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• W2055709849 endingPage "8347" @default.
• W2055709849 startingPage "8331" @default.
• W2055709849 abstract "The CCR4-NOT complex, the major deadenylase in eukaryotes, plays crucial roles in gene expression at the levels of transcription, mRNA decay, and protein degradation. GW182/TNRC6 proteins, which are core components of the microRNA-induced silencing complex in animals, stimulate deadenylation and repress translation via recruitment of the CCR4-NOT complex. Here we report a heterologous experimental system that recapitulates the recruitment of CCR4-NOT complex by TNRC6 in S. cerevisiae. Using this system, we characterize conserved functions of the CCR4-NOT complex. The complex stimulates degradation of mRNA from the 5′ end by Xrn1, in a manner independent of both translation and deadenylation. This degradation pathway is probably conserved in miRNA-mediated gene silencing in zebrafish. Furthermore, the mRNA fate modulators Dhh1 and Pat1 redundantly stimulate mRNA decay, but both factors are required for poly(A) tail-independent translation repression by tethered TNRC6A. Our tethering-based reconstitution system reveals that the conserved architecture of Not1/CNOT1 provides a binding surface for TNRC6, thereby connecting microRNA-induced silencing complex to the decapping machinery as well as the translation apparatus." @default.
• W2055709849 created "2016-06-24" @default.
• W2055709849 creator A5004901799 @default.
• W2055709849 creator A5022850583 @default.
• W2055709849 creator A5052409368 @default.
• W2055709849 creator A5061533640 @default.
• W2055709849 date "2015-03-01" @default.
• W2055709849 modified "2023-10-13" @default.
• W2055709849 title "Roles of mRNA Fate Modulators Dhh1 and Pat1 in TNRC6-dependent Gene Silencing Recapitulated in Yeast" @default.
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• W2055709849 doi "https://doi.org/10.1074/jbc.m114.615088" @default.
• W2055709849 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/4375487" @default.
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• W2055709849 hasPublicationYear "2015" @default.
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