Literature DB >> 21764915

Membrane proteases and aminoglycoside antibiotic resistance.

Aaron Hinz1, Samuel Lee, Kyle Jacoby, Colin Manoil.   

Abstract

We present genetic studies that help define the functional network underlying intrinsic aminoglycoside resistance in Pseudomonas aeruginosa. Our analysis shows that proteolysis, particularly that controlled by the membrane protease FtsH, is a major determinant of resistance. First, we examined the consequences of inactivating genes controlled by AmgRS, a two-component regulator required for intrinsic tobramycin resistance. Three of the gene products account for resistance: a modulator of FtsH protease (YccA), a membrane protease (HtpX), and a membrane protein of unknown function (PA5528). Second, we screened mutations inactivating 66 predicted proteases and related functions. Insertions inactivating two FtsH protease accessory factors (HflK and HflC) and a cytoplasmic protease (HslUV) increased tobramycin sensitivity. Finally, we generated an ftsH deletion mutation. The mutation dramatically increased aminoglycoside sensitivity. Many of the functions whose inactivation increased sensitivity appeared to act independently, since multiple mutations led to additive or synergistic effects. Up to 500-fold increases in tobramycin sensitivity were observed. Most of the mutations also were highly pleiotropic, increasing sensitivity to a membrane protein hybrid, several classes of antibiotics, alkaline pH, NaCl, and other compounds. We propose that the network of proteases provides robust protection from aminoglycosides and other substances through the elimination of membrane-disruptive mistranslation products.
Copyright © 2011, American Society for Microbiology. All Rights Reserved.

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Year:  2011        PMID: 21764915      PMCID: PMC3165699          DOI: 10.1128/JB.05133-11

Source DB:  PubMed          Journal:  J Bacteriol        ISSN: 0021-9193            Impact factor:   3.490


  35 in total

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6.  Proteolytic activity of HtpX, a membrane-bound and stress-controlled protease from Escherichia coli.

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7.  Structural basis for aminoglycoside inhibition of bacterial ribosome recycling.

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  37 in total

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4.  Comprehensive Genome-wide Perturbations via CRISPR Adaptation Reveal Complex Genetics of Antibiotic Sensitivity.

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6.  Transcriptional and Mutational Profiling of an Aminoglycoside-Resistant Pseudomonas aeruginosa Small-Colony Variant.

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7.  Mechanisms of Resistance to Aminoglycoside Antibiotics: Overview and Perspectives.

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8.  Mutational activation of the AmgRS two-component system in aminoglycoside-resistant Pseudomonas aeruginosa.

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9.  Determinants of intrinsic aminoglycoside resistance in Pseudomonas aeruginosa.

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