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Junctional and allele-specific residues are critical for MERS-CoV neutralization by an exceptionally potent germline-like antibody.

Nat Commun. 2015; 
YingTianlei,PrabakaranPonraj,DuLanying,ShiWei,FengYang,WangYanping,WangLingshu,LiWei,JiangShibo,DimitrovDimiter S,ZhouTong
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Gene Synthesis The light chains of m336-gL-FR and m336-gL were synthesized by GenScript (Piscataway, NJ) and inserted into the m336 IgG1-expressing plasmid, respectively, to replace the original light chain of m336. Get A Quote

摘要

The MERS-CoV is an emerging virus, which already infected more than 1,300 humans with high (∼36%) mortality. Here, we show that m336, an exceptionally potent human anti-MERS-CoV antibody, is almost germline with only one somatic mutation in the heavy chain. The structure of Fab m336 in complex with the MERS-CoV receptor-binding domain reveals that its IGHV1-69-derived heavy chain provides more than 85% binding surface and that its epitope almost completely overlaps with the receptor-binding site. Analysis of antibodies from 69 healthy humans suggests an important role of the V(D)J recombination-generated junctional and allele-specific residues for achieving high affinity of binding at such low level... More

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