Literature DB >> 35385605

Structure-Activity Relationships for 5'' Modifications of 4,5-Aminoglycoside Antibiotics.

Jonathan C K Quirke1, Girish C Sati2, Amr Sonousi2,3, Marina Gysin4, Klara Haldimann4, Erik C Böttger4, Andrea Vasella5, Sven N Hobbie4, David Crich1,2.   

Abstract

Modification at the 5''-position of 4,5-disubstituted aminoglycoside antibiotics (AGAs) to circumvent inactivation by aminoglycoside modifying enzymes (AMEs) is well known. Such modifications, however, unpredictably impact activity and affect target selectivity thereby hindering drug development. A survey of 5''-modifications of the 4,5-AGAs and the related 5-O-furanosyl apramycin derivatives is presented. In the neomycin and the apralog series, all modifications were well-tolerated, but other 4,5-AGAs require a hydrogen bonding group at the 5''-position for maintenance of antibacterial activity. The 5''-amino modification resulted in parent-like activity, but reduced selectivity against the human cytosolic decoding A site rendering this modification unfavorable in paromomycin, propylamycin, and ribostamycin. Installation of a 5''-formamido group and, to a lesser degree, a 5''-ureido group resulted in parent-like activity without loss of selectivity. These lessons will aid the design of next-generation AGAs capable of circumventing AME action while maintaining high antibacterial activity and target selectivity.
© 2022 Wiley-VCH GmbH.

Entities:  

Keywords:  aminoglycoside modifying enzymes; antibacterial; antiribosomal; ototoxicity

Mesh:

Substances:

Year:  2022        PMID: 35385605      PMCID: PMC9256791          DOI: 10.1002/cmdc.202200120

Source DB:  PubMed          Journal:  ChemMedChem        ISSN: 1860-7179            Impact factor:   3.540


  50 in total

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8.  An Advanced Apralog with Increased in vitro and in vivo Activity toward Gram-negative Pathogens and Reduced ex vivo Cochleotoxicity.

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9.  Synthesis and Antibacterial Activity of Propylamycin Derivatives Functionalized at the 5''- and Other Positions with a View to Overcoming Resistance Due to Aminoglycoside Modifying Enzymes.

Authors:  Dimitrijs Lubriks; Rimants Zogota; Vikram A Sarpe; Takahiko Matsushita; Girish C Sati; Klara Haldimann; Marina Gysin; Erik C Böttger; Andrea Vasella; Edgars Suna; Sven N Hobbie; David Crich
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10.  Engineering the rRNA decoding site of eukaryotic cytosolic ribosomes in bacteria.

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