Tob2 phosphorylation regulates global mRNA turnover to reshape transcriptome and impact cell proliferation

Chyi Ying A. Chen, Krista Strouz, Kai Lieh Huang, Ann Bin Shyu

Research output: Contribution to journalArticlepeer-review

1 Scopus citations

Abstract

Tob2, an anti-proliferative protein, promotes deadenylation through recruiting Caf1 deadenylase to the mRNA poly(A) tail by simultaneously interacting with both Caf1 and poly(A)-binding protein (PABP). Previously,wefound that changes in Tob2 phosphorylation can alter its PABP-binding ability and deadenylation-promoting function. However, it remained unknown regarding the relevant kinase(s). Moreover, it was unclear whether Tob2 phosphorylation modulates the transcriptome and whether the phosphorylation is linked to Tob2's anti-proliferative function. In this study,wefound that c-Jun amino-terminal kinase (JNK) increases phosphorylation of Tob2 at many Ser/Thr sites in the intrinsically disordered region (IDR) that contains two separate PABP-interacting PAM2 motifs. JNK-induced phosphorylation or phosphomimetic mutations at these sitesweaken the Tob2-PABPinteraction. In contrast, JNK-independent phosphorylation of Tob2 at serine 254 (S254) greatly enhances Tob2 interaction with PABP and its ability to promote deadenylation.We discovered that both PAM2motifs are required for Tob2 to display these features. Combining mass spectrometry analysis, poly(A) size-distribution profiling, transcriptome-widemRNAturnover analyses, and cell proliferation assays,wefound that the phosphomimetic mutation at S254 (S254D) enhances Tob2's association with PABP, leading to accelerated deadenylation and decay of mRNAs globally. Moreover, the Tob2-S254D mutant accelerates the decay of many transcripts coding for cell cycle related proteins and enhances anti-proliferation function. Our findings reveal a novel mechanism by which Ccr4-Not complex is recruited by Tob2 to themRNA3' poly(A)-PABP complex in a phosphorylation dependent manner to promote rapid deadenylation and decay across the transcriptome, eliciting transcriptome reprogramming and suppressed cell proliferation.

Original languageEnglish (US)
Pages (from-to)1143-1159
Number of pages17
JournalRNA
Volume26
Issue number9
DOIs
StatePublished - Sep 2020

Keywords

  • Ccr4-Not complex
  • Deadenylation
  • PABP interaction
  • Phosphorylation
  • Transcriptome programming
  • mRNA turnover

ASJC Scopus subject areas

  • Molecular Biology

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