Molecular architecture and mechanism of the anaphase-promoting complex

被引:0
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作者
Leifu Chang
Ziguo Zhang
Jing Yang
Stephen H. McLaughlin
David Barford
机构
[1] Institute of Cancer Research,Division of Structural Biology
[2] 237 Fulham Road,undefined
[3] London SW3 6JB,undefined
[4] UK,undefined
[5] MRC Laboratory of Molecular Biology,undefined
[6] Cambridge CB2 0QH,undefined
[7] UK,undefined
[8] Present address: MRC Laboratory of Molecular Biology,undefined
[9] Cambridge CB2 0QH,undefined
[10] UK (L.C.,undefined
[11] Z.Z.,undefined
[12] J.Y. and D.B.).,undefined
来源
Nature | 2014年 / 513卷
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摘要
The ubiquitination of cell cycle regulatory proteins by the anaphase-promoting complex/cyclosome (APC/C) controls sister chromatid segregation, cytokinesis and the establishment of the G1 phase of the cell cycle. The APC/C is an unusually large multimeric cullin-RING ligase. Its activity is strictly dependent on regulatory coactivator subunits that promote APC/C–substrate interactions and stimulate its catalytic reaction. Because the structures of many APC/C subunits and their organization within the assembly are unknown, the molecular basis for these processes is poorly understood. Here, from a cryo-electron microscopy reconstruction of a human APC/C–coactivator–substrate complex at 7.4 Å resolution, we have determined the complete secondary structural architecture of the complex. With this information we identified protein folds for structurally uncharacterized subunits, and the definitive location of all 20 APC/C subunits within the 1.2 MDa assembly. Comparison with apo APC/C shows that the coactivator promotes a profound allosteric transition involving displacement of the cullin-RING catalytic subunits relative to the degron-recognition module of coactivator and APC10. This transition is accompanied by increased flexibility of the cullin-RING subunits and enhanced affinity for UBCH10–ubiquitin, changes which may contribute to coactivator-mediated stimulation of APC/C E3 ligase activity.
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页码:388 / 393
页数:5
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