A multi-enzyme machine polymerizes the Haemophilus influenzae type b capsule

Author:

Cifuente Javier O.ORCID,Schulze JuliaORCID,Bethe Andrea,Di Domenico ValerioORCID,Litschko ChristaORCID,Budde Insa,Eidenberger LukasORCID,Thiesler HaukeORCID,Ramón Roth Isabel,Berger Monika,Claus HeikeORCID,D’Angelo CeciliaORCID,Marina AlbertoORCID,Gerardy-Schahn RitaORCID,Schubert MarioORCID,Guerin Marcelo E.ORCID,Fiebig TimmORCID

Abstract

AbstractBacterial capsules have critical roles in host-pathogen interactions. They provide a protective envelope against host recognition, leading to immune evasion and bacterial survival. Here we define the capsule biosynthesis pathway of Haemophilus influenzae serotype b (Hib), a Gram-negative bacterium that causes severe infections in infants and children. Reconstitution of this pathway enabled the fermentation-free production of Hib vaccine antigens starting from widely available precursors and detailed characterization of the enzymatic machinery. The X-ray crystal structure of the capsule polymerase Bcs3 reveals a multi-enzyme machine adopting a basket-like shape that creates a protected environment for the synthesis of the complex Hib polymer. This architecture is commonly exploited for surface glycan synthesis by both Gram-negative and Gram-positive pathogens. Supported by biochemical studies and comprehensive 2D nuclear magnetic resonance, our data explain how the ribofuranosyltransferase CriT, the phosphatase CrpP, the ribitol-phosphate transferase CroT and a polymer-binding domain function as a unique multi-enzyme assembly.

Publisher

Springer Science and Business Media LLC

Subject

Cell Biology,Molecular Biology

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