A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.

Proper assembly of the spindle apparatus is crucially important for faithful chromosome segregation during anaphase. Thanks to the effort over the last decades, we have very detailed information about many events leading to spindle assembly and chromosome segregation, however we still do not underst...

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Main Authors: Lucia Novakova, Kristina Kovacovicova, Thanh Quang Dang-Nguyen, Martin Sodek, Michal Skultety, Martin Anger
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4757572?pdf=render
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spelling doaj-b055a2b2855146f5bf2e68ca3034ee4e2020-11-24T22:15:44ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01112e014953510.1371/journal.pone.0149535A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.Lucia NovakovaKristina KovacovicovaThanh Quang Dang-NguyenMartin SodekMichal SkultetyMartin AngerProper assembly of the spindle apparatus is crucially important for faithful chromosome segregation during anaphase. Thanks to the effort over the last decades, we have very detailed information about many events leading to spindle assembly and chromosome segregation, however we still do not understand certain aspects, including, for example, spindle length control. When tight regulation of spindle size is lost, chromosome segregation errors emerge. Currently, there are several hypotheses trying to explain the molecular mechanism of spindle length control. The number of kinetochores, activity of molecular rulers, intracellular gradients, cell size, limiting spindle components, and the balance of the spindle forces seem to contribute to spindle size regulation, however some of these mechanisms are likely specific to a particular cell type. In search for a general regulatory mechanism, in our study we focused on the role of cell size and nuclear to cytoplasmic ratio in this process. To this end, we used relatively large cells isolated from 2-cell mouse embryos. Our results showed that the spindle size upper limit is not reached in these cells and suggest that accurate control of spindle length requires balanced ratio between nuclear and cytoplasmic volumes.http://europepmc.org/articles/PMC4757572?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Lucia Novakova
Kristina Kovacovicova
Thanh Quang Dang-Nguyen
Martin Sodek
Michal Skultety
Martin Anger
spellingShingle Lucia Novakova
Kristina Kovacovicova
Thanh Quang Dang-Nguyen
Martin Sodek
Michal Skultety
Martin Anger
A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
PLoS ONE
author_facet Lucia Novakova
Kristina Kovacovicova
Thanh Quang Dang-Nguyen
Martin Sodek
Michal Skultety
Martin Anger
author_sort Lucia Novakova
title A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
title_short A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
title_full A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
title_fullStr A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
title_full_unstemmed A Balance between Nuclear and Cytoplasmic Volumes Controls Spindle Length.
title_sort balance between nuclear and cytoplasmic volumes controls spindle length.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2016-01-01
description Proper assembly of the spindle apparatus is crucially important for faithful chromosome segregation during anaphase. Thanks to the effort over the last decades, we have very detailed information about many events leading to spindle assembly and chromosome segregation, however we still do not understand certain aspects, including, for example, spindle length control. When tight regulation of spindle size is lost, chromosome segregation errors emerge. Currently, there are several hypotheses trying to explain the molecular mechanism of spindle length control. The number of kinetochores, activity of molecular rulers, intracellular gradients, cell size, limiting spindle components, and the balance of the spindle forces seem to contribute to spindle size regulation, however some of these mechanisms are likely specific to a particular cell type. In search for a general regulatory mechanism, in our study we focused on the role of cell size and nuclear to cytoplasmic ratio in this process. To this end, we used relatively large cells isolated from 2-cell mouse embryos. Our results showed that the spindle size upper limit is not reached in these cells and suggest that accurate control of spindle length requires balanced ratio between nuclear and cytoplasmic volumes.
url http://europepmc.org/articles/PMC4757572?pdf=render
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