AI Article Synopsis

  • GW182 proteins are critical for the function of microRNA-protein complexes, helping to suppress gene expression by linking Argonaute proteins to silencing machinery.
  • The carboxyl-terminal domain of GW182 interacts with the CCR4-NOT complex, which is involved in mRNA degradation and translation inhibition.
  • New findings reveal that a specific amino-terminal region of GW182 can also bind to the CCR4-NOT complex, highlighting the complexity of GW182's interactions and its multiple binding sites.

Article Abstract

GW182 family proteins are a key component of microRNA-protein complex eliciting translational repression and/or degradation of microRNA-targets. The microRNAs in complex with Argonaute proteins bind to target mRNAs, and GW182 proteins are recruited by association with Argonaute proteins. The GW182 protein acts as a scaffold that links the Argonaute protein to silencing machineries including the CCR4-NOT complex which accelerates deadenylation and inhibits translation. The carboxyl-terminal effector domain of GW182 protein, also called the silencing domain, has been shown to bind to the subunits of the CCR4-NOT complex, the CNOT1 and the CNOT9. Here we show that a small region within the amino-terminal Argonaute-binding domain of human GW182/TNRC6A can associate with the CCR4-NOT complex. This region resides between the two Argonaute-binding sites and contains reiterated GW/WG-motifs. Alanine mutation experiments showed that multiple tryptophan residues are required for the association with the CCR4-NOT complex. Furthermore, co-expression and immunoprecipitation assays suggested that the CNOT9 subunit of the CCR4-NOT complex is a possible binding partner of this region. Our work, taken together with previous studies, indicates that the human GW182 protein contains multiple binding interfaces to the CCR4-NOT complex.

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Source
http://dx.doi.org/10.1111/gtc.12974DOI Listing

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