Kinetics of Macrolide Action

Lovmar, Martin; Tenson, Tanel; Ehrenberg, Måns

doi:10.1074/jbc.m401625200

Cited by 58 publications

(36 citation statements)

References 37 publications

(57 reference statements)

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“…3A) and the rate constants obtained from our cell-free in vitro translation system (Table 2 and Ref. 21) are sufficient to fully account for the in vivo induced resistance in a large interval of erythromycin concentrations and peptide expression levels (Figs. 3, B and C (and inset)).…”

Section: Discussionmentioning

confidence: 99%

“…Expression of a mini-gene buried in the 23 S rRNA causes low level resistance to erythromycin (6), and it has been suggested that synthesis of this resistance peptide on an erythromycin-containing ribosome can clean it from the drug, thereby making an erythromycin-free 50 S subunit available for a new round of initiation of protein synthesis with another mRNA (8). When the nascent peptide is longer than six to eight amino acids, it covers the erythromycin binding site, which makes the ribosome refractory to further inhibition by erythromycin, allowing for synthesis of full-length proteins (3,21).…”

Section: Discussionmentioning

confidence: 99%

“…1). Because the two drugs have overlapping ribosomal binding sites (1,20,21), josamycin cannot bind and shut down peptide synthesis until after dissociation of erythromycin from the 50 S subunit. The josamycin concentration used in the chase (83 M) leads to an association rate of 2.7 s Ϫ1 (21).…”

Section: Stoichiometric Removal Of Erythromycin By Resistance Peptidementioning

confidence: 99%

“…We constructed a model for erythromycin resistance in bacterial populations (Fig. 3A) based on these and other parameters (listed in the supplemental material) for protein synthesis obtained from our cell-free mRNA translation system (21). The model (detailed description in the supplemental material) contains seven different states of the large ribosomal subunit (50 S) (Fig.…”

Section: Dissociation Of Erythromycin During Different Stages Of Resimentioning

confidence: 99%

“…The value of the rate constant for dissociation of erythromycin from ribosomes synthesizing the control peptide was estimated as 0.01 s Ϫ1 (Fig. 1B), which corresponds to the rate constant for spontaneous dissociation of erythromycin from empty ribosomes (21). In contrast, the value of the rate constant for dissociation of erythromycin from ribosomes synthesizing the resistance peptide was estimated as 0.03 s Ϫ1 , a value coinciding with the rate (s Ϫ1 ) of pentapeptide synthesis per ribosome in the absence of josamycin (Fig.…”

Section: Stoichiometric Removal Of Erythromycin By Resistance Peptidementioning

confidence: 99%

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The Molecular Mechanism of Peptide-mediated Erythromycin Resistance

Lovmar

Nilsson

Vimberg

et al. 2006

Journal of Biological Chemistry

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The macrolide antibiotic erythromycin binds at the entrance of the nascent peptide exit tunnel of the large ribosomal subunit and blocks synthesis of peptides longer than between six and eight amino acids. Expression of a short open reading frame in 23 S rRNA encoding five amino acids confers resistance to erythromycin by a mechanism that depends strongly on both the sequence and the length of the peptide. In this work we have used a cell-free system for protein synthesis with components of high purity to clarify the molecular basis of the mechanism. We have found that the nascent resistance peptide interacts with erythromycin and destabilizes its interaction with 23 S rRNA. It is, however, in the termination step when the pentapeptide is removed from the peptidyl-tRNA by a class 1 release factor that erythromycin is ejected from the ribosome with high probability. Synthesis of a hexa-or heptapeptide with the same five N-terminal amino acids neither leads to ejection of erythromycin nor to drug resistance. We propose a structural model for the resistance mechanism, which is supported by docking studies. The rate constants obtained from our biochemical experiments are also used to predict the degree of erythromycin resistance conferred by varying levels of resistance peptide expression in living Escherichia coli cells subjected to varying concentrations of erythromycin. These model predictions are compared with experimental observations from growing bacterial cultures, and excellent agreement is found between theoretical prediction and experimental observation.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Stoichiometric Removal Of Erythromycin By Resistance Peptidementioning

confidence: 99%

Section: Dissociation Of Erythromycin During Different Stages Of Resimentioning

confidence: 99%

Section: Stoichiometric Removal Of Erythromycin By Resistance Peptidementioning

confidence: 99%

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The Molecular Mechanism of Peptide-mediated Erythromycin Resistance

Lovmar

Nilsson

Vimberg

et al. 2006

Journal of Biological Chemistry

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Comprehensive proteome analysis of Mycobacterium ulcerans and quantitative comparison of mycolactone biosynthesis

et al. 2008

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Mycobacterium ulcerans is the causative agent of Buruli ulcer, a rapidly emerging human disease in which mycolactone, a cytotoxic and immunosuppressive macrocyclic polyketide, is responsible for massive skin destruction. The genome sequencing of M. ulcerans has recently been accomplished (http://genolist.pasteur.fr/BuruList/) enabling the first proteome study of this important human pathogen. Here, we present a comprehensive proteome analysis of different subcellular fractions and culture supernatant of in vitro grown M. ulcerans. By a combination of gel-based and gel-free techniques for protein and peptide separation with subsequent analysis by MS, we identified 1074 different proteins, corresponding to 25% of the protein-coding DNA sequence. Interestingly, new information was obtained about central metabolism and lipid biosynthesis, and as many as 192 conserved hypothetical proteins were found. Comparative analysis of the wild-type strain and an isogenic mycolactone-deficient mutant, by 2-DE and iTRAQ labeling of the cytoplasmic fraction, revealed differences in the expression profiles of proteins involved in lipid metabolism and information pathways, as well as stress responses.

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Antibiotic Discovery and Development

Dougherty¹,

Pucci²

2012

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Kinetics of Macrolide Action

Cited by 58 publications

References 37 publications

The Molecular Mechanism of Peptide-mediated Erythromycin Resistance

The Molecular Mechanism of Peptide-mediated Erythromycin Resistance

Comprehensive proteome analysis of Mycobacterium ulcerans and quantitative comparison of mycolactone biosynthesis

Antibiotic Discovery and Development

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