Article

 

The nuclear interactome of DYRK1A reveals a functional role in DNA damage repair Pubblico Deposited

Contenuto scaricabile

Scarica il pdf
https://scholar.colorado.edu/concern/articles/n583xv98f
Abstract
  • The chromosome 21 encoded protein kinase DYRK1A is essential for normal human development. Mutations in DYRK1A underlie a spectrum of human developmental disorders, and increased dosage in trisomy 21 is implicated in Down syndrome related pathologies. DYRK1A regulates a diverse array of cellular processes through physical interactions with substrates and binding partners in various subcellular compartments. Despite recent large-scale protein-protein interaction profiling efforts, DYRK1A interactions specific to different subcellular compartments remain largely unknown, impeding progress toward understanding emerging roles for this kinase. Here, we used immunoaffinity purification and quantitative mass spectrometry to identify nuclear interaction partners of endogenous DYRK1A. This interactome was enriched in DNA damage repair factors, transcriptional elongation factors and E3 ubiquitin ligases. We validated an interaction with RNF169, a factor that promotes homology directed repair upon DNA damage, and found that DYRK1A expression and kinase activity are required for maintenance of 53BP1 expression and subsequent recruitment to DNA damage loci. Further, DYRK1A knock out conferred resistance to ionizing radiation in colony formation assays, suggesting that DYRK1A expression decreases cell survival efficiency in response to DNA damage and points to a tumor suppressive role for this kinase.

Creator
Academic Affiliation
Journal Title
Journal Issue/Number
  • 1
Journal Volume
  • 9
Ultima modifica
  • 2020-07-01
Resource Type
Dichiarazione dei diritti
DOI
ISSN
  • 2045-2322
Language
License

Le relazioni

Elementi