BRCA1 ubiquitinates its phosphorylation-dependent binding partner CtIP

  1. Xiaochun Yu1,3,
  2. Shuang Fu2,3,
  3. Maoyi Lai1,
  4. Richard Baer2,5, and
  5. Junjie Chen1,4
  1. 1 Department of Oncology, Mayo Clinic and Foundation, Rochester, Minnesota 55905, USA;
  2. 2 Institute for Cancer Genetics, Department of Pathology, Columbia University, New York, New York 10032, USA
  1. 3

    3 These authors contributed equally to this work.

Abstract

BRCA1 (Breast Cancer Susceptibility Gene 1) possesses an N-terminal Ring domain and tandem C-terminal BRCT motifs. While the Ring domain has E3 ubiquitin ligase activity, the BRCA1 BRCT domains specifically recognize phospho-serine motifs. Here, we demonstrate that BRCA1 Ring domain catalyzes CtIP ubiquitination in a manner that depends on a phosphorylation-mediated interaction between CtIP and BRCA1 BRCT domains. The BRCA1-dependent ubiquitination of CtIP does not target CtIP for degradation. Instead, ubiquitinated CtIP associates with chromatin following DNA damage and participates in G2/M checkpoint control. Thus, we propose that BRCA1 can regulate the functions of its substrates through nonproteasomal pathways that do not involve substrate degradation.

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  1. doi: 10.1101/gad.1431006 Genes & Dev. 20: 1721-1726 Copyright © 2006, Cold Spring Harbor Laboratory Press

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