Department of Cell Biology, Harvard Medical School, Boston, MA, USA.
Department of Biochemistry and Biophysics, University of North Carolina School of Medicine, Chapel Hill, NC, USA.
Nat Chem Biol. 2020 May;16(5):546-555. doi: 10.1038/s41589-020-0495-z. Epub 2020 Mar 9.
The anaphase-promoting complex/cyclosome (APC/C) is a ubiquitin ligase that initiates anaphase and mitotic exit. APC/C is activated by Cdc20 and inhibited by the mitotic checkpoint complex (MCC), which delays mitotic exit when the spindle assembly checkpoint (SAC) is activated. We previously identified apcin as a small molecule ligand of Cdc20 that inhibits APC/C and prolongs mitosis. Here we find that apcin paradoxically shortens mitosis when SAC activity is high. These opposing effects of apcin arise from targeting of a common binding site in Cdc20 required for both substrate ubiquitination and MCC-dependent APC/C inhibition. Furthermore, we found that apcin cooperates with p31 to relieve MCC-dependent inhibition of APC/C. Apcin therefore causes either net APC/C inhibition, prolonging mitosis when SAC activity is low, or net APC/C activation, shortening mitosis when SAC activity is high, demonstrating that a small molecule can produce opposing biological effects depending on regulatory context.
后期促进复合物/环体(APC/C)是一种泛素连接酶,可引发后期和有丝分裂退出。APC/C 由 Cdc20 激活,由有丝分裂检查点复合物(MCC)抑制,当纺锤体组装检查点(SAC)被激活时,MCC 延迟有丝分裂退出。我们之前发现 apcin 是 Cdc20 的小分子配体,可抑制 APC/C 并延长有丝分裂。在这里,我们发现当 SAC 活性高时,apcin 反常地缩短了有丝分裂。apcin 的这些相反作用源于针对 Cdc20 中一个共同结合位点的靶向,该位点对于底物泛素化和 MCC 依赖性 APC/C 抑制都是必需的。此外,我们发现 apcin 与 p31 合作,解除 MCC 依赖性 APC/C 抑制。因此,apcin 导致 APC/C 的净抑制,当 SAC 活性低时延长有丝分裂,或净 APC/C 激活,当 SAC 活性高时缩短有丝分裂,表明小分子可以根据调节背景产生相反的生物学效应。
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