Repurposed Drugs That Block the Gonococcus-Complement Receptor 3 Interaction Can Prevent and Cure Gonococcal Infection of Primary Human Cervical Epithelial Cells

Jessica Poole; Christopher J. Day; Thomas Haselhorst; Freda E.-C. Jen; Victor J. Torres; Jennifer L. Edwards; Michael P. Jennings

doi:10.1128/mBio.03046-19

mBio (Apr 2020)

Repurposed Drugs That Block the Gonococcus-Complement Receptor 3 Interaction Can Prevent and Cure Gonococcal Infection of Primary Human Cervical Epithelial Cells

Jessica Poole,
Christopher J. Day,
Thomas Haselhorst,
Freda E.-C. Jen,
Victor J. Torres,
Jennifer L. Edwards,
Michael P. Jennings

Affiliations

Jessica Poole: Institute for Glycomics, Griffith University, Southport, Queensland, Australia
Christopher J. Day: Institute for Glycomics, Griffith University, Southport, Queensland, Australia
Thomas Haselhorst: Institute for Glycomics, Griffith University, Southport, Queensland, Australia
Freda E.-C. Jen: Institute for Glycomics, Griffith University, Southport, Queensland, Australia
Victor J. Torres: Department of Microbiology, New York University School of Medicine, New York, New York, USA
Jennifer L. Edwards: The Center for Microbial Pathogenesis, The Abigail Wexner Research Institute at Nationwide Children’s Hospital and The Department of Pediatrics, The Ohio State University, Columbus, Ohio, USA
Michael P. Jennings: Institute for Glycomics, Griffith University, Southport, Queensland, Australia

DOI: https://doi.org/10.1128/mBio.03046-19
Journal volume & issue: Vol. 11, no. 2

Abstract

Read online

ABSTRACT In the absence of a vaccine, multidrug-resistant Neisseria gonorrhoeae has emerged as a major human health threat, and new approaches to treat gonorrhea are urgently needed. N. gonorrhoeae pili are posttranslationally modified by a glycan that terminates in a galactose. The terminal galactose is critical for initial contact with the human cervical mucosa via an interaction with the I-domain of complement receptor 3 (CR3). We have now identified the I-domain galactose-binding epitope and characterized its galactose-specific lectin activity. Using surface plasmon resonance and cellular infection assays, we found that a peptide mimic of this galactose-binding region competitively inhibited the N. gonorrhoeae-CR3 interaction. A compound library was screened for potential drugs that could similarly prohibit the N. gonorrhoeae-CR3 interaction and be repurposed as novel host-targeted therapeutics for multidrug-resistant gonococcal infections in women. Two drugs, methyldopa and carbamazepine, prevented and cured cervical cell infection by multidrug-resistant gonococci by blocking the gonococcal-CR3 I-domain interaction. IMPORTANCE Novel therapies that avert the problem of Neisseria gonorrhoeae with acquired antibiotic resistance are urgently needed. Gonococcal infection of the human cervix is initiated by an interaction between a galactose modification made to its surface appendages, pili, and the I-domain region of (host) complement receptor 3 (CR3). By targeting this crucial gonococcal–I-domain interaction, it may be possible to prevent cervical infection in females. To this end, we identified the I-domain galactose-binding epitope of CR3 and characterized its galactose lectin activity. Moreover, we identified two drugs, carbamazepine and methyldopa, as effective host-targeted therapies for gonorrhea treatment. At doses below those currently used for their respective existing indications, both carbamazepine and methyldopa were more effective than ceftriaxone in curing cervical infection ex vivo. This host-targeted approach would not be subject to N. gonorrhoeae drug resistance mechanisms. Thus, our data suggest a long-term solution to the growing problem of multidrug-resistant N. gonorrhoeae infections.

Published in mBio

ISSN: 2161-2129 (Print); 2150-7511 (Online)
Publisher: American Society for Microbiology
Country of publisher: United States
LCC subjects: Science: Microbiology
Website: https://journals.asm.org/journal/mbio

About the journal

Abstract

Keywords