2016
DOI: 10.1128/aac.01344-16
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Genomic Characterization of Colistin Heteroresistance in Klebsiella pneumoniae during a Nosocomial Outbreak

Abstract: dKlebsiella pneumoniae is emerging as an important nosocomial pathogen due to its rapidly increasing multidrug resistance, which has led to a renewed interest in polymyxin antibiotics, such as colistin, as antibiotics of last resort. However, heteroresistance (i.e., the presence of a subpopulation of resistant bacteria in an otherwise susceptible culture) may hamper the effectiveness of colistin treatment in patients. In a previous study, we showed that colistin resistance among extendedspectrum-beta-lactamase… Show more

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Cited by 82 publications
(78 citation statements)
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References 52 publications
(61 reference statements)
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“…Transposases can inactivate a gene that is required for antibiotic susceptibility through insertion. This mechanism has been well characterized in K. pneumoniae , where transposon‐mediated inactivation of mgrB is a common mechanism leading to colistin resistance . Alternatively, transposon insertions can increase the expression of intrinsic resistance genes, as illustrated by transposon‐mediated upregulation of ampC in A. baumannii , causing third‐generation cephalosporin resistance, or increased expression of an efflux system in E. coli , which contributes to fluoroquinolone resistance .…”
Section: Antibiotic‐resistance Surveillance: Bioinformatics Challengementioning
confidence: 99%
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“…Transposases can inactivate a gene that is required for antibiotic susceptibility through insertion. This mechanism has been well characterized in K. pneumoniae , where transposon‐mediated inactivation of mgrB is a common mechanism leading to colistin resistance . Alternatively, transposon insertions can increase the expression of intrinsic resistance genes, as illustrated by transposon‐mediated upregulation of ampC in A. baumannii , causing third‐generation cephalosporin resistance, or increased expression of an efflux system in E. coli , which contributes to fluoroquinolone resistance .…”
Section: Antibiotic‐resistance Surveillance: Bioinformatics Challengementioning
confidence: 99%
“…It is increasingly being recognized as a crucial antibiotic of last resort, particularly in countries where carbapenem resistance is endemic . Resistance to colistin can emerge in Gram‐negative bacteria (particularly in K. pneumoniae and Acinetobacter baumannii ) owing to mutational events, particularly in genes encoding regulators of LPS modification or LPS biosynthesis proteins, which include gene amplification, gene inactivation due to the insertion of an insertion sequence (IS) element in a gene encoding a regulator, or the accumulation of point mutations . While the emergence of resistance during therapy may affect the effectiveness of colistin therapy and is an important cause of outbreaks with colistin‐resistant strains in hospitals, the mutations contributing to the resistant phenotype are fixed on the chromosome and thus cannot be transferred between bacteria.…”
Section: Genomic Epidemiology Of Emergence and Spread Of Antibiotic Rmentioning
confidence: 99%
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“…There are only 2 reports of genomic analysis of colistin-heteroresistant K. pneumoniae isolates, which were multidrug-resistant bacteria: one OXA-48 carbapenemaseproducing strain with a mutation in protein PhoP (7) and five extended-spectrum ␤-lactamase (ESBL)-expressing isolates with mutations in the phoQ, lpxM, and yciM genes, as well as two with mutations on the mgrB gene (the presence of an insertion sequence and deletion) (30). This is the first description of a colistin-heteroresistant Klebsiella pneumoniae isolate in France and the first description of a truncated MgrB protein after an insertion of a single nucleotide.…”
mentioning
confidence: 99%