A Multidisciplinary Structural Approach to the Identification of the Type B Capsular Polysaccharide Protective Epitope

Overview

Journal ACS Cent Sci

Specialty Chemistry

Date 2024 May 27

PMID 38799664

Authors

Francesca Nonne

Lucia Dello Iacono

Sara Bertuzzi

Luca Unione

Daniela Proietti

Nathalie Norais

Immaculada Margarit

Roberto Adamo

Jesus Jimenez-Barbero

Filippo Carboni

Maria Rosaria Romano

Affiliations

Soon will be listed here.

Abstract

Glycoconjugate vaccines so far licensed are generally composed of a native or size-reduced capsular polysaccharide conjugated to carrier proteins. Detailed information on the structural requirements necessary for CPS recognition is becoming the key to accelerating the development of next-generation improved glycoconjugate vaccines. Structural glycobiology studies using oligosaccharides (OS) complexed with functional monoclonal antibodies represent a powerful tool for gaining information on CPS immunological determinants at the atomic level. Herein, the minimal structural epitope of type b (Hib) CPS recognized by a functional human monoclonal antibody (hmAb) is reported. Short and well-defined Hib oligosaccharides originating from the depolymerization of the native CPS have been used to elucidate saccharide-mAb interactions by using a multidisciplinary approach combining surface plasmon resonance (SPR), saturation transfer difference-nanomagnetic resonance (STD-NMR), and X-ray crystallography. Our study demonstrates that the minimal structural epitope of Hib is comprised within two repeating units (RUs) where ribose and ribitol are directly engaged in the hmAb interaction, and the binding pocket fully accommodates two RUs without any additional involvement of a third one. Understanding saccharide antigen structural characteristics can provide the basis for the design of innovative glycoconjugate vaccines based on alternative technologies, such as synthetic or enzymatic approaches.

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