nonredundant requirement for multiple histone modifications for the early anaphase release of the mitotic exit regulator cdc14 from nucleolar chromatinnonredundant要求多个组蛋白修饰的早期的后期有丝分裂退出监管机构cdc14核仁的染色质.pdfVIP
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nonredundant requirement for multiple histone modifications for the early anaphase release of the mitotic exit regulator cdc14 from nucleolar chromatinnonredundant要求多个组蛋白修饰的早期的后期有丝分裂退出监管机构cdc14核仁的染色质
Nonredundant Requirement for Multiple Histone
Modifications for the Early Anaphase Release of the
Mitotic Exit Regulator Cdc14 from Nucleolar Chromatin
William W. Hwang, Hiten D. Madhani*
Department of Biochemistry and Biophysics, University of California San Francisco, San Francisco, California, United States of America
Abstract
In Saccharomyces cerevisiae, the conserved phosphatase Cdc14 is required for the exit from mitosis. It is anchored on
nucleolar chromatin by the Cfi1/Net1 protein until early anaphase, at which time it is released into the nucleoplasm. Two
poorly understood, redundant pathways promote Cdc14 release, the FEAR (Cdc fourteen early release) network and the
MEN (mitotic exit network). Through the analysis of genetic interactions, we report here a novel requirement for the
ubiquitination of histone H2B by the Bre1 ubiquitin ligase in the cell cycle–dependent release of Cdc14 from nucleolar
chromatin when the MEN is inactivated. This function for H2B ubiquitination is mediated by its activation of histone H3
methylation on lysines 4 and 79 (meH3K4 and meH3K79) but, surprisingly, is not dependent on the histone deacetylase
(HDAC) Sir2, which associates with Cdc14 on nucleolar chromatin as part of the RENT complex. We also observed a defect in
Cdc14 release in cells lacking H3 lysine 36 methylation (meH3K36) and in cells lacking an HDAC recruited by this
modification. These histone modifications represent previously unappreciated factors required for the accessibility to and/or
action on nucleolar chromatin of FEAR network components. The nonredundant role for these modifications in this context
contrasts with the notion of a highly combinatorial code by which histone marks act to control biological processes.
Citation: Hwang WW, Madhani HD (2009) Nonredundant Requiremen
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