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Development of Nanobodies as Theranostic Agents against CMY-2-Like Class C β-Lactamases.

Frédéric CawezPaola Sandra MercuriFrancisco Javier Morales-YãnezRita MaaloufMarylène VandevenneFrederic KerffVirginie GuérinJacques G MainilDamien ThiryMarc SaulmontAlain VanderplasschenPierre LafayeGabriel AyméPierre BogaertsMireille DumoulinMoreno Galleni
Published in: Antimicrobial agents and chemotherapy (2023)
Three soluble single-domain fragments derived from the unique variable region of camelid heavy-chain antibodies (VHHs) against the CMY-2 β-lactamase behaved as inhibitors. The structure of the complex VHH cAb CMY-2 (254)/CMY-2 showed that the epitope is close to the active site and that the CDR3 of the VHH protrudes into the catalytic site. The β-lactamase inhibition pattern followed a mixed profile with a predominant noncompetitive component. The three isolated VHHs recognized overlapping epitopes since they behaved as competitive binders. Our study identified a binding site that can be targeted by a new class of β-lactamase inhibitors designed on the sequence of the paratope. Furthermore, the use of mono- or bivalent VHH and rabbit polyclonal anti-CMY-2 antibodies enables the development of the first generation of enzyme-linked immunosorbent assay (ELISA) for the detection of CMY-2 produced by CMY-2-expressing bacteria, irrespective of resistotype.
Keyphrases
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