Structure-Activity Relationships among the Kanamycin Aminoglycosides: Role of Ring I Hydroxyl and Amino Groups

Salian, Sumantha; Matt, Tanja; Akbergenov, Rashid; Harish, Shinde; Meyer, Martin; Duscha, Stefan; Shcherbakov, Dmitry; Bernet, Bruno; Vasella, Andrea; Westhof, Éric; Böttger, Erik C.

doi:10.1128/aac.01326-12

Cited by 50 publications

(43 citation statements)

References 43 publications

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“…Ataluren's influence over the extent of specific tRNA selection implies that this drug's target could be the ribosome, a conclusion consistent with the drug's markedly diminished efficacy in the presence of tobramycin (Fig. 4), an aminoglycoside known to bind to the ribosome's A site (34). The apparent tRNA selection bias also suggests that both endogenous and ataluren-stimulated near-cognate tRNA mispairing are not random processes and that factors contributing to the apparent preferences are conserved.…”

Section: Discussionmentioning

confidence: 71%

“…Taken together, these data suggest that some nonstandard base pairs are favored over others for near-cognate tRNA insertion at PTCs and that the geometry of the base pairs is the most likely determinant of this bias. significant response to ataluren if they were concurrently being treated with inhaled tobramycin, an aminoglycoside with strong affinity for the ribosomal A site (34). This observation suggested that tobramycin might be an inhibitor of ataluren's nonsense suppression activity, a possibility considered in the experiments of Fig.…”

Section: Resultsmentioning

confidence: 84%

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Ataluren stimulates ribosomal selection of near-cognate tRNAs to promote nonsense suppression

Roy

Friesen

Tomizawa

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

188

218

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A premature termination codon (PTC) in the ORF of an mRNA generally leads to production of a truncated polypeptide, accelerated degradation of the mRNA, and depression of overall mRNA expression. Accordingly, nonsense mutations cause some of the most severe forms of inherited disorders. The small-molecule drug ataluren promotes therapeutic nonsense suppression and has been thought to mediate the insertion of near-cognate tRNAs at PTCs. However, direct evidence for this activity has been lacking. Here, we expressed multiple nonsense mutation reporters in human cells and yeast and identified the amino acids inserted when a PTC occupies the ribosomal A site in control, ataluren-treated, and aminoglycoside-treated cells. We find that ataluren’s likely target is the ribosome and that it produces full-length protein by promoting insertion of near-cognate tRNAs at the site of the nonsense codon without apparent effects on transcription, mRNA processing, mRNA stability, or protein stability. The resulting readthrough proteins retain function and contain amino acid replacements similar to those derived from endogenous readthrough, namely Gln, Lys, or Tyr at UAA or UAG PTCs and Trp, Arg, or Cys at UGA PTCs. These insertion biases arise primarily from mRNA:tRNA mispairing at codon positions 1 and 3 and reflect, in part, the preferred use of certain nonstandard base pairs, e.g., U-G. Ataluren’s retention of similar specificity of near-cognate tRNA insertion as occurs endogenously has important implications for its general use in therapeutic nonsense suppression.

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Section: Discussionmentioning

confidence: 71%

Section: Resultsmentioning

confidence: 84%

Ataluren stimulates ribosomal selection of near-cognate tRNAs to promote nonsense suppression

Roy

Friesen

Tomizawa

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

188

218

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“…In addition to promoting mistranslation, neomycin and paromomycin also negatively impact assembly of the 30S ribosomal subunit (42), although the 4,6-disubstituted aminoglycosides were not examined in this study and it is unclear if they have ever been assessed in this context. Similarly, switching the 6= substituent of ring 1 of 4,5-versus 4,6-disubstituted aminoglycosides differentially impacts ribosome inhibitory activity-replacing the 6= NH 2 group with an OH has a major negative impact on ribosome inhibition by the 4,6-disubstituted aminoglycoside kanamycin, while replacing the NH 2 of neomycin with OH (resulting in paromomycin) has a minimal impact (43). In any case, there are clearly differences in the AmgRS-responsive stress signals propagated by neomycin and paromomycin compared to the other aminoglycosides.…”

