Cell Reports (Nov 2014)

Trim25 Is an RNA-Specific Activator of Lin28a/TuT4-Mediated Uridylation

  • Nila Roy Choudhury,
  • Jakub S. Nowak,
  • Juan Zuo,
  • Juri Rappsilber,
  • Steven H. Spoel,
  • Gracjan Michlewski

DOI
https://doi.org/10.1016/j.celrep.2014.10.017
Journal volume & issue
Vol. 9, no. 4
pp. 1265 – 1272

Abstract

Read online

RNA binding proteins have thousands of cellular RNA targets and often exhibit opposite or passive molecular functions. Lin28a is a conserved RNA binding protein involved in pluripotency and tumorigenesis that was previously shown to trigger TuT4-mediated pre-let-7 uridylation, inhibiting its processing and targeting it for degradation. Surprisingly, despite binding to other pre-microRNAs (pre-miRNAs), only pre-let-7 is efficiently uridylated by TuT4. Thus, we hypothesized the existence of substrate-specific cofactors that stimulate Lin28a-mediated pre-let-7 uridylation or restrict its functionality on non-let-7 pre-miRNAs. Through RNA pull-downs coupled with quantitative mass spectrometry, we identified the E3 ligase Trim25 as an RNA-specific cofactor for Lin28a/TuT4-mediated uridylation. We show that Trim25 binds to the conserved terminal loop (CTL) of pre-let-7 and activates TuT4, allowing for more efficient Lin28a-mediated uridylation. These findings reveal that protein-modifying enzymes, only recently shown to bind RNA, can guide the function of canonical ribonucleoprotein (RNP) complexes in cis, thereby providing an additional level of specificity.