Cdc48p is required for the cell cycle commitment point at Start via degradation of the G1-CDK inhibitor Far1p

Xinrong Fu; Christine Ng; Daorong Feng; Chun Liang

doi:10.1083/jcb.200307025

Cdc48p is required for the cell cycle commitment point at Start via degradation of the G1-CDK inhibitor Far1p

Xinrong Fu, Christine Ng, Daorong Feng, Chun Liang

Research output: Contribution to journal › Article › peer-review

67 Scopus citations

Abstract

The budding yeast Cdc48p and its mammalian homologue p97 are involved in many important cellular activities. Because previous cdc48 mutants have exclusive G2/M arrest, Cdc48p was thought to play an essential role only during mitosis. We found that Cdc48p is required for the execution of Start (a yeast cell cycle commitment point equivalent to the restriction point in mammalian cells) in both a normal mitotic cell cycle and cell cycle reentry after mating pheromone withdrawal through degradation of the G1-cyclin-dependent kinase inhibitor Far1p. Our work is the first to uncover novel roles of Cdc48p as a critical cell cycle regulator in G1, and to shed new light on cell cycle regulation of Far1p, which is the first cyclin-dependent kinase inhibitor shown to be a substrate of an essential proteolysis event mediated by Cdc48p.

Original language	English (US)
Pages (from-to)	21-26
Number of pages	6
Journal	Journal of Cell Biology
Volume	163
Issue number	1
DOIs	https://doi.org/10.1083/jcb.200307025
State	Published - Oct 13 2003
Externally published	Yes

Keywords

CDK
CDK inhibitor
P97
Ubiquitin-proteosome proteolysis
VCP

ASJC Scopus subject areas

Cell Biology

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10.1083/jcb.200307025

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title = "Cdc48p is required for the cell cycle commitment point at Start via degradation of the G1-CDK inhibitor Far1p",

abstract = "The budding yeast Cdc48p and its mammalian homologue p97 are involved in many important cellular activities. Because previous cdc48 mutants have exclusive G2/M arrest, Cdc48p was thought to play an essential role only during mitosis. We found that Cdc48p is required for the execution of Start (a yeast cell cycle commitment point equivalent to the restriction point in mammalian cells) in both a normal mitotic cell cycle and cell cycle reentry after mating pheromone withdrawal through degradation of the G1-cyclin-dependent kinase inhibitor Far1p. Our work is the first to uncover novel roles of Cdc48p as a critical cell cycle regulator in G1, and to shed new light on cell cycle regulation of Far1p, which is the first cyclin-dependent kinase inhibitor shown to be a substrate of an essential proteolysis event mediated by Cdc48p.",

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author = "Xinrong Fu and Christine Ng and Daorong Feng and Chun Liang",

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doi = "10.1083/jcb.200307025",

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T1 - Cdc48p is required for the cell cycle commitment point at Start via degradation of the G1-CDK inhibitor Far1p

AU - Fu, Xinrong

AU - Ng, Christine

AU - Feng, Daorong

AU - Liang, Chun

PY - 2003/10/13

Y1 - 2003/10/13

N2 - The budding yeast Cdc48p and its mammalian homologue p97 are involved in many important cellular activities. Because previous cdc48 mutants have exclusive G2/M arrest, Cdc48p was thought to play an essential role only during mitosis. We found that Cdc48p is required for the execution of Start (a yeast cell cycle commitment point equivalent to the restriction point in mammalian cells) in both a normal mitotic cell cycle and cell cycle reentry after mating pheromone withdrawal through degradation of the G1-cyclin-dependent kinase inhibitor Far1p. Our work is the first to uncover novel roles of Cdc48p as a critical cell cycle regulator in G1, and to shed new light on cell cycle regulation of Far1p, which is the first cyclin-dependent kinase inhibitor shown to be a substrate of an essential proteolysis event mediated by Cdc48p.

AB - The budding yeast Cdc48p and its mammalian homologue p97 are involved in many important cellular activities. Because previous cdc48 mutants have exclusive G2/M arrest, Cdc48p was thought to play an essential role only during mitosis. We found that Cdc48p is required for the execution of Start (a yeast cell cycle commitment point equivalent to the restriction point in mammalian cells) in both a normal mitotic cell cycle and cell cycle reentry after mating pheromone withdrawal through degradation of the G1-cyclin-dependent kinase inhibitor Far1p. Our work is the first to uncover novel roles of Cdc48p as a critical cell cycle regulator in G1, and to shed new light on cell cycle regulation of Far1p, which is the first cyclin-dependent kinase inhibitor shown to be a substrate of an essential proteolysis event mediated by Cdc48p.

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KW - P97

KW - Ubiquitin-proteosome proteolysis

KW - VCP

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Cdc48p is required for the cell cycle commitment point at Start via degradation of the G1-CDK inhibitor Far1p

Abstract

Keywords

ASJC Scopus subject areas

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