Literature DB >> 27618454

Expanding Aminoglycoside Resistance Enzyme Regiospecificity by Mutation and Truncation.

Selina Y L Holbrook1, Sylvie Garneau-Tsodikova1.   

Abstract

Aminoglycosides (AGs) are broad-spectrum antibiotics famous for their antibacterial activity against Gram-positive and Gram-negative bacteria, as well as mycobacteria. In the United States, the most prescribed AGs, including amikacin (AMK), gentamicin (GEN), and tobramycin (TOB), are vital components of the treatment for resistant bacterial infections. Arbekacin (ABK), a semisynthetic AG, is widely used for the treatment of resistant Pseudomonas aeruginosa and methicillin-resistant Staphylococcus aureus in Asia. However, the rapid emergence and development of bacterial resistance are limiting the clinical application of AG antibiotics. Of all bacterial resistance mechanisms against AGs, the acquisition of AG-modifying enzymes (AMEs) by bacteria is the most common. It was previously reported that a variant of a bifunctional AME, the 6'-N-AG acetyltransferase-Ie/2″-O-AG phosphotransferase-Ia [AAC(6')-Ie/APH(2″)-Ia], containing a D80G point mutation and a truncation after amino acid 240 modified ABK and AMK at a new position, the 4‴-amine, therefore displaying a change in regiospecificity. In this study, we aimed to verify the altered regiospecificity of this bifunctional enzyme by mutation and truncation for the potential of derivatizing AGs with chemoenzymatic reactions. With the three variant enzymes in this study that contained either mutation only (D80G), truncation only (1-240), or mutation and truncation (D80G-1-240), we characterized their activity by profiling their substrate promiscuity, determined their kinetics parameters, and performed mass spectrometry to determine how and where ABK and AMK were acetylated by these enzymes. We found that the three mutant enzymes possessed distinct acetylation regiospecificity compared to that of the bifunctional AAC(6')-Ie/APH(2″)-Ia enzyme and the functional AAC(6')-Ie domain [AAC(6')/APH(2″)-1-194].

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Year:  2016        PMID: 27618454      PMCID: PMC5174979          DOI: 10.1021/acs.biochem.6b00770

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  46 in total

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Journal:  FEMS Microbiol Lett       Date:  2000-09-15       Impact factor: 2.742

2.  Domain-domain interactions in the aminoglycoside antibiotic resistance enzyme AAC(6')-APH(2'').

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Journal:  Biochemistry       Date:  2004-08-03       Impact factor: 3.162

3.  Amphiphilic Tobramycin Analogues as Antibacterial and Antifungal Agents.

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4.  Biochemical and structural analysis of an Eis family aminoglycoside acetyltransferase from bacillus anthracis.

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Journal:  Biochemistry       Date:  2015-05-12       Impact factor: 3.162

5.  Redesign of substrate specificity and identification of the aminoglycoside binding residues of Eis from Mycobacterium tuberculosis.

Authors:  Benjamin C Jennings; Kristin J Labby; Keith D Green; Sylvie Garneau-Tsodikova
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Review 6.  Aminoglycoside-induced translational read-through in disease: overcoming nonsense mutations by pharmacogenetic therapy.

Authors:  L V Zingman; S Park; T M Olson; A E Alekseev; A Terzic
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Journal:  Am J Respir Cell Mol Biol       Date:  2014-04       Impact factor: 6.914

8.  Biochemical and structural analysis of aminoglycoside acetyltransferase Eis from Anabaena variabilis.

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9.  Specificity of 4'''-acetylation by an aminoglycoside-modifying enzyme in arbekacin-resistant strains of methicillin-resistant Staphylococcus aureus.

Authors:  S Fujimura; Y Tokue; H Takahashi; T Nukiwa; A Watanabe
Journal:  Tohoku J Exp Med       Date:  1998-09       Impact factor: 1.848

10.  A random sequential mechanism of aminoglycoside acetylation by Mycobacterium tuberculosis Eis protein.

Authors:  Oleg V Tsodikov; Keith D Green; Sylvie Garneau-Tsodikova
Journal:  PLoS One       Date:  2014-04-03       Impact factor: 3.240

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Journal:  Chem Soc Rev       Date:  2018-02-19       Impact factor: 54.564

2.  Nucleoside triphosphate cosubstrates control the substrate profile and efficiency of aminoglycoside 3'-O-phosphotransferase type IIa.

Authors:  Selina Y L Holbrook; Matthew S Gentry; Oleg V Tsodikov; Sylvie Garneau-Tsodikova
Journal:  Medchemcomm       Date:  2018-07-16       Impact factor: 3.597

3.  Plasticity of Aminoglycoside Binding to Antibiotic Kinase APH(2″)-Ia.

Authors:  Shane J Caldwell; Albert M Berghuis
Journal:  Antimicrob Agents Chemother       Date:  2018-06-26       Impact factor: 5.191

4.  Investigating the promiscuity of the chloramphenicol nitroreductase from Haemophilus influenzae towards the reduction of 4-nitrobenzene derivatives.

Authors:  Keith D Green; Marina Y Fosso; Abdelrahman S Mayhoub; Sylvie Garneau-Tsodikova
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5.  The evolution of substrate discrimination in macrolide antibiotic resistance enzymes.

Authors:  Andrew C Pawlowski; Peter J Stogios; Kalinka Koteva; Tatiana Skarina; Elena Evdokimova; Alexei Savchenko; Gerard D Wright
Journal:  Nat Commun       Date:  2018-01-09       Impact factor: 14.919

Review 6.  Amikacin: Uses, Resistance, and Prospects for Inhibition.

Authors:  Maria S Ramirez; Marcelo E Tolmasky
Journal:  Molecules       Date:  2017-12-19       Impact factor: 4.411

7.  Development of 6'-N-Acylated Isepamicin Analogs with Improved Antibacterial Activity Against Isepamicin-Resistant Pathogens.

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