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Intra-spike crosslinking overcomes antibody evasion by HIV-1.

Cell. 2015-01; 
GalimidiRachel P,KleinJoshua S,PolitzerMaria S,BaiShiyu,SeamanMichael S,NussenzweigMichel C,WestAnthony P,BjorkmanPame
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Peptide Synthesis Peptides (GGGK with C-terminal azide and cyclooctyne click handles) were synthesized by GenScript, and sortase-catalyzed peptide ligation was used to attach the azide-containing peptide to PG16 Fab and the cyclooctyne-containing peptide to the 3BNC60-TPR12 fusion protein as described. Get A Quote

摘要

Antibodies developed during HIV-1 infection lose efficacy as the viral spike mutates. We postulated that anti-HIV-1 antibodies primarily bind monovalently because HIV's low spike density impedes bivalent binding through inter-spike crosslinking, and the spike structure prohibits bivalent binding through intra-spike crosslinking. Monovalent binding reduces avidity and potency, thus expanding the range of mutations permitting antibody evasion. To test this idea, we engineered antibody-based molecules capable of bivalent binding through intra-spike crosslinking. We used DNA as a "molecular ruler" to measure intra-epitope distances on virion-bound spikes and construct intra-spike crosslinking molecules. Optim... More

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