Structural basis for cooperativity of human monoclonal antibodies to meningococcal factor H-binding protein

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作者
Ilaria Peschiera
Maria Giuliani
Fabiola Giusti
Roberto Melero
Eugenio Paccagnini
Danilo Donnarumma
Werner Pansegrau
José M. Carazo
Carlos O. S. Sorzano
Maria Scarselli
Vega Masignani
Lassi J. Liljeroos
Ilaria Ferlenghi
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[1] Centro National de Biotecnologia,Department of Life Sciences
[2] GSK Vaccines Srl,undefined
[3] University of Siena,undefined
[4] Roche,undefined
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Monoclonal antibody (mAb) cooperativity is a phenomenon triggered when mAbs couples promote increased bactericidal killing compared to individual partners. Cooperativity has been deeply investigated among mAbs elicited by factor H-binding protein (fHbp), a Neisseria meningitidis surface-exposed lipoprotein and one of the key antigens included in both serogroup B meningococcus vaccine Bexsero and Trumenba. Here we report the structural and functional characterization of two cooperative mAbs pairs isolated from Bexsero vaccines. The 3D electron microscopy structures of the human mAb–fHbp–mAb cooperative complexes indicate that the angle formed between the antigen binding fragments (fAbs) assume regular angle and that fHbp is able to bind simultaneously and stably the cooperative mAbs pairs and human factor H (fH) in vitro. These findings shed light on molecular basis of the antibody-based mechanism of protection driven by simultaneous recognition of the different epitopes of the fHbp and underline that cooperativity is crucial in vaccine efficacy.
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