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Mechanisms of resistance to aminoglycoside antibiotics: overview and perspectives

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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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Ribosome-Targeting Antibiotics: Modes of Action, Mechanisms of Resistance, and Implications for Drug Design.

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Antibiotic Resistance and the MRSA Problem

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References
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Journal ArticleDOI

An In Silico Approach for Characterization of an Aminoglycoside Antibiotic-Resistant Methyltransferase Protein from Pyrococcus furiosus (DSM 3638)

TL;DR: Pyrococcus furiosus is a hyperthermophilic archaea, and binding of the geneticin bound to the eubacterial 16S rRNA A-site in the active site of the PF0847 gave the indication to predict the protein responsible for aminoglycoside antibiotic resistance.
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Salmonella enterica serotype Gambia with CTX-M-3 and armA resistance markers: nosocomial infections with a fatal outcome

TL;DR: This is the first report of S. Gambia exhibiting CTX-M-3 and armA markers involved in serious infections, and the isolates showed indistinguishable genotypes and infrequent resistance markers.
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The Emergence of the 16S rRNA Methyltransferase RmtB in a Multidrug-Resistant Serratia marcescens Isolate in China

TL;DR: The acquisition of multidrug resistance in nosocomial pathogens such as Serratia marcescens has been reported in the absence of antibiotic selection pressure and the broad antimicrobial spectrum of aminoglycosides suggest the possible use of these antibiotics as a therapy for life-threatening infections.
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