Binding of NUFIP2 to Roquin promotes recognition and regulation of ICOS mRNA

  • Nina Rehage
  • , Elena Davydova
  • , Christine Conrad
  • , Gesine Behrens
  • , Andreas Maiser
  • , Jenny E. Stehklein
  • , Sven Brenner
  • , Juliane Klein
  • , Aicha Jeridi
  • , Anne Hoffmann
  • , Eunhae Lee
  • , Umberto Dianzani
  • , Rob Willemsen
  • , Regina Feederle
  • , Kristin Reiche
  • , Jörg Hackermüller
  • , Heinrich Leonhardt
  • , Sonia Sharma
  • , Dierk Niessing
  • , Vigo Heissmeyer

Risultato della ricerca: Contributo su rivistaArticolo in rivistapeer review

Abstract

The ubiquitously expressed RNA-binding proteins Roquin-1 and Roquin-2 are essential for appropriate immune cell function and postnatal survival of mice. Roquin proteins repress target mRNAs by recognizing secondary structures in their 3′-UTRs and by inducing mRNA decay. However, it is unknown if other cellular proteins contribute to target control. To identify cofactors of Roquin, we used RNA interference to screen ~1500 genes involved in RNA-binding or mRNA degradation, and identified NUFIP2 as a cofactor of Roquin-induced mRNA decay. NUFIP2 binds directly and with high affinity to Roquin, which stabilizes NUFIP2 in cells. Post-transcriptional repression of human ICOS by endogenous Roquin proteins requires two neighboring non-canonical stem-loops in the ICOS 3′-UTR. This unconventional cis-element as well as another tandem loop known to confer Roquin-mediated regulation of the Ox40 3′-UTR, are bound cooperatively by Roquin and NUFIP2. NUFIP2 therefore emerges as a cofactor that contributes to mRNA target recognition by Roquin.

Lingua originaleInglese
Numero di articolo299
RivistaNature Communications
Volume9
Numero di pubblicazione1
DOI
Stato di pubblicazionePubblicato - 1 dic 2018

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