Literature DB >> 16923950

23S rRNA 2058A-->G alteration mediates ketolide resistance in combination with deletion in L22.

Rita Berisio1, Natascia Corti, Peter Pfister, Ada Yonath, Erik C Böttger.   

Abstract

Resistance to macrolides and ketolides occurs mainly via alterations in RNA moieties of the drug-binding site. Using an A2058G mutant of Mycobacterium smegmatis, additional telithromycin resistance was acquired via deletion of 15 residues from protein L22. Molecular modeling, based on the crystal structure of the large ribosomal subunit from Deinococcus radiodurans complexed with telithromycin, shows that the telithromycin carbamate group is located in the proximity of the tip of the L22 hairpin-loop, allowing for weak interactions between them. These weak interactions may become more important once the loss of A2058 interactions destabilizes drug binding, presumably resulting in a shift of the drug toward the other side of the tunnel, namely, to the vicinity of L22. Hence, the deletion of 15 residues from L22 may further destabilize telithromycin binding and confer telithromycin resistance. Such deletions may also lead to notable differences in the tunnel outline, as well as to an increase of its diameter to a size, allowing the progression of the nascent chain.

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Year:  2006        PMID: 16923950      PMCID: PMC1635173          DOI: 10.1128/AAC.00767-06

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  29 in total

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6.  23S rRNA base pair 2057-2611 determines ketolide susceptibility and fitness cost of the macrolide resistance mutation 2058A-->G.

Authors:  Peter Pfister; Natascia Corti; Sven Hobbie; Christian Bruell; Raz Zarivach; Ada Yonath; Erik C Böttger
Journal:  Proc Natl Acad Sci U S A       Date:  2005-03-28       Impact factor: 11.205

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3.  In vitro antibacterial activity of α-methoxyimino acylide derivatives against macrolide-resistant pathogens and mutation analysis in 23S rRNA.

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6.  A High Throughput Screening Assay for Anti-Mycobacterial Small Molecules Based on Adenylate Kinase Release as a Reporter of Cell Lysis.

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Review 7.  Ribosomal Antibiotics: Contemporary Challenges.

Authors:  Tamar Auerbach-Nevo; David Baram; Anat Bashan; Matthew Belousoff; Elinor Breiner; Chen Davidovich; Giuseppe Cimicata; Zohar Eyal; Yehuda Halfon; Miri Krupkin; Donna Matzov; Markus Metz; Mruwat Rufayda; Moshe Peretz; Ophir Pick; Erez Pyetan; Haim Rozenberg; Moran Shalev-Benami; Itai Wekselman; Raz Zarivach; Ella Zimmerman; Nofar Assis; Joel Bloch; Hadar Israeli; Rinat Kalaora; Lisha Lim; Ofir Sade-Falk; Tal Shapira; Leena Taha-Salaime; Hua Tang; Ada Yonath
Journal:  Antibiotics (Basel)       Date:  2016-06-29

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  8 in total

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