Section: Discussionmentioning

confidence: 99%

Mutational Activation of the AmgRS Two-Component System in Aminoglycoside-Resistant Pseudomonas aeruginosa

Lau

Fraud

Jones

et al. 2013

Antimicrob Agents Chemother

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The amgRS operon encodes a presumed membrane stress-responsive two-component system linked to intrinsic aminoglycoside resistance in Pseudomonas aeruginosa. Genome sequencing of a lab isolate showing modest pan-aminoglycoside resistance, strain K2979, revealed a number of mutations, including a substitution in amgS that produced an R182C change in the AmgS sensor kinase product of this gene. Introduction of this mutation into an otherwise wild-type strain recapitulated the resistance phenotype, while correcting the mutation in the resistant mutant abrogated the resistant phenotype, confirming that the amgS mutation is responsible for the aminoglycoside resistance of strain K2979. The amgS R182 mutation promoted an AmgR-dependent, 2-to 3-fold increase in expression of the AmgRS target genes htpX and PA5528, mirroring the impact of aminoglycoside exposure of wild-type cells on htpX and PA5528 expression. This suggests that amgS R182 is a gain-of-function mutation that activates AmgS and the AmgRS two-component system in promoting modest resistance to aminoglycosides. Screening of several pan-aminoglycoside-resistant clinical isolates of P. aeruginosa revealed three that showed elevated htpX and PA5528 expression and harbored single amino acid-altering mutations in amgS (V121G or D106N) and no mutations in amgR. Introduction of the amgS V121G mutation into wild-type P. aeruginosa generated a resistance phenotype reminiscent of the amgS R182 mutant and produced a 2-to 3-fold increase in htpX and PA5528 expression, confirming that it, too, is a gain-of-function aminoglycoside resistance-promoting mutation. These results highlight the contribution of amgS mutations and activation of the AmgRS two-component system to acquired aminoglycoside resistance in lab and clinical isolates of P. aeruginosa.

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“…Several derivatives were synthesized by linking INH with another conventional drug (morpholine, 2-amino methyl pyridine, benzylamine, PAS, ciprofloxacin) by the CH fragment and evaluated for the activities. The compounds 2-Hydroxy-4-{[(isonicotinoyl hydra zono) methyl] amino}benzoic acid (19) and 1-Cyclopropyl-6-fluoro-7-{4-[(isonicotinoyl hydra zono) methyl] piperazin-1-yl}-4-oxo-1,4-dihydro quinoline-3-carboxylic acid (20) were found to possess higher activity against non-tuberculous strains than INH 62 . …”

Section: Isoniazid As Targetmentioning

confidence: 99%

Untitled

2017

IJPSR

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Tuberculosis (TB) remains one of the main causes of death from an infectious disease till date. Recent data shows that currently 9.6 million people are infected with TB. Over 95% of TB deaths occur in low-and middle-income countries and it is among the top 5 causes of death for women aged 15 to 44. TB is a leading killer of HIV-positive people and around 1 in 3HIV deaths was due to TB. Furthermore, multidrug-resistant (MDR)-TB and extensively drug-resistant (XDR)-TB is spreading and poses a major threat to progress in global TB control program. The emergence of drug resistant TB strains makes the invention of new molecular scaffold a priority. One of the possible strategies to overcome drug resistance in an economic and simple manner would involve re-engineering and repositioning of some old drugs to obtain derivatives that can work on resistant TB bacilli. These may have enhanced bioavailability, be more effective, and serve as cost-effective substitutes, as compared to new drugs identified through conventional methods of drug discovery and development. In view of this, the present review aims to provide a summarizing report on the derivatives of firstline drugs (isoniazid and pyrazinamide) that have the potential to conquer the resistance to the parental drug and could thus serve as effective alternatives.

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Structure-Activity Relationships among the Kanamycin Aminoglycosides: Role of Ring I Hydroxyl and Amino Groups

Cited by 50 publications

References 43 publications

Ataluren stimulates ribosomal selection of near-cognate tRNAs to promote nonsense suppression

Ataluren stimulates ribosomal selection of near-cognate tRNAs to promote nonsense suppression

Mutational Activation of the AmgRS Two-Component System in Aminoglycoside-Resistant Pseudomonas aeruginosa

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