Article abstract
Nature Structural & Molecular Biology 14, 941 - 948 (2007)
Published online: 16 September 2007 | doi:10.1038/nsmb1295
E2–BRCA1 RING interactions dictate synthesis of mono- or specific polyubiquitin chain linkages
Devin E Christensen1, Peter S Brzovic1 & Rachel E Klevit1
Abstract
An E3 ubiquitin ligase mediates the transfer of activated ubiquitin from an E2 ubiquitin-conjugating enzyme to its substrate lysine residues. Using a structure-based, yeast two-hybrid strategy, we discovered six previously unidentified interactions between the human heterodimeric RING E3 BRCA1-BARD1 and the human E2s UbcH6, Ube2e2, UbcM2, Ubc13, Ube2k and Ube2w. All six E2s bind directly to the BRCA1 RING motif and are active with BRCA1-BARD1 for autoubiquitination in vitro. Four of the E2s direct monoubiquitination of BRCA1. Ubc13-Mms2 and Ube2k direct the synthesis of Lys63- or Lys48-linked ubiquitin chains on BRCA1 and require an acceptor ubiquitin attached to BRCA1. Differences between the mono- and polyubiquitination activities of the BRCA1-interacting E2s correlate with their ability to bind ubiquitin noncovalently at a site distal to the active site. Thus, BRCA1 has the ability to direct the synthesis of specific polyubiquitin chain linkages, depending on the E2 bound to its RING.
- Department of Biochemistry, University of Washington, Box 357350, Seattle, Washington 98195-7350, USA.
Correspondence to: Rachel E Klevit1 e-mail: klevit@u.washington.edu
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