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具有不同种系起源的病毒受体结合位点抗体。

Viral receptor-binding site antibodies with diverse germline origins.

作者信息

Schmidt Aaron G, Therkelsen Matthew D, Stewart Shaun, Kepler Thomas B, Liao Hua-Xin, Moody M Anthony, Haynes Barton F, Harrison Stephen C

机构信息

Laboratory of Molecular Medicine, Children's Hospital, Harvard Medical School, Boston, MA 02115, USA.

Novartis Vaccines and Diagnostics, Cambridge MA, USA.

出版信息

Cell. 2015 May 21;161(5):1026-1034. doi: 10.1016/j.cell.2015.04.028. Epub 2015 May 7.

Abstract

Vaccines for rapidly evolving pathogens will confer lasting immunity if they elicit antibodies recognizing conserved epitopes, such as a receptor-binding site (RBS). From characteristics of an influenza-virus RBS-directed antibody, we devised a signature motif to search for similar antibodies. We identified, from three vaccinees, over 100 candidates encoded by 11 different VH genes. Crystal structures show that antibodies in this class engage the hemagglutinin RBS and mimic binding of the receptor, sialic acid, by supplying a critical dipeptide on their projecting, heavy-chain third complementarity determining region. They share contacts with conserved, receptor-binding residues but contact different residues on the RBS periphery, limiting the likelihood of viral escape when several such antibodies are present. These data show that related modes of RBS recognition can arise from different germline origins and mature through diverse affinity maturation pathways. Immunogens focused on an RBS-directed response will thus have a broad range of B cell targets.

摘要

对于快速进化的病原体,如果疫苗能引发识别保守表位(如受体结合位点,RBS)的抗体,就能赋予持久免疫力。根据流感病毒RBS导向抗体的特性,我们设计了一个特征基序来搜索相似抗体。我们从三名疫苗接种者中鉴定出100多个由11个不同VH基因编码的候选抗体。晶体结构表明,这类抗体与血凝素RBS结合,并通过在其伸出的重链第三互补决定区提供一个关键二肽来模拟受体唾液酸的结合。它们与保守的受体结合残基有共同接触,但在RBS周边接触不同残基,当存在几种这样的抗体时,限制了病毒逃逸的可能性。这些数据表明,RBS识别的相关模式可源自不同的种系起源,并通过多样的亲和力成熟途径成熟。因此,专注于RBS导向反应的免疫原将有广泛的B细胞靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c71/4441819/77f6b52aec78/nihms689029f1.jpg

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