Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells

Little is known about mammalian preRC stoichiometry, the number of preRCs on chromosomes, and how this relates to replicon size and usage. We show here that, on average, each 100-kb of the mammalian genome contains a preRC composed of approximately one ORC hexamer, 4–5 MCM hexamers, and 2 Cdc6. Rela...

Descripción completa

Detalles Bibliográficos
Autores principales: Wong, Philip G., Winter, Sherry L., Zaika, Elena, Cao, Thinh V., Oguz, Umut, Koomen, John M., Hamlin, Joyce L., Alexandrow, Mark G.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2011
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3046982/
https://www.ncbi.nlm.nih.gov/pubmed/21390258
http://dx.doi.org/10.1371/journal.pone.0017533
_version_ 1782199010934652928
author Wong, Philip G.
Winter, Sherry L.
Zaika, Elena
Cao, Thinh V.
Oguz, Umut
Koomen, John M.
Hamlin, Joyce L.
Alexandrow, Mark G.
author_facet Wong, Philip G.
Winter, Sherry L.
Zaika, Elena
Cao, Thinh V.
Oguz, Umut
Koomen, John M.
Hamlin, Joyce L.
Alexandrow, Mark G.
author_sort Wong, Philip G.
collection PubMed
description Little is known about mammalian preRC stoichiometry, the number of preRCs on chromosomes, and how this relates to replicon size and usage. We show here that, on average, each 100-kb of the mammalian genome contains a preRC composed of approximately one ORC hexamer, 4–5 MCM hexamers, and 2 Cdc6. Relative to these subunits, ∼0.35 total molecules of the pre-Initiation Complex factor Cdc45 are present. Thus, based on ORC availability, somatic cells contain ∼70,000 preRCs of this average total stoichiometry, although subunits may not be juxtaposed with each other. Except for ORC, the chromatin-bound complement of preRC subunits is even lower. Cdc45 is present at very low levels relative to the preRC subunits, but is highly stable, and the same limited number of stable Cdc45 molecules are present from the beginning of S-phase to its completion. Efforts to artificially increase Cdc45 levels through ectopic expression block cell growth. However, microinjection of excess purified Cdc45 into S-phase nuclei activates additional replication foci by three-fold, indicating that Cdc45 functions to activate dormant preRCs and is rate-limiting for somatic replicon usage. Paradoxically, although Cdc45 colocalizes in vivo with some MCM sites and is rate-limiting for DNA replication to occur, neither Cdc45 nor MCMs colocalize with active replication sites. Embryonic metazoan chromatin consists of small replicons that are used efficiently via an excess of preRC subunits. In contrast, somatic mammalian cells contain a low density of preRCs, each containing only a few MCMs that compete for limiting amounts of Cdc45. This provides a molecular explanation why, relative to embryonic replicon dynamics, somatic replicons are, on average, larger and origin efficiency tends to be lower. The stable, continuous, and rate-limiting nature of Cdc45 suggests that Cdc45 contributes to the staggering of replicon usage throughout S-phase, and that replicon activation requires reutilization of existing Cdc45 during S-phase.
format Text
id pubmed-3046982
institution National Center for Biotechnology Information
language English
publishDate 2011
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-30469822011-03-09 Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells Wong, Philip G. Winter, Sherry L. Zaika, Elena Cao, Thinh V. Oguz, Umut Koomen, John M. Hamlin, Joyce L. Alexandrow, Mark G. PLoS One Research Article Little is known about mammalian preRC stoichiometry, the number of preRCs on chromosomes, and how this relates to replicon size and usage. We show here that, on average, each 100-kb of the mammalian genome contains a preRC composed of approximately one ORC hexamer, 4–5 MCM hexamers, and 2 Cdc6. Relative to these subunits, ∼0.35 total molecules of the pre-Initiation Complex factor Cdc45 are present. Thus, based on ORC availability, somatic cells contain ∼70,000 preRCs of this average total stoichiometry, although subunits may not be juxtaposed with each other. Except for ORC, the chromatin-bound complement of preRC subunits is even lower. Cdc45 is present at very low levels relative to the preRC subunits, but is highly stable, and the same limited number of stable Cdc45 molecules are present from the beginning of S-phase to its completion. Efforts to artificially increase Cdc45 levels through ectopic expression block cell growth. However, microinjection of excess purified Cdc45 into S-phase nuclei activates additional replication foci by three-fold, indicating that Cdc45 functions to activate dormant preRCs and is rate-limiting for somatic replicon usage. Paradoxically, although Cdc45 colocalizes in vivo with some MCM sites and is rate-limiting for DNA replication to occur, neither Cdc45 nor MCMs colocalize with active replication sites. Embryonic metazoan chromatin consists of small replicons that are used efficiently via an excess of preRC subunits. In contrast, somatic mammalian cells contain a low density of preRCs, each containing only a few MCMs that compete for limiting amounts of Cdc45. This provides a molecular explanation why, relative to embryonic replicon dynamics, somatic replicons are, on average, larger and origin efficiency tends to be lower. The stable, continuous, and rate-limiting nature of Cdc45 suggests that Cdc45 contributes to the staggering of replicon usage throughout S-phase, and that replicon activation requires reutilization of existing Cdc45 during S-phase. Public Library of Science 2011-03-01 /pmc/articles/PMC3046982/ /pubmed/21390258 http://dx.doi.org/10.1371/journal.pone.0017533 Text en Wong et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wong, Philip G.
Winter, Sherry L.
Zaika, Elena
Cao, Thinh V.
Oguz, Umut
Koomen, John M.
Hamlin, Joyce L.
Alexandrow, Mark G.
Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title_full Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title_fullStr Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title_full_unstemmed Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title_short Cdc45 Limits Replicon Usage from a Low Density of preRCs in Mammalian Cells
title_sort cdc45 limits replicon usage from a low density of prercs in mammalian cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3046982/
https://www.ncbi.nlm.nih.gov/pubmed/21390258
http://dx.doi.org/10.1371/journal.pone.0017533
work_keys_str_mv AT wongphilipg cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT wintersherryl cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT zaikaelena cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT caothinhv cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT oguzumut cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT koomenjohnm cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT hamlinjoycel cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells
AT alexandrowmarkg cdc45limitsrepliconusagefromalowdensityofprercsinmammaliancells

Ejemplares similares