Literature DB >> 17499044

An antisense RNA inhibits translation by competing with standby ribosomes.

Fabien Darfeuille1, Cecilia Unoson, Jörg Vogel, E Gerhart H Wagner.   

Abstract

Most antisense RNAs in bacteria inhibit translation by competing with ribosomes for translation initiation regions (TIRs) on nascent mRNA. We propose a mechanism by which an antisense RNA inhibits translation without binding directly to a TIR. The tisAB locus encodes an SOS-induced toxin, and IstR-1 is the antisense RNA that counteracts toxicity. We show that full-length tisAB mRNA (+1) is translationally inactive and endonucleolytic processing produces an active mRNA (+42). IstR-1 binding inhibits translation of this mRNA, and subsequent RNase III cleavage generates a truncated, inactive mRNA (+106). In vitro translation, toeprinting, and structure mapping suggest that active, but not inactive, tisAB mRNAs contain an upstream ribosome loading or "standby" site. Standby binding is required for initiation at the highly structured tisB TIR. This may involve ribosome sliding to a transiently open tisB TIR. IstR-1 competes with ribosomes by base pairing to the standby site located approximately 100 nucleotides upstream.

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Year:  2007        PMID: 17499044     DOI: 10.1016/j.molcel.2007.04.003

Source DB:  PubMed          Journal:  Mol Cell        ISSN: 1097-2765            Impact factor:   17.970


  104 in total

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8.  Recent advances in the expression, evolution, and dynamics of prokaryotic genomes.

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Review 9.  Small toxic proteins and the antisense RNAs that repress them.

Authors:  Elizabeth M Fozo; Matthew R Hemm; Gisela Storz
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10.  Translation inhibition from a distance: The small RNA SgrS silences a ribosomal protein S1-dependent enhancer.

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Journal:  Mol Microbiol       Date:  2020-05-02       Impact factor: 3.501

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