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Examining the mechanistic relationship of <scp>APC</scp>/<scp>C<sup>CDH1</sup></scp> and its interphase inhibitor <scp>EMI1</scp>

Derek L. Bolhuis, Raquel C. Martinez‐Chacin, Kaeli A. Welsh, Tatyana Bodrug, Liying Cui, Michael J. Emanuele, Nicholas G. Brown

2022Protein Science33 citationsDOIOpen Access PDF

Abstract

Proper protein destruction by the ubiquitin (Ub)-proteasome system is vital for a faithful cell cycle. Hence, the activity of Ub ligases is tightly controlled. The Anaphase-Promoting Complex/Cyclosome (APC/C) is a 1.2 MDa Ub ligase responsible for mitotic progression and G1 maintenance. At the G1/S transition, the APC/C is inhibited by EMI1 to prevent APC/C-dependent polyubiquitination of cell cycle effectors. EMI1 uses several interaction motifs to block the recruitment of APC/C substrates as well as the APC/C-associated E2s, UBE2C, and UBE2S. Paradoxically, EMI1 is also an APC/C substrate during G1. Using a comprehensive set of enzyme assays, we determined the context-dependent involvement of the EMI1 motifs in APC/C-dependent ubiquitination of EMI1 and other substrates. Furthermore, we demonstrated that an isolated C-terminal peptide fragment of EMI1 activates APC/C-dependent substrate priming by UBE2C. Together, these findings reveal the multiple roles of the EMI1 C-terminus for G1 maintenance and the G1/S transition.

Topics & Concepts

Cell division control protein 4Cell biologyUbiquitin ligaseChemistryCell cycleAnaphase-promoting complexUbiquitinMitosisBiochemistryBiologyCellGeneUbiquitin and proteasome pathwaysMicrotubule and mitosis dynamicsProtein Degradation and Inhibitors