Structural Flexibility Enables Alternative Maturation, ARGONAUTE Sorting and Activities of miR168, a Global Gene Silencing Regulator in Plants
In eukaryotes, the RNase-III Dicer often produces length/sequence microRNA (miRNA) variants, called “isomiRs”, owing to intrinsic structural/sequence determinants of the miRNA precursors (pre-miRNAs). In this study, we combined biophysics, genetics and biochemistry approaches to study Arabidopsis mi...
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Veröffentlicht in: | Molecular plant 2018-08, Vol.11 (8), p.1008-1023 |
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Zusammenfassung: | In eukaryotes, the RNase-III Dicer often produces length/sequence microRNA (miRNA) variants, called “isomiRs”, owing to intrinsic structural/sequence determinants of the miRNA precursors (pre-miRNAs). In this study, we combined biophysics, genetics and biochemistry approaches to study Arabidopsis miR168, the key feedback regulator of central plant silencing effector protein ARGONAUTE1 (AGO1). We identified a motif conserved among plant pre-miR168 orthologs, which enables flexible internal base-pairing underlying at least three metastable structural configurations. These configurations promote alternative, accurate Dicer cleavage events generating length and structural isomiR168 variants with distinctive AGO sorting properties and modes of action. Among these isomiR168s, a duplex with a 22-nt guide strand exhibits strikingly preferential affinity for AGO10, the closest AGO1 paralog. The 22-nt miR168-AGO10 complex antagonizes AGO1 accumulation in part via “transitive RNAi”, a silencing-amplification process, to maintain appropriate AGO1 cellular homeostasis. Furthermore, we found that the tombusviral P19 silencing-suppressor protein displays markedly weaker affinity for the 22-nt form among its isomiR168 cargoes, thereby promoting AGO10-directed suppression of AGO1-mediated antiviral silencing. Taken together, these findings indicate that structural flexibility, a previously overlooked property of pre-miRNAs, considerably increases the versatility and regulatory potential of individual MIRNA genes, and that some pathogens might have evolved the capacity or mechanisms to usurp this property.
A double-stranded flexible motif in all eudicot miR168 precursors dynamically alters their secondary structure and predictably changes their processing by Dicer. Ensuing miR168 length isoforms display alternative AGO sorting and modes of action, including induction of transitivity by a 22-nt miR168 variant. Tombusvirus P19 usurps this structural flexibility by facilitating loading of 22-nt miR168 into AGO10, which in turn promotes down-regulation of antiviral AGO1. |
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ISSN: | 1674-2052 1752-9867 |
DOI: | 10.1016/j.molp.2018.05.006 |