Cdc25 and Wee1: analogous opposites?

<p>Abstract</p> <p>Movement through the cell cycle is controlled by the temporally and spatially ordered activation of cyclin-dependent kinases paired with their respective cyclin binding partners. Cell cycle events occur in a stepwise fashion and are monitored by molecular surveil...

Full description

Bibliographic Details
Main Authors: Kornbluth Sally, Perry Jennifer A
Format: Article
Language:English
Published: BMC 2007-05-01
Series:Cell Division
Online Access:http://www.celldiv.com/content/2/1/12
id doaj-f07a3606a73f4ae9af7f7f24ef9e7869
record_format Article
spelling doaj-f07a3606a73f4ae9af7f7f24ef9e78692020-11-24T21:08:43ZengBMCCell Division1747-10282007-05-01211210.1186/1747-1028-2-12Cdc25 and Wee1: analogous opposites?Kornbluth SallyPerry Jennifer A<p>Abstract</p> <p>Movement through the cell cycle is controlled by the temporally and spatially ordered activation of cyclin-dependent kinases paired with their respective cyclin binding partners. Cell cycle events occur in a stepwise fashion and are monitored by molecular surveillance systems to ensure that each cell cycle process is appropriately completed before subsequent events are initiated. Cells prevent entry into mitosis while DNA replication is ongoing, or if DNA is damaged, via checkpoint mechanisms that inhibit the activators and activate the inhibitors of mitosis, Cdc25 and Wee1, respectively. Once DNA replication has been faithfully completed, Cdc2/Cyclin B is swiftly activated for a timely transition from interphase into mitosis. This sharp transition is propagated through both positive and negative feedback loops that impinge upon Cdc25 and Wee1 to ensure that Cdc2/Cyclin B is fully activated. Recent reports from a number of laboratories have revealed a remarkably complex network of kinases and phosphatases that coordinately control Cdc25 and Wee1, thereby precisely regulating the transition into mitosis. Although not all factors that inhibit Cdc25 have been shown to activate Wee1 and vice versa, a number of regulatory modules are clearly shared in common. Thus, studies on either the Cdc25 or Wee1-regulatory arm of the mitotic control pathway should continue to shed light on how both arms are coordinated to smoothly regulate mitotic entry.</p> http://www.celldiv.com/content/2/1/12
collection DOAJ
language English
format Article
sources DOAJ
author Kornbluth Sally
Perry Jennifer A
spellingShingle Kornbluth Sally
Perry Jennifer A
Cdc25 and Wee1: analogous opposites?
Cell Division
author_facet Kornbluth Sally
Perry Jennifer A
author_sort Kornbluth Sally
title Cdc25 and Wee1: analogous opposites?
title_short Cdc25 and Wee1: analogous opposites?
title_full Cdc25 and Wee1: analogous opposites?
title_fullStr Cdc25 and Wee1: analogous opposites?
title_full_unstemmed Cdc25 and Wee1: analogous opposites?
title_sort cdc25 and wee1: analogous opposites?
publisher BMC
series Cell Division
issn 1747-1028
publishDate 2007-05-01
description <p>Abstract</p> <p>Movement through the cell cycle is controlled by the temporally and spatially ordered activation of cyclin-dependent kinases paired with their respective cyclin binding partners. Cell cycle events occur in a stepwise fashion and are monitored by molecular surveillance systems to ensure that each cell cycle process is appropriately completed before subsequent events are initiated. Cells prevent entry into mitosis while DNA replication is ongoing, or if DNA is damaged, via checkpoint mechanisms that inhibit the activators and activate the inhibitors of mitosis, Cdc25 and Wee1, respectively. Once DNA replication has been faithfully completed, Cdc2/Cyclin B is swiftly activated for a timely transition from interphase into mitosis. This sharp transition is propagated through both positive and negative feedback loops that impinge upon Cdc25 and Wee1 to ensure that Cdc2/Cyclin B is fully activated. Recent reports from a number of laboratories have revealed a remarkably complex network of kinases and phosphatases that coordinately control Cdc25 and Wee1, thereby precisely regulating the transition into mitosis. Although not all factors that inhibit Cdc25 have been shown to activate Wee1 and vice versa, a number of regulatory modules are clearly shared in common. Thus, studies on either the Cdc25 or Wee1-regulatory arm of the mitotic control pathway should continue to shed light on how both arms are coordinated to smoothly regulate mitotic entry.</p>
url http://www.celldiv.com/content/2/1/12
work_keys_str_mv AT kornbluthsally cdc25andwee1analogousopposites
AT perryjennifera cdc25andwee1analogousopposites
_version_ 1716759728019734528