# Preclinical validation of an Escherichia coli O-antigen glycoconjugate for the prevention of serotype O1 invasive disease

**Authors:** Laurent Chorro, Duston Ndreu, Axay Patel, Srinivas Kodali, Zhenghui Li, David Keeney, Kaushik Dutta, Aniruddha Sasmal, Arthur Illenberger, C. Lynn Torres, Rosalind Pan, Natalie C. Silmon de Monerri, Ling Chu, Raphael Simon, Annaliesa S. Anderson, Robert G. K. Donald

PMC · DOI: 10.1128/spectrum.04213-23 · 2024-05-03

## TL;DR

Researchers developed a promising vaccine candidate against Escherichia coli O1 bloodstream infections by creating a glycoconjugate antigen that protects mice from lethal challenges.

## Contribution

The study introduces a novel glycoconjugate vaccine candidate for preventing invasive E. coli O1 infections using a conserved O1a antigen.

## Key findings

- The O1a glycoconjugate elicited functional antibodies and protected mice from lethal K1-encapsulated O1a isolates.
- Two ST95 strains were susceptible to OPA killing with O1a glycoconjugate post-immune sera.
- Mice immunized with the glycoconjugate were protected against neonatal sepsis strains.

## Abstract

A US collection of invasive Escherichia coli serotype O1 bloodstream infection (BSI) isolates were assessed for genotypic and phenotypic diversity as the basis for designing a broadly protective O-antigen vaccine. Eighty percent of the BSI isolate serotype O1 strains were genotypically ST95 O1:K1:H7. The carbohydrate repeat unit structure of the O1a subtype was conserved in the three strains tested representing core genome multi-locus sequence types (MLST) sequence types ST95, ST38, and ST59. A long-chain O1a CRM197 lattice glycoconjugate antigen was generated using oxidized polysaccharide and reductive amination chemistry. Two ST95 strains were investigated for use in opsonophagocytic assays (OPA) with immune sera from vaccinated animals and in murine lethal challenge models. Both strains were susceptible to OPA killing with O1a glycoconjugate post-immune sera. One of these, a neonatal sepsis strain, was found to be highly lethal in the murine challenge model for which virulence was shown to be dependent on the presence of the K1 capsule. Mice immunized with the O1a glycoconjugate were protected from challenges with this strain or a second, genotypically related, and similarly virulent neonatal isolate. This long-chain O1a CRM197 lattice glycoconjugate shows promise as a component of a multi-valent vaccine to prevent invasive E. coli infections.

The Escherichia coli serotype O1 O-antigen serogroup is a common cause of invasive bloodstream infections (BSI) in populations at risk such as newborns and the elderly. Sequencing of US BSI isolates and structural analysis of O polysaccharide antigens purified from strains that are representative of genotypic sub-groups confirmed the relevance of the O1a subtype as a vaccine antigen. O polysaccharide was purified from a strain engineered to produce long-chain O1a O-antigen and was chemically conjugated to CRM197 carrier protein. The resulting glycoconjugate elicited functional antibodies and was protective in mice against lethal challenges with virulent K1-encapsulated O1a isolates.

## Linked entities

- **Diseases:** neonatal sepsis (MONDO:0700217)
- **Species:** Escherichia coli (taxon 562), Mus musculus (taxon 10090)

## Full-text entities

- **Diseases:** invasive disease (MESH:D009361), neonatal sepsis (MESH:D000071074), BSI (MESH:D018805)
- **Chemicals:** polysaccharide (MESH:D011134), O (MESH:D010100), carbohydrate (MESH:D002241)
- **Species:** Escherichia coli (E. coli, species) [taxon 562], Mus musculus (house mouse, species) [taxon 10090]

## Figures

6 figures with captions in the complete paper: https://tomesphere.com/paper/PMC11237799/full.md

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Source: https://tomesphere.com/paper/PMC11237799