Abstract

With dire predictions of antibiotic resistance reaching a tipping point, it is imperative that novel, antibiotic-sparing medicines are developed to avoid facing increasing deaths due to previously treatable common infections. This project is focused on this mission by elucidating potential therapeutic targets critical in host-pathogen interactions for urinary tract infections (UTI), one of the most common infections leading to significant antibiotic use and economic burden. Over 11 million women suffer from UTIs in the U.S. per year. Further, 20-30% of women diagnosed with a UTI will experience a recurrent UTI (rUTI) in the following months, resulting in a serious deterioration in the quality of life through pain, discomfort, disruption of daily activities, and increased healthcare cost. This problem is exacerbated by rising antimicrobial resistance among uropathogenic Escherichia coli (UPEC), the cause of over 80% of uncomplicated UTIs. Rates of antibiotic resistance are confounding UTI treatment for millions of women annually. One critical aspect of uropathogenesis is the ability of bacteria to bind to host tissues to establish an infection or colonization. Gram-negative bacteria typically utilize adhesive chaperone usher pathway (CUP) pili, tipped with adhesins that bind to receptors with stereochemical specificity, mediating host and tissue tropisms. Pilus adhesins are two-domain molecules consisting of a C-terminal pilin domain that links the adhesin to the pilus tip and an N-terminal receptor-binding domain. The pangenome of E. coli alone encodes thirty-eight distinct CUP pilus types and single E. coli genomes encode as many as 16, each likely mediating colonization of a particular habitat. However, only a handful of UPEC adhesins have been investigated to date. Each of them play critical roles in particular niches. FimH mediates critical binding to mannose residues on bladder tissue to promote invasion into superficial facet cells during acute cystitis; FmlH mediates binding to galactose moieties on inflamed bladder epithelial tissue during chronic cystitis; PapG mediates binding to human kidney during pyelonephritis; and UclD mediates colonization of the gut where UPEC forms a reservoir. Catheterization increases the susceptibility of the urinary tract to infection with a wider variety of strains, including Acinetobacter baumanii resulting in increasingly common multidrug resistant catheter- associated UTIs (CAUTI). Acinetobacter baumanii are known to encode at least two CUP pili known to be important in CAUTI. This proposal seeks to elucidate: i) the molecular dynamics of adhesin conformational equilibriums that govern host-pathogen interactions; ii) structure-function correlates of UPEC CUP adhesins with unknown functions; and iii) structure-function correlates of Acinetobacter baumanii CUP adhesins critical in CAUTIs. This proposal will enhance the understanding of the mechanism of action of host-pathogen interactions and elucidate opportunities to develop much needed antibiotic-sparing therapeutics that block the ability of these uropathogens to colonize/infect host tissues such as mannosides for which a candidate has been chosen for clinical trials.

Public Health Relevance

Urinary tract infections (UTIs) and catheter associated UTIs are common and increasingly antibiotic resistant. Thus, a high resolution understanding of the mechanisms of host-pathogen interactions is needed to spawn the development of new antibiotic-sparing therapeutics that interrupt interactions necessary for virulence. Thus, we will elucidate structure-function correlates of a repertoire of chaperone usher pathway (CUP) pilus adhesins encoded by the most common uropathogen, uropathogenic E. coli, and CUP adhesins encoded by Acinetobacter baumanii, a frequently multidrug pathogen that causes increasing numbers of opportunistic infections. The receptor specificity, structures and dynamics of CUP adhesins will transform the field by providing a new conceptual framework in microbial pathogenesis focused on events critical to host colonization and uncovering new therapeutic strategies to treat or prevent disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
2R01AI048689-21
Application #
10121286
Study Section
Bacterial Pathogenesis Study Section (BACP)
Program Officer
Ernst, Nancy L
Project Start
2001-02-01
Project End
2026-01-31
Budget Start
2021-02-01
Budget End
2022-01-31
Support Year
21
Fiscal Year
2021
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Spaulding, Caitlin N; Schreiber 4th, Henry Louis; Zheng, Weili et al. (2018) Functional role of the type 1 pilus rod structure in mediating host-pathogen interactions. Elife 7:
Omattage, Natalie S; Deng, Zengqin; Pinkner, Jerome S et al. (2018) Structural basis for usher activation and intramolecular subunit transfer in P pilus biogenesis in Escherichia coli. Nat Microbiol 3:1362-1368
Schwan, William R; Beck, Michael T; Hung, Chia S et al. (2018) Differential Regulation of Escherichia coli fim Genes following Binding to Mannose Receptors. J Pathog 2018:2897581
Paharik, Alexandra E; Schreiber 4th, Henry L; Spaulding, Caitlin N et al. (2017) Narrowing the spectrum: the new frontier of precision antimicrobials. Genome Med 9:110
Sheikh, Alaullah; Rashu, Rasheduzzaman; Begum, Yasmin Ara et al. (2017) Highly conserved type 1 pili promote enterotoxigenic E. coli pathogen-host interactions. PLoS Negl Trop Dis 11:e0005586
Kalas, Vasilios; Pinkner, Jerome S; Hannan, Thomas J et al. (2017) Evolutionary fine-tuning of conformational ensembles in FimH during host-pathogen interactions. Sci Adv 3:e1601944
Spaulding, Caitlin N; Klein, Roger D; Ruer, Ségolène et al. (2017) Selective depletion of uropathogenic E. coli from the gut by a FimH antagonist. Nature 546:528-532
Hospenthal, Manuela K; Redzej, Adam; Dodson, Karen et al. (2016) Structure of a Chaperone-Usher Pilus Reveals the Molecular Basis of Rod Uncoiling. Cell 164:269-278
Conover, Matt S; Ruer, Ségolène; Taganna, Joemar et al. (2016) Inflammation-Induced Adhesin-Receptor Interaction Provides a Fitness Advantage to Uropathogenic E. coli during Chronic Infection. Cell Host Microbe 20:482-492
O'Brien, Valerie P; Hannan, Thomas J; Nielsen, Hailyn V et al. (2016) Drug and Vaccine Development for the Treatment and Prevention of Urinary Tract Infections. Microbiol Spectr 4:

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