Regulated interaction of ID2 with the anaphase-promoting complex links progression through mitosis with reactivation of cell-type-specific transcription

  • Lee, Sang Bae
  • Garofano, Luciano
  • Ko, Aram
  • D'Angelo, Fulvio
  • Frangaj, Brulinda
  • ... Kim, KyeongJin
  • 외 5명
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초록

Tissue-specific transcriptional activity is silenced in mitotic cells. Here the authors reveal a general phosphorylation-dependent mechanism of recognition for the anaphase-promoting complex (APC) substrates, and show that the APC targets ID2 during the establishment of post-mitotic transcription. Tissue-specific transcriptional activity is silenced in mitotic cells but it remains unclear whether the mitotic regulatory machinery interacts with tissue-specific transcriptional programs. We show that such cross-talk involves the controlled interaction between core subunits of the anaphase-promoting complex (APC) and the ID2 substrate. The N-terminus of ID2 is independently and structurally compatible with a pocket composed of core APC/C subunits that may optimally orient ID2 onto the APC(CDH1) complex. Phosphorylation of serine-5 by CDK1 prevented the association of ID2 with core APC, impaired ubiquitylation and stabilized ID2 protein at the mitosis-G1 transition leading to inhibition of basic Helix-Loop-Helix (bHLH)-mediated transcription. The serine-5 phospho-mimetic mutant of ID2 that inefficiently bound core APC remained stable during mitosis, delayed exit from mitosis and reloading of bHLH transcription factors on chromatin. It also locked cells into a "mitotic stem cell" transcriptional state resembling the pluripotent program of embryonic stem cells. The substrates of APC(CDH1) SKP2 and Cyclin B1 share with ID2 the phosphorylation-dependent, D-box-independent interaction with core APC. These results reveal a new layer of control of the mechanism by which substrates are recognized by APC.

키워드

LOOP-HELIX PROTEINSSTEM-CELLSUBIQUITIN LIGASEHOMEOBOX GENESSELF-RENEWALCENP-ACYCLEPHOSPHORYLATIONDEGRADATIONFAMILY
제목
Regulated interaction of ID2 with the anaphase-promoting complex links progression through mitosis with reactivation of cell-type-specific transcription
저자
Lee, Sang BaeGarofano, LucianoKo, AramD'Angelo, FulvioFrangaj, BrulindaSommer, DanikaGan, QiwenKim, KyeongJinCardozo, TimothyIavarone, AntonioLasorella, Anna
DOI
10.1038/s41467-022-29502-2
발행일
2022-04-19
유형
Article
저널명
Nature Communications
13
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