Whole-genome sequencing of Mycobacterium tuberculosis directly from clinical samples for high-resolution genomic epidemiology and drug resistance surveillance: an observational study

Galo A Goig; Irving Cancino-Muñoz; Manuela Torres-Puente; Luis M Villamayor; David Navarro; Rafael Borrás; Iñaki Comas

doi:10.1016/S2666-5247(20)30060-4

Whole-genome sequencing of Mycobacterium tuberculosis directly from clinical samples for high-resolution genomic epidemiology and drug resistance surveillance: an observational study

Lancet Microbe. 2020 Aug;1(4):e175-e183. doi: 10.1016/S2666-5247(20)30060-4. Epub 2020 Aug 6.

Authors

Galo A Goig¹, Irving Cancino-Muñoz¹, Manuela Torres-Puente¹, Luis M Villamayor², David Navarro³, Rafael Borrás³, Iñaki Comas⁴

Affiliations

¹ Institute of Biomedicine of Valencia (CSIC), Valencia, Spain.
² Foundation for the Promotion of Health and Biomedical Research of Valencia Region (FISABIO) Public Health (CSISP), Valencia, Spain.
³ Microbiology Service, University Clinic Hospital, Valencia, Spain; School of Medicine, University of Valencia, Valencia, Spain.
⁴ Institute of Biomedicine of Valencia (CSIC), Valencia, Spain; Biomedical Research Networking Centre (CIBER) in Epidemiology and Public Health, Madrid, Spain. Electronic address: icomas@ibv.csic.es.

PMID: 35544271
DOI: 10.1016/S2666-5247(20)30060-4

Abstract

Background: Direct whole-genome sequencing of Mycobacterium tuberculosis from clinical specimens will be a major breakthrough in tuberculosis diagnosis and control. To date, direct whole-genome sequencing has never been used in genomic epidemiology, and its accuracy in transmission inference remains unknown. We investigated the technical challenges imposed by direct whole-genome sequencing, and used it to infer transmission clusters and predict drug resistance.

Methods: Using an optimised workflow, we did direct whole-genome sequencing for 37 clinical specimens from 23 tuberculosis patients. Nine sputum samples from nine patients who were infected with different non-tuberculous mycobacteria and culture-negative for tuberculosis were used as controls in the qPCR assays and pre-sequencing runs. Additionally, 780 clinical isolates in the region of Comunidad Valenciana (Spain) were whole-genome sequenced between Jan 1, 2014, and Dec 31, 2016. We analysed the genomic variants to build a tuberculosis transmission network for the region, including the clinical specimens, and to predict drug susceptibility profiles.

Findings: After sequencing 37 clinical specimens, 28 specimens (22 [85%] of 26 smear-positive and six [55%] of 11 smear-negative) met the quality criteria for downstream analysis. All 28 clinical specimens clustered with their matching culture isolates, with a median distance of 0 single nucleotide polymorphisms. Of the 28 clinical specimens, 16 (57%) were accurately assigned to ten transmission clusters in the region, and 12 (43%) were unique cases. Transmission inferences and drug-susceptibility predictions from direct whole-genome sequencing data were concordant with sequences from corresponding cultures and phenotypic drug-susceptibility testing. Complete genomic analysis, within a week of specimen receipt, cost €217 per sample (excluding personnel costs).

Interpretation: Direct whole-genome sequencing could be used to accurately delineate transmission clusters of tuberculosis and conduct culture-independent surveillance. Compared with conventional approaches, direct whole-genome sequencing allows researchers to do real-time genomic epidemiology and drug resistance surveillance in settings where culture and drug susceptibility testing are not available.

Funding: European Research Council; Ministerio de Ciencia, Innovación y Universidades (Spanish Government).