Resistance patterns and transmission of mono- and polyresistant TB: clinical impact of WGS

Author:

Dohál Matúš1,Dvořáková Věra2,Šperková Miluše2,Pinková Martina2,Spitaleri Andrea34,Rasmussen Erik Michael5,Škereňová Mária16,Krivošová Michaela1,Gondáš Eduard1,Porvazník Igor78,Solovič Ivan7,Cirillo Daniela Maria3,Mokrý Juraj9

Affiliation:

1. Biomedical Centre Martin, Jessenius Faculty of Medicine in Martin, Comenius University , Bratislava , Slovakia

2. National Reference Laboratory for Mycobacteria, National Institute of Public Health , Prague , Czech Republic

3. Emerging Bacterial Pathogens Unit, Division of Immunology, Transplantation and Infectious Diseases, IRCCS San Raffaele Scientific Institute , Milan , Italy

4. Vita-Salute San Raffaele University , Milan , Italy

5. International Reference Laboratory of Mycobacteriology, Statens Serum Institut , Copenhagen , Denmark

6. Department of Molecular Medicine, Jessenius Faculty of Medicine in Martin, Comenius University , Bratislava , Slovakia

7. Department of Clinical Microbiology and Department of Pneumophthiology, National Institute of Tuberculosis, Lung Diseases and Thoracic Surgery , Vyšné Hágy , Slovakia

8. Faculty of Health, Catholic University , Ružomberok , Slovakia

9. Department of Pharmacology, Jessenius Faculty of Medicine in Martin, Comenius University , Bratislava , Slovakia

Abstract

Abstract Objectives Rapidly diagnosing drug-resistant TB is crucial for improving treatment and transmission control. WGS is becoming increasingly accessible and has added value to the diagnosis and treatment of TB. The aim of the study was to perform WGS to determine the rate of false-positive results of phenotypic drug susceptibility testing (pDST) and characterize the molecular mechanisms of resistance and transmission of mono- and polyresistant Mycobacterium (M.) tuberculosis. Methods WGS was performed on 53 monoresistant and 25 polyresistant M. tuberculosis isolates characterized by pDST. Sequencing data were bioinformatically processed to infer mutations encoding resistance and determine the origin of resistance and phylogenetic relationship between isolates studied. Results The data showed the variable sensitivity and specificity of WGS in comparison with pDST as the gold standard: isoniazid 92.7% and 92.3%; streptomycin 41.9% and 100.0%; pyrazinamide 15% and 94.8%; and ethambutol 75.0% and 98.6%, respectively. We found novel mutations encoding resistance to streptomycin (in gidB) and pyrazinamide (in kefB). Most isolates belonged to lineage 4 (80.1%) and the overall clustering rate was 11.5%. We observed lineage-specific gene variations encoding resistance to streptomycin and pyrazinamide. Conclusions This study highlights the clinical potential of WGS in ruling out false-positive drug resistance following phenotypic or genetic drug testing, and recommend this technology together with the WHO catalogue in designing an optimal individualized treatment regimen and preventing the development of MDR TB. Our results suggest that resistance is primarily developed through spontaneous mutations or selective pressure.

Funder

The National Institute of Public Health—NIPH

Publisher

Oxford University Press (OUP)

Subject

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

Reference42 articles.

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