The Crystal Structure of the NHL Domain in Complex with RNA Reveals the Molecular Basis of Drosophila Brain-Tumor-Mediated Gene Regulation.

نویسندگان

  • Inga Loedige
  • Leonhard Jakob
  • Thomas Treiber
  • Debashish Ray
  • Mathias Stotz
  • Nora Treiber
  • Janosch Hennig
  • Kate B Cook
  • Quaid Morris
  • Timothy R Hughes
  • Julia C Engelmann
  • Michael P Krahn
  • Gunter Meister
چکیده

TRIM-NHL proteins are conserved among metazoans and control cell fate decisions in various stem cell linages. The Drosophila TRIM-NHL protein Brain tumor (Brat) directs differentiation of neuronal stem cells by suppressing self-renewal factors. Brat is an RNA-binding protein and functions as a translational repressor. However, it is unknown which RNAs Brat regulates and how RNA-binding specificity is achieved. Using RNA immunoprecipitation and RNAcompete, we identify Brat-bound mRNAs in Drosophila embryos and define consensus binding motifs for Brat as well as a number of additional TRIM-NHL proteins, indicating that TRIM-NHL proteins are conserved, sequence-specific RNA-binding proteins. We demonstrate that Brat-mediated repression and direct RNA-binding depend on the identified motif and show that binding of the localization factor Miranda to the Brat-NHL domain inhibits Brat activity. Finally, to unravel the sequence specificity of the NHL domain, we crystallize the Brat-NHL domain in complex with RNA and present a high-resolution protein-RNA structure of this fold.

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عنوان ژورنال:
  • Cell reports

دوره 13 6  شماره 

صفحات  -

تاریخ انتشار 2015