Literature DB >> 24754005

Evolutionary Origin and Conserved Structural Building Blocks of Riboswitches and Ribosomal RNAs: Riboswitches as Probable Target Sites for Aminoglycosides Interaction.

Elnaz Mehdizadeh Aghdam1, Abolfazl Barzegar2, Mohammad Saeid Hejazi3.   

Abstract

PURPOSE: Riboswitches, as noncoding RNA sequences, control gene expression through direct ligand binding. Sporadic reports on the structural relation of riboswitches with ribosomal RNAs (rRNA), raises an interest in possible similarity between riboswitches and rRNAs evolutionary origins. Since aminoglycoside antibiotics affect microbial cells through binding to functional sites of the bacterial rRNA, finding any conformational and functional relation between riboswitches/rRNAs is utmost important in both of medicinal and basic research.
METHODS: Analysis of the riboswitches structures were carried out using bioinformatics and computational tools. The possible functional similarity of riboswitches with rRNAs was evaluated based on the affinity of paromomycin antibiotic (targeting "A site" of 16S rRNA) to riboswitches via docking method.
RESULTS: There was high structural similarity between riboswitches and rRNAs, but not any particular sequence based similarity between them was found. The building blocks including "hairpin loop containing UUU", "peptidyl transferase center conserved hairpin A loop"," helix 45" and "S2 (G8) hairpin" as high identical rRNA motifs were detected in all kinds of riboswitches. Surprisingly, binding energies of paromomycin with different riboswitches are considerably better than the binding energy of paromomycin with "16S rRNA A site". Therefore the high affinity of paromomycin to bind riboswitches in comparison with rRNA "A site" suggests a new insight about riboswitches as possible targets for aminoglycoside antibiotics.
CONCLUSION: These findings are considered as a possible supporting evidence for evolutionary origin of riboswitches/rRNAs and also their role in the exertion of antibiotics effects to design new drugs based on the concomitant effects via rRNA/riboswitches.

Entities:  

Keywords:  Docking; Motif; Ribosomal RNA; Riboswitch; Structural similarity

Year:  2014        PMID: 24754005      PMCID: PMC3992957          DOI: 10.5681/apb.2014.033

Source DB:  PubMed          Journal:  Adv Pharm Bull        ISSN: 2228-5881


  51 in total

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Review 2.  Gene regulation by riboswitches.

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3.  Highly modular structure and ligand binding by conformational capture in a minimalistic riboswitch.

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Authors:  Donna K Hendrix; Steven E Brenner; Stephen R Holbrook
Journal:  Q Rev Biophys       Date:  2006-07-03       Impact factor: 5.318

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Authors:  Alejandro Toledo-Arana; Francis Repoila; Pascale Cossart
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6.  Selective recognition of RNA helices containing dangling ends by a quinoline derivative.

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7.  The crystal structure of an all-RNA hammerhead ribozyme: a proposed mechanism for RNA catalytic cleavage.

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Review 8.  Amino acid recognition and gene regulation by riboswitches.

Authors:  Alexander Serganov; Dinshaw J Patel
Journal:  Biochim Biophys Acta       Date:  2009-07-18

9.  Computational study of unfolding and regulation mechanism of preQ1 riboswitches.

Authors:  Zhou Gong; Yunjie Zhao; Changjun Chen; Yi Xiao
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10.  DIAL: a web server for the pairwise alignment of two RNA three-dimensional structures using nucleotide, dihedral angle and base-pairing similarities.

Authors:  F Ferrè; Y Ponty; W A Lorenz; Peter Clote
Journal:  Nucleic Acids Res       Date:  2007-06-13       Impact factor: 16.971

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  2 in total

1.  Development of a new oligonucleotide block location-based feature extraction (BLBFE) method for the classification of riboswitches.

Authors:  F Golabi; Mousa Shamsi; M H Sedaaghi; A Barzegar; Mohammad Saeid Hejazi
Journal:  Mol Genet Genomics       Date:  2020-01-04       Impact factor: 3.291

2.  Development of a new sequential block finding strategy for detection of conserved sequences in riboswitches.

Authors:  Faegheh Golabi; Mousa Shamsi; Mohammad Hosein Sedaaghi; Abolfazl Barzegar; Mohammad Saeid Hejazi
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  2 in total

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