XB-ART-45067
Nat Cell Biol
2012 Jan 29;142:168-76. doi: 10.1038/ncb2425.
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APC/C-mediated multiple monoubiquitylation provides an alternative degradation signal for cyclin B1.
Dimova NV
,
Hathaway NA
,
Lee BH
,
Kirkpatrick DS
,
Berkowitz ML
,
Gygi SP
,
Finley D
,
King RW
.
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The anaphase-promoting complex or cyclosome (APC/C) initiates mitotic exit by ubiquitylating cell-cycle regulators such as cyclin B1 and securin. Lys 48-linked ubiquitin chains represent the canonical signal targeting proteins for degradation by the proteasome, but they are not required for the degradation of cyclin B1. Lys 11-linked ubiquitin chains have been implicated in degradation of APC/C substrates, but the Lys 11-chain-forming E2 UBE2S is not essential for mitotic exit, raising questions about the nature of the ubiquitin signal that targets APC/C substrates for degradation. Here we demonstrate that multiple monoubiquitylation of cyclin B1, catalysed by UBCH10 or UBC4/5, is sufficient to target cyclin B1 for destruction by the proteasome. When the number of ubiquitylatable lysines in cyclin B1 is restricted, Lys 11-linked ubiquitin polymers elaborated by UBE2S become increasingly important. We therefore explain how a substrate that contains multiple ubiquitin acceptor sites confers flexibility in the requirement for particular E2 enzymes in modulating the rate of ubiquitin-dependent proteolysis.
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???displayArticle.grants??? [+]
GM095526 NIGMS NIH HHS , GM66492 NIGMS NIH HHS , R37 GM043601-22 NIGMS NIH HHS , R01 GM066492-07 NIGMS NIH HHS , R01 GM066492-07S1 NIGMS NIH HHS , R01 GM066492-08 NIGMS NIH HHS , R01 GM066492-09 NIGMS NIH HHS , R56 GM066492-06 NIGMS NIH HHS , R01 GM095526 NIGMS NIH HHS , R01 GM066492 NIGMS NIH HHS , R37 GM043601 NIGMS NIH HHS , R56 GM066492 NIGMS NIH HHS
Species referenced: Xenopus
Genes referenced: ccnb1 cdk1 psmd4 rrad ube2d1 ube2s usp14
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