Insight into pathogenomics and phylogeography of hypervirulent and highly-lethal Mycobacterium tuberculosis strain cluster

Author:

Mokrousov Igor,Vyazovaya Anna,Shitikov Egor,Badleeva Maria,Belopolskaya Olesya,Bespiatykh Dmitry,Gerasimova Alena,Ioannidis Panayotis,Jiao Weiwei,Khromova Polina,Masharsky Aleksey,Naizabayeva Dinara,Papaventsis Dimitrios,Pasechnik Oksana,Perdigão João,Rastogi Nalin,Shen Adong,Sinkov Viacheslav,Skiba Yuriy,Solovieva Natalia,Tafaj Silva,Valcheva Violeta,Kostyukova Irina,Zhdanova Svetlana,Zhuravlev Viacheslav,Ogarkov Oleg

Abstract

Abstract Background . The Mycobacterium tuberculosis Beijing genotype is globally spread lineage with important medical properties that however vary among its subtypes. M. tuberculosis Beijing 14717-15-cluster was recently discovered as both multidrug-resistant, hypervirulent, and highly-lethal strain circulating in the Far Eastern region of Russia. Here, we aimed to analyze its pathogenomic features and phylogeographic pattern. Results . The study collection included M. tuberculosis DNA collected between 1996 and 2020 in different world regions. The bacterial DNA was subjected to genotyping and whole genome sequencing followed by bioinformatics and phylogenetic analysis. The PCR-based assay to detect specific SNPs of the Beijing 14717-15-cluster was developed and used for its screening in the global collections. Phylogenomic and phylogeographic analysis confirmed endemic prevalence of the Beijing 14717-15-cluster in the Asian part of Russia, and distant common ancestor with isolates from Korea (> 115 SNPs). The Beijing 14717-15-cluster isolates had two common resistance mutations RpsL Lys88Arg and KatG Ser315Thr and belonged to spoligotype SIT269. The Russian isolates of this cluster were from the Asian Russia while 4 isolates were from the Netherlands and Spain. The cluster-specific SNPs that significantly affect the protein function were identified in silico in genes within different categories (lipid metabolism, regulatory proteins, intermediary metabolism and respiration, PE/PPE, cell wall and cell processes). Conclusions . We developed a simple method based on real-time PCR to detect clinically significant MDR and hypervirulent Beijing 14717-15-cluster. Most of the identified cluster-specific mutations were previously unreported and could potentially be associated with increased pathogenic properties of this hypervirulent M. tuberculosis strain. Further experimental study to assess the pathobiological role of these mutations is warranted.

Funder

Russian Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

Infectious Diseases

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