P-1553. Exploring the Role of Capsule in Innate Immune Interactions of Multidrug-Resistant Klebsiella pneumoniae
Nathalie Chen, Margaret Cassady, Emma Mills, Shekina Gonzalez-Ferrer, Marrisa P Griffifth, Lora Pless, Lee Harrison, William Bain, Daria Van Tyne

TL;DR
This study compares two clades of multidrug-resistant Klebsiella pneumoniae and finds that Clade 2 is more pathogenic, possibly due to differences in their capsule composition.
Contribution
The study identifies capsule composition and immune interaction differences as potential drivers of pathogenicity in KP ST258 clades.
Findings
Clade 2 isolates are more frequently associated with severe infections and show higher pathogenicity in mice.
Clade 2 isolates have a capsule rich in rhamnose and are more resistant to human serum killing.
Clade 2 isolates produce more C5a upon exposure to human serum compared to Clade 1.
Abstract
Klebsiella pneumoniae (KP) belonging to multi-locus sequence type 258 (ST258) is a frequent cause of hospital-associated outbreaks. KP ST258 isolates display extensive multidrug-resistance; however, this feature alone does not explain the global dissemination and pathogenic success of this lineage. KP ST258 consists of two genetically distinct clades, Clade 1 and Clade 2. While bacteria belonging to both clades are isolated from clinical infections, Clade 2 is isolated more frequently compared to Clade 1. To investigate drivers of this difference in distribution, we leveraged a collection of 50 sequenced clinical KP ST258 isolates (N=13 Clade 1, N=37 Clade 2) to genotypically and phenotypically assess the two clades. A primary difference between the two clades is the polysaccharide capsule, which is a critical virulence factor for KP. Analysis of the Clade 1 capsule showed that it…
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Taxonomy
TopicsAntibiotic Resistance in Bacteria · Escherichia coli research studies · Bacterial biofilms and quorum sensing
