2014
DOI: 10.1186/1471-2164-15-308
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Genome-wide Mycobacterium tuberculosis variation (GMTV) database: a new tool for integrating sequence variations and epidemiology

Abstract: BackgroundTuberculosis (TB) poses a worldwide threat due to advancing multidrug-resistant strains and deadly co-infections with Human immunodeficiency virus. Today large amounts of Mycobacterium tuberculosis whole genome sequencing data are being assessed broadly and yet there exists no comprehensive online resource that connects M. tuberculosis genome variants with geographic origin, with drug resistance or with clinical outcome.DescriptionHere we describe a broadly inclusive unifying Genome-wide Mycobacteriu… Show more

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Cited by 82 publications
(88 citation statements)
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References 28 publications
(31 reference statements)
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“…In the current work, 58,025 amino acid substitutions in 1,623 Mtb strains recorded in GMTV database [14] were analyzed for their distribution in the global Mtb population. Information about drug associated mutations was obtained from the TB Drug Resistance Mutation Database [8].…”
Section: Statistical Analysis Of Mtb Genomic Polymorphismmentioning
confidence: 99%
See 1 more Smart Citation
“…In the current work, 58,025 amino acid substitutions in 1,623 Mtb strains recorded in GMTV database [14] were analyzed for their distribution in the global Mtb population. Information about drug associated mutations was obtained from the TB Drug Resistance Mutation Database [8].…”
Section: Statistical Analysis Of Mtb Genomic Polymorphismmentioning
confidence: 99%
“…Induction of drug resistance reversion in MDR-TB by FS-1 made it possible to study this phenomenon on the genetic level. Furthermore, statistical analysis of distribution of polymorphic sites in the global Mtb population based on the data from GMTV database [14] allowed getting insight into functional relations between drug resistance mutations of Mtb. A work hypothesis was that FS-1 could cause an active counter-selection of drug resistant variants from Mtb populations by aggravating the cumulated fitness cost of the drug resistance mutations as it was predicted previously by a mathematical model by Cohen and Murray [15].…”
Section: Introductionmentioning
confidence: 99%
“…We identified a SNV (Single Nucleotide Variation) in genomic position G 1097023 A in mprA gene that led to the substitution of an amino acid, glycine to serine at 70 th position (G70S) in one of our clinical isolates VPCI591. This variation was detected in 3% of the global clinical isolates, as analyzed from GMTV database (Chernyaeva et al, 2014) and tbVar database (Joshi et al, 2014) containing about 1553 global clinical isolates of M.tuberculosis. In the light of the identification of MprA as late antigen and its role implied in persistence of M. tuberculosis, we examined the effect SNP.…”
Section: Resultsmentioning
confidence: 99%
“…Database analysis for mutations in Rv0191, Rv3756c, Rv3008, and Rv1667c. Genome-wide Mycobacterium tuberculosis Variation (GMTV) is a database that covers the whole-genome sequencing information of 1,084 M. tuberculosis isolates from various data sets in different regions of Russia (37). The GMTV database contains data involving molecular biology, epidemiology, tuberculosis clinical data, year, region, and drug resistance information for Mycobacterium tuberculosis, which can be used to identify the genetic variation of drug resistance, clinical outcomes, or pathogens related to geographical distribution.…”
Section: Methodsmentioning
confidence: 99%