E2-C, a cyclin-selective ubiquitin carrier protein required for the destruction of mitotic cyclins

  1. A Aristarkhov,
  2. E Eytan,
  3. A Moghe,
  4. A Admon,
  5. A Hershko, and
  6. J V Ruderman
  1. Department of Cell Biology, Harvard Medical School, Boston, MA 02115, USA.

Abstract

Ubiquitin-dependent proteolysis of the mitotic cyclins A and B is required for the completion of mitosis and entry into the next cell cycle. This process is catalyzed by the cyclosome, an approximately 22S particle that contains a cyclin-selective ubiquitin ligase activity, E3-C, that requires a cyclin-selective ubiquitin carrier protein (UBC) E2-C. Here we report the purification and cloning of E2-C from clam oocytes. The deduced amino acid sequence of E2-C indicates that it is a new UBC family member. Bacterially expressed recombinant E2-C is active in in vitro cyclin ubiquitination assays, where it exhibits the same substrate specificities seen with native E2-C. These results demonstrate that E2-C is not a homolog of UBC4 or UBC9, proteins previously suggested to be involved in cyclin ubiquitination, but is a new UBC family member with unique properties.

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  1. PNAS April 30, 1996 vol. 93 no. 9 4294-4299
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