Emergence of Micronuclei and Their Effects on the Fate of Cells under Replication Stress
PLoS ONE Volume 5 Issue 4
Page e10089-1-e10089-12
published_at 2010
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Title ( eng ) |
Emergence of Micronuclei and Their Effects on the Fate of Cells under Replication Stress
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Creator |
Utani Koh-ichi
Kohno Yuka
Okamoto Atsushi
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Source Title |
PLoS ONE
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Volume | 5 |
Issue | 4 |
Start Page | e10089-1 |
End Page | e10089-12 |
Abstract |
The presence of micronuclei in mammalian cells is related to several mutagenetic stresses. In order to understand how micronuclei emerge, behave in cells, and affect cell fate, we performed extensive time-lapse microscopy of HeLa H2B-GFP cells in the presence of hydroxyurea at low concentration. Micronuclei formed after mitosis from lagging chromatids or chromatin bridges between anaphase chromosomes and were stably maintained in the cells for up to one cell cycle. Nuclear buds also formed from chromatin bridges or during interphase. If the micronuclei-bearing cells entered mitosis, they either produced daughter cells without micronuclei or, more frequently, produced cells with additional micronuclei. Low concentrations of hydroxyurea efficiently induced multipolar mitosis, which generated lagging chromatids or chromatin bridges, and also generated multinuclear cells that were tightly linked to apoptosis. We found that the presence of micronuclei is related to apoptosis but not to multipolar mitosis. Furthermore, the structural heterogeneity among micronuclei, with respect to chromatin condensation or the presence of lamin B, derived from the mechanism of micronuclei formation. Our study reinforces the notion that micronucleation has important implications in the genomic plasticity of tumor cells.
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NDC |
Biology [ 460 ]
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Language |
eng
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Resource Type | journal article |
Publisher |
Public Library Science
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Date of Issued | 2010 |
Rights |
Copyright (c) 2010 2010 Utani et al. 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 credited.
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Publish Type | Version of Record |
Access Rights | open access |
Source Identifier |
[ISSN] 1932-6203
[DOI] 10.1371/journal.pone.0010089
[DOI] http://dx.doi.org/10.1371/journal.pone.0010089
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