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Mechanisms of resistance to aminoglycoside antibiotics: overview and perspectives

TLDR
By far the most widespread mechanism of resistance to AGs is the inactivation of these antibiotics by AG-modifying enzymes, and an overview of these mechanisms is provided.
Abstract
Aminoglycoside (AG) antibiotics are used to treat many Gram-negative and some Gram-positive infections and, importantly, multidrug-resistant tuberculosis. Among various bacterial species, resistance to AGs arises through a variety of intrinsic and acquired mechanisms. The bacterial cell wall serves as a natural barrier for small molecules such as AGs and may be further fortified via acquired mutations. Efflux pumps work to expel AGs from bacterial cells, and modifications here too may cause further resistance to AGs. Mutations in the ribosomal target of AGs, while rare, also contribute to resistance. Of growing clinical prominence is resistance caused by ribosome methyltransferases. By far the most widespread mechanism of resistance to AGs is the inactivation of these antibiotics by AG-modifying enzymes. We provide here an overview of these mechanisms by which bacteria become resistant to AGs and discuss their prevalence and potential for clinical relevance.

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High Genomic Diversity of Multi-Drug Resistant Wastewater

TL;DR: The genomic diversity of the indicator Escherichia coli in a German wastewater treatment plant is analysed and it is found that while treatment plants reduce the amount of bacteria released into the environment, they do not reduce the potential for antibiotic resistance of these bacteria.
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Graphene oxide and carbon dots as broad-spectrum antimicrobial agents – a minireview

TL;DR: Carbon-based materials, especially graphene oxide (GO) and carbon dots (C-Dots), are promising candidates for future applications against multidrug-resistant bacteria based on their strong capacity in disruption of microbial membranes.
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Antibiotics, Resistome and Resistance Mechanisms: A Bacterial Perspective.

TL;DR: Proficiency of bacteria to obtain resistance genes generated an unpleasant situation; a grave, but a lot unacknowledged, feature of resistance gene transfer.
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Ribosome-Targeting Antibiotics: Modes of Action, Mechanisms of Resistance, and Implications for Drug Design.

TL;DR: The modes of action of many ribosome-targeting antibiotics are described, the major resistance mechanisms developed by pathogenic bacteria are highlighted, and recent advances in structure-assisted design of new molecules are discussed.
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Antibiotic Resistance and the MRSA Problem

TL;DR: Besides development of new small molecules affecting cell viability, alternative approaches including anti-virulence and bacteriophage therapeutics are being investigated and may become important tools to combat staphylococcal infections in the future.
References
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Journal ArticleDOI

Dissemination of the rmtB gene carried on IncF and IncN plasmids among Enterobacteriaceae in a pig farm and its environment

TL;DR: This study is the first report of rmtB-positive bacteria from farmland soils and indicates that these antibiotic-resistant bacteria and/or resistance genes could be acquired by humans through the food chain.
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A novel multidrug resistance plasmid isolated from an Escherichia coli strain resistant to aminoglycosides

TL;DR: This study investigated the aminoglycoside resistance patterns for 224 Escherichia coli isolates from diseased chickens and ducks in China, characterized a novel MDR plasmid, pXZ, and collected prevalence data on similar resistance plasmids.
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16S rRNA Methyltransferase RmtC in Salmonella enterica Serovar Virchow

TL;DR: The authors screened Salmonella and Escherichia coli isolates, collected 2004–2008 in the United Kingdom, for 16S rRNA methyltransferases and found rmtC was identified in S. enterica serovar Virchow isolates from clinical samples and food.
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Emergence of 16S rRNA methylase gene armA and cocarriage of blaIMP-1 in Pseudomonas aeruginosa isolates from South Korea

TL;DR: This study is the first report of occurrence of armA in P. aeruginosa, and fourteen armA-positive isolates were classified into 8 pulsotypes.
Journal ArticleDOI

Limited diversity in the gene pool allows prediction of third-generation cephalosporin and aminoglycoside resistance in Escherichia coli and Klebsiella pneumoniae.

TL;DR: In a country like Australia, with a background prevalence of resistance to third-generation cephalosporins of 5-10%, this equates to a negative predictive value of >99.5% for non-susceptibility and is therefore suitable for diagnostic application and is an important proof-of-principle that should be tested in other geographic locations.
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