Rapid molecular detection of CMY-2, and CTX-M group 1 and 9 variants via recombinase polymerase amplification

Author:

Ertl Nicole G1,Irwin Adam D12ORCID,Macdonald Joanne3,Bauer Michelle J1,Wang Claire Y T2,Harris Patrick N A14ORCID,Heney Claire4,Zowawi Hosam M156,Whiley David M124

Affiliation:

1. The University of Queensland, UQ Centre for Clinical Research, Faculty of Medicine , Brisbane, QLD , Australia

2. Infection Management and Prevention Service, Children’s Health Queensland , Brisbane, QLD , Australia

3. Centre for Bioinnovation and School of Science, Technology and Engineering, University of the Sunshine Coast , Sippy Downs, QLD , Australia

4. Microbiology Department, Central Laboratory, Pathology Queensland , Brisbane, QLD , Australia

5. College of Medicine, King Saud bin Abdul-Aziz University for Health Science (KSAU-HS) , Riyadh , Saudi Arabia

6. King Abdullah International Medical Research Centre (KAIMRC) , Riyadh , Saudi Arabia

Abstract

AbstractBackgroundDue to their prevalence worldwide, the β-lactamases CTX-M and plasmid-mediated CMY-2 are important antimicrobial resistance enzymes in a clinical setting. While culture- and PCR-based detection methods exist for these targets, they are time consuming and require specialist equipment and trained personnel to carry out.MethodsIn this study, three rapid diagnostic single-plex and a prototype triplex assay were developed, using recombinase polymerase amplification with lateral flow detection (RPA-LF), and tested for their sensitivity and specificity using two isolate DNA panels (n = 90 and n = 120 isolates). In addition, the RPA-LF assays were also tested with a small number of faecal extract samples (n = 18).ResultsThe RPA-LF assays were able to detect blaCXT-M-group-1, blaCTX-M-group-9 and blaCMY-2-type variants with high sensitivity (82.1%–100%) and specificity (100%) within a short turnaround time (15–20 min for amplification and detection).ConclusionsRPA-LF assays developed in this study have the potential to be used at or close to the point of care, as well as in low-resource settings, producing rapid results to support healthcare professionals in their treatment decisions.

Funder

Children’s Hospital Foundation Innovator

Publisher

Oxford University Press (OUP)

Subject

Microbiology (medical),Infectious Diseases,Immunology and Allergy,Microbiology,Immunology

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