Drug susceptibility testing of Mycobacterium tuberculosis using next generation sequencing and Mykrobe software

V Tolchkov,Yu Atanasova,D Cirillo,Y Hodzhev,B Tsafarova,E Bachiyska,S Panaiotov,A Trovato,A Baykova,S Yordanova

doi:10.36233/0372-9311-191

Abstract

Introduction. Mycobacterium tuberculosis is the causative agent of tuberculosis. Drug susceptibility testing is performed by phenotypic and molecular tests. Commonly used for phenotypic drug susceptibility testing is the automated BACTEC system in a liquid culture medium. Drug susceptibility by line probe molecular tests was introduced almost 15 years ago. Recently whole genome sequencing (WGS) analysis of M. tuberculosis strains demonstrated that genotyping of drug-resistance could be accurately performed. Several software tools were developed.Our study aimed to perform whole-genome sequencing on phenotypically confirmed multi-drug resistant (MDR) M. tuberculosis strains, to identify drug-resistant mutations and to compare whole-genome sequencing profiles with line probe assay and phenotypic results.Materials and methods. We performed analysis on 34 MDR M. tuberculosis Bulgarian strains. Phenotypic drug susceptibility testing was performed on the BACTEC system. For molecular testing of drug susceptibility to first- and second-line tuberculostatics, we applied line probe assay Geno Type MTBDR plus v.1.0 и Geno Type MTBDR sl v.1.0. Sequencing was performed on MiSeq. Generated FASTQ files were analyzed for known drugresistant mutations with the software platform Mykrobe v.0.8.1.Results. All three methods — phenotypic analysis using the BACTEC system, genetic analysis of strains applying the Geno Type test and Mykrobe software gave comparable sensitivity/resistance results for the studied strains. All phenotypically proven rifampicin and isoniazid-resistant strains were 100% confirmed using Mykrobe software. The C-15T mutation is a marker for isoniazid resistance in strains of the SIT41 spoligotype. We observed a 75% (21/28) agreement between BACTEC and Mykrobe for ethambutol resistance. Phenotypically, 87% (n = 27) of the strains are resistant to streptomycin, but only 59% (n = 19) are proven by Mykrobe software. Comparing phenotypic and genotypic resistance to ofloxacin, amikacin and kanamycin, we observed 100% coincidence of results.Conclusions. Whole-genome sequencing approach is relatively expensive and laborious but useful for detailed analysis such as epidemiological genotyping and molecular drug susceptibility testing.

Highlights

Mycobacterium tuberculosis is the causative agent of tuberculosis
The genotypic resistance for most of them was determined by the line probe assay (LPA) (71% of them were tested for first-line drugs and 21% were tested for second-line drugs) at the National Reference Laboratory of tuberculosis, NCIPD
We determined the drug-susceptibility of 34 strains of M. tuberculosis collected at the National Reference Laboratory of Tuberculosis, NCIPD, Sofia, Bulgaria

Summary

Introduction

Mycobacterium tuberculosis is the causative agent of tuberculosis. Drug susceptibility testing is performed by phenotypic and molecular tests. All three methods — phenotypic analysis using the BACTEC system, genetic analysis of strains applying the Geno Type test and Mykrobe software gave comparable sensitivity/resistance results for the studied strains. The introduction of next-generation sequencing technologies gave to researchers new opportunities for more powerful and detailed analysis [8,9,10,11] Another advantage of NGS analysis is that when a strain once being sequenced, the information could be stored in formats such as FASTQ, FAST5 or others, depending on the technology, this strain can be analyzed in further studies with different software tools for different genetic, phylogenetic and epidemiological investigations. Soon application of next-generation sequencing technology will be mandatory in the description of bacterial or viral strains and will be widely used in other fields of medicine and will displace many phenotypic and current molecular genetic methods. Software tools were developed for drug resistance determination using data of whole-genome sequenced micro-

Methods

Results

Conclusion