virus neutralization assay, albeit with reduced potency (approximately 25-fold) compared to that of 2F5 and 4E10. Alanine scanning mutagenesis maps a novel epitope to a shallow groove on the N helices of gp41 that is exposed between two C helices in the fusogenic six-helix bundle conformation of gp41. Bivalent Fab 3674 and the C34 peptide (a potent fusion inhibitor derived from the C helix of gp41) are shown to act at similar stages of the fusion reaction and to neutralize HIV-1 synergistically, providing additional evidence that the epitope of Fab 3674 is new and distinct from the binding site of C34.

摘要

描述了一种通过针对嵌合构建体N(CCG)-gp41(其包含在螺旋相中融合到gp41最小热稳定胞外域上的gp41 N螺旋的暴露卷曲螺旋三聚体)从人非免疫噬菌体文库中筛选出的单克隆Fab(Fab 3674)。在Env假型病毒中和试验中,Fab 3674显示出能中和多种实验室适应的1型人类免疫缺陷病毒(HIV-1)B株以及A、B和C亚型的原代分离株,尽管与2F5和4E10相比效力有所降低(约25倍)。丙氨酸扫描诱变将一个新表位定位到gp41 N螺旋上的一个浅沟中,该浅沟在gp41融合性六螺旋束构象的两个C螺旋之间暴露。二价Fab 3674和C34肽(一种源自gp41 C螺旋的有效融合抑制剂)显示在融合反应的相似阶段起作用并协同中和HIV-1,这提供了额外证据表明Fab 3674的表位是新的且与C34的结合位点不同。

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