Literature DB >> 19451546

A single RNA-dependent RNA polymerase assembles with mutually exclusive nucleotidyl transferase subunits to direct different pathways of small RNA biogenesis.

Suzanne Rebecca Lee1, Kristin Benjamin Talsky, Kathleen Collins.   

Abstract

Members of the conserved family of eukaryotic RNA-dependent RNA polymerases (Rdrs) synthesize double-stranded RNA (dsRNA) intermediates in diverse pathways of small RNA (sRNA) biogenesis and RNA-mediated silencing. Rdr-dependent pathways of sRNA production are poorly characterized relative to Rdr-independent pathways, and the Rdr enzymes themselves are poorly characterized relative to their viral RNA-dependent RNA polymerase counterparts. We previously described a physical and functional coupling of the Tetrahymena thermophila Rdr, Rdr1, and a Dicer enzyme, Dcr2, in the production of approximately 24-nucleotide (nt) sRNA in vitro. Here we characterize the endogenous complexes that harbor Rdr1, termed RDRCs. Distinct RDRCs assemble to contain Rdr1 and subsets of the total of four tightly Rdr1-associated proteins. Of particular interest are two RDRC subunits, Rdn1 and Rdn2, which possess noncanonical ribonucleotidyl transferase motifs. We show that the two Rdn proteins are uridine-specific polymerases of separate RDRCs. Two additional RDRC subunits, Rdf1 and Rdf2, are present only in RDRCs containing Rdn1. Rdr1 catalytic activity is retained in RDRCs purified from cell extracts lacking any of the nonessential RDRC subunits (Rdn2, Rdf1, Rdf2) or if the RDRC harbors a catalytically inactive Rdn. However, specific disruption of each RDRC imposes distinct loss-of-function consequences at the cellular level and has a differential impact on the accumulation of specific 23-24-nt sRNA sequences in vivo. The biochemical and biological phenotypes of RDRC subunit disruption reveal a previously unanticipated complexity of Rdr-dependent sRNA biogenesis in vivo.

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Year:  2009        PMID: 19451546      PMCID: PMC2704071          DOI: 10.1261/rna.1630309

Source DB:  PubMed          Journal:  RNA        ISSN: 1355-8382            Impact factor:   4.942


  41 in total

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3.  A member of the polymerase beta nucleotidyltransferase superfamily is required for RNA interference in C. elegans.

Authors:  Chun-Chieh G Chen; Martin J Simard; Hiroaki Tabara; Daniel R Brownell; Jennifer A McCollough; Craig C Mello
Journal:  Curr Biol       Date:  2005-02-22       Impact factor: 10.834

4.  Transcription and RNAi in heterochromatic gene silencing.

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Authors:  Kazufumi Mochizuki; Martin A Gorovsky
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8.  A beta-tubulin mutation selectively uncouples nuclear division and cytokinesis in Tetrahymena thermophila.

Authors:  Joshua J Smith; J Sebastian Yakisich; Geoffrey M Kapler; Eric S Cole; Daniel P Romero
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  15 in total

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Review 3.  New perspectives on the diversification of the RNA interference system: insights from comparative genomics and small RNA sequencing.

Authors:  Alexander Maxwell Burroughs; Yoshinari Ando; L Aravind
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4.  Strand-asymmetric endogenous Tetrahymena small RNA production requires a previously uncharacterized uridylyltransferase protein partner.

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6.  Sequence, biogenesis, and function of diverse small RNA classes bound to the Piwi family proteins of Tetrahymena thermophila.

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7.  Efficient transient protein expression in tomato cultivars and wild species using agroinfiltration-mediated high expression system.

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8.  A ribonuclease coordinates siRNA amplification and mRNA cleavage during RNAi.

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9.  Dicer-independent primal RNAs trigger RNAi and heterochromatin formation.

Authors:  Mario Halic; Danesh Moazed
Journal:  Cell       Date:  2010-02-19       Impact factor: 41.582

10.  Small-RNA-Mediated Genome-wide trans-Recognition Network in Tetrahymena DNA Elimination.

Authors:  Tomoko Noto; Kensuke Kataoka; Jan H Suhren; Azusa Hayashi; Katrina J Woolcock; Martin A Gorovsky; Kazufumi Mochizuki
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