Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.

Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.

Synthetic oligonucleotides targeting functional regions of the prokaryotic rRNA could be promising antimicrobial agents. Indeed, such oligonucleotides were proven to inhibit bacterial growth. 2'-O-methylated (2'-O-Me) oligoribonucleotides with a sequence complementary to the decoding site...

Full description

Bibliographic Details
Main Authors: Maciej Jasiński, Marta Kulik, Monika Wojciechowska, Ryszard Stolarski, Joanna Trylska
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2018-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5774723?pdf=render
id doaj-4fc34545ffec48d6aec38b239f7a18bb
record_format Article
spelling doaj-4fc34545ffec48d6aec38b239f7a18bb2020-11-24T21:30:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032018-01-01131e019113810.1371/journal.pone.0191138Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.Maciej JasińskiMarta KulikMonika WojciechowskaRyszard StolarskiJoanna TrylskaSynthetic oligonucleotides targeting functional regions of the prokaryotic rRNA could be promising antimicrobial agents. Indeed, such oligonucleotides were proven to inhibit bacterial growth. 2'-O-methylated (2'-O-Me) oligoribonucleotides with a sequence complementary to the decoding site in 16S rRNA were reported as inhibitors of bacterial translation. However, the binding mode and structures of the formed complexes, as well as the level of selectivity of the oligonucleotides between the prokaryotic and eukaryotic target, were not determined. We have analyzed three 2'-O-Me oligoribonucleotides designed to hybridize with the models of the prokaryotic rRNA containing two neighboring aminoglycoside binding pockets. One pocket is the paromomycin/kanamycin binding site corresponding to the decoding site in the small ribosomal subunit and the other one is the close-by hygromycin B binding site whose dynamics has not been previously reported. Molecular dynamics (MD) simulations, as well as isothermal titration calorimetry, gel electrophoresis and spectroscopic studies have shown that the eukaryotic rRNA model is less conformationally stable (in terms of hydrogen bonds and stacking interactions) than the corresponding prokaryotic one. In MD simulations of the eukaryotic construct, the nucleotide U1498, which plays an important role in correct positioning of mRNA during translation, is flexible and spontaneously flips out into the solvent. In solution studies, the 2'-O-Me oligoribonucleotides did not interact with the double stranded rRNA models but all formed stable complexes with the single-stranded prokaryotic target. 2'-O-Me oligoribonucleotides with one and two mismatches bound less tightly to the eukaryotic target. This shows that at least three mismatches between the 2'-O-Me oligoribonucleotide and eukaryotic rRNA are required to ensure target selectivity. The results also suggest that, in the ribosome environment, the strand invasion is the preferred binding mode of 2'-O-Me oligoribonucleotides targeting the aminoglycoside binding sites in 16S rRNA.http://europepmc.org/articles/PMC5774723?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Maciej Jasiński
Marta Kulik
Monika Wojciechowska
Ryszard Stolarski
Joanna Trylska
spellingShingle Maciej Jasiński
Marta Kulik
Monika Wojciechowska
Ryszard Stolarski
Joanna Trylska
Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
PLoS ONE
author_facet Maciej Jasiński
Marta Kulik
Monika Wojciechowska
Ryszard Stolarski
Joanna Trylska
author_sort Maciej Jasiński
title Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
title_short Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
title_full Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
title_fullStr Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
title_full_unstemmed Interactions of 2'-O-methyl oligoribonucleotides with the RNA models of the 30S subunit A-site.
title_sort interactions of 2'-o-methyl oligoribonucleotides with the rna models of the 30s subunit a-site.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2018-01-01
description Synthetic oligonucleotides targeting functional regions of the prokaryotic rRNA could be promising antimicrobial agents. Indeed, such oligonucleotides were proven to inhibit bacterial growth. 2'-O-methylated (2'-O-Me) oligoribonucleotides with a sequence complementary to the decoding site in 16S rRNA were reported as inhibitors of bacterial translation. However, the binding mode and structures of the formed complexes, as well as the level of selectivity of the oligonucleotides between the prokaryotic and eukaryotic target, were not determined. We have analyzed three 2'-O-Me oligoribonucleotides designed to hybridize with the models of the prokaryotic rRNA containing two neighboring aminoglycoside binding pockets. One pocket is the paromomycin/kanamycin binding site corresponding to the decoding site in the small ribosomal subunit and the other one is the close-by hygromycin B binding site whose dynamics has not been previously reported. Molecular dynamics (MD) simulations, as well as isothermal titration calorimetry, gel electrophoresis and spectroscopic studies have shown that the eukaryotic rRNA model is less conformationally stable (in terms of hydrogen bonds and stacking interactions) than the corresponding prokaryotic one. In MD simulations of the eukaryotic construct, the nucleotide U1498, which plays an important role in correct positioning of mRNA during translation, is flexible and spontaneously flips out into the solvent. In solution studies, the 2'-O-Me oligoribonucleotides did not interact with the double stranded rRNA models but all formed stable complexes with the single-stranded prokaryotic target. 2'-O-Me oligoribonucleotides with one and two mismatches bound less tightly to the eukaryotic target. This shows that at least three mismatches between the 2'-O-Me oligoribonucleotide and eukaryotic rRNA are required to ensure target selectivity. The results also suggest that, in the ribosome environment, the strand invasion is the preferred binding mode of 2'-O-Me oligoribonucleotides targeting the aminoglycoside binding sites in 16S rRNA.
url http://europepmc.org/articles/PMC5774723?pdf=render
work_keys_str_mv AT maciejjasinski interactionsof2omethyloligoribonucleotideswiththernamodelsofthe30ssubunitasite
AT martakulik interactionsof2omethyloligoribonucleotideswiththernamodelsofthe30ssubunitasite
AT monikawojciechowska interactionsof2omethyloligoribonucleotideswiththernamodelsofthe30ssubunitasite
AT ryszardstolarski interactionsof2omethyloligoribonucleotideswiththernamodelsofthe30ssubunitasite
AT joannatrylska interactionsof2omethyloligoribonucleotideswiththernamodelsofthe30ssubunitasite
_version_ 1725963335534379008

Similar Items