Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator

BACKGROUND: Depletion of replication factors often causes cell death in cancer cells. Depletion of Cdc7, a kinase essential for initiation of DNA replication, induces cancer cell death regardless of its p53 status, but the precise pathways of cell death induction have not been characterized. METHODO...

Descripción completa

Detalles Bibliográficos
Autores principales: Ito, Sayuri, Ishii, Ai, Kakusho, Naoko, Taniyama, Chika, Yamazaki, Satoshi, Fukatsu, Rino, Sakaue-Sawano, Asako, Miyawaki, Atsushi, Masai, Hisao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3344859/
https://www.ncbi.nlm.nih.gov/pubmed/22574151
http://dx.doi.org/10.1371/journal.pone.0036372
_version_ 1782232086530228224
author Ito, Sayuri
Ishii, Ai
Kakusho, Naoko
Taniyama, Chika
Yamazaki, Satoshi
Fukatsu, Rino
Sakaue-Sawano, Asako
Miyawaki, Atsushi
Masai, Hisao
author_facet Ito, Sayuri
Ishii, Ai
Kakusho, Naoko
Taniyama, Chika
Yamazaki, Satoshi
Fukatsu, Rino
Sakaue-Sawano, Asako
Miyawaki, Atsushi
Masai, Hisao
author_sort Ito, Sayuri
collection PubMed
description BACKGROUND: Depletion of replication factors often causes cell death in cancer cells. Depletion of Cdc7, a kinase essential for initiation of DNA replication, induces cancer cell death regardless of its p53 status, but the precise pathways of cell death induction have not been characterized. METHODOLOGY/PRINCIPAL FINDINGS: We have used the recently-developed cell cycle indicator, Fucci, to precisely characterize the cell death process induced by Cdc7 depletion. We have also generated and utilized similar fluorescent cell cycle indicators using fusion with other cell cycle regulators to analyze modes of cell death in live cells in both p53-positive and -negative backgrounds. We show that distinct cell-cycle responses are induced in p53-positive and -negative cells by Cdc7 depletion. p53-negative cells predominantly arrest temporally in G2-phase, accumulating CyclinB1 and other mitotic regulators. Prolonged arrest at G2-phase and abrupt entry into aberrant M-phase in the presence of accumulated CyclinB1 are followed by cell death at the post-mitotic state. Abrogation of cytoplasmic CyclinB1 accumulation partially decreases cell death. The ATR-MK2 pathway is responsible for sequestration of CyclinB1 with 14-3-3σ protein. In contrast, p53-positive cancer cells do not accumulate CyclinB1, but appear to die mostly through entry into aberrant S-phase after Cdc7 depletion. The combination of Cdc7 inhibition with known anti-cancer agents significantly stimulates cell death effects in cancer cells in a genotype-dependent manner, providing a strategic basis for future combination therapies. CONCLUSIONS: Our results show that the use of Fucci, and similar fluorescent cell cycle indicators, offers a convenient assay system with which to identify cell cycle events associated with cancer cell death. They also indicate genotype-specific cell death modes induced by deficient initiation of DNA replication in cancer cells and its potential exploitation for development of efficient cancer therapies.
format Online
Article
Text
id pubmed-3344859
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-33448592012-05-09 Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator Ito, Sayuri Ishii, Ai Kakusho, Naoko Taniyama, Chika Yamazaki, Satoshi Fukatsu, Rino Sakaue-Sawano, Asako Miyawaki, Atsushi Masai, Hisao PLoS One Research Article BACKGROUND: Depletion of replication factors often causes cell death in cancer cells. Depletion of Cdc7, a kinase essential for initiation of DNA replication, induces cancer cell death regardless of its p53 status, but the precise pathways of cell death induction have not been characterized. METHODOLOGY/PRINCIPAL FINDINGS: We have used the recently-developed cell cycle indicator, Fucci, to precisely characterize the cell death process induced by Cdc7 depletion. We have also generated and utilized similar fluorescent cell cycle indicators using fusion with other cell cycle regulators to analyze modes of cell death in live cells in both p53-positive and -negative backgrounds. We show that distinct cell-cycle responses are induced in p53-positive and -negative cells by Cdc7 depletion. p53-negative cells predominantly arrest temporally in G2-phase, accumulating CyclinB1 and other mitotic regulators. Prolonged arrest at G2-phase and abrupt entry into aberrant M-phase in the presence of accumulated CyclinB1 are followed by cell death at the post-mitotic state. Abrogation of cytoplasmic CyclinB1 accumulation partially decreases cell death. The ATR-MK2 pathway is responsible for sequestration of CyclinB1 with 14-3-3σ protein. In contrast, p53-positive cancer cells do not accumulate CyclinB1, but appear to die mostly through entry into aberrant S-phase after Cdc7 depletion. The combination of Cdc7 inhibition with known anti-cancer agents significantly stimulates cell death effects in cancer cells in a genotype-dependent manner, providing a strategic basis for future combination therapies. CONCLUSIONS: Our results show that the use of Fucci, and similar fluorescent cell cycle indicators, offers a convenient assay system with which to identify cell cycle events associated with cancer cell death. They also indicate genotype-specific cell death modes induced by deficient initiation of DNA replication in cancer cells and its potential exploitation for development of efficient cancer therapies. Public Library of Science 2012-05-04 /pmc/articles/PMC3344859/ /pubmed/22574151 http://dx.doi.org/10.1371/journal.pone.0036372 Text en Ito 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
Ito, Sayuri
Ishii, Ai
Kakusho, Naoko
Taniyama, Chika
Yamazaki, Satoshi
Fukatsu, Rino
Sakaue-Sawano, Asako
Miyawaki, Atsushi
Masai, Hisao
Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title_full Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title_fullStr Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title_full_unstemmed Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title_short Mechanism of Cancer Cell Death Induced by Depletion of an Essential Replication Regulator
title_sort mechanism of cancer cell death induced by depletion of an essential replication regulator
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3344859/
https://www.ncbi.nlm.nih.gov/pubmed/22574151
http://dx.doi.org/10.1371/journal.pone.0036372
work_keys_str_mv AT itosayuri mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT ishiiai mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT kakushonaoko mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT taniyamachika mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT yamazakisatoshi mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT fukatsurino mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT sakauesawanoasako mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT miyawakiatsushi mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator
AT masaihisao mechanismofcancercelldeathinducedbydepletionofanessentialreplicationregulator

Ejemplares similares