Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories

Chromatin moves with subdiffusive and spatially constrained dynamics within the cell nucleus. Here, we use single-locus tracking by time-lapse fluorescence microscopy to uncover information regarding the forces that influence chromatin movement following the induction of a persistent DNA double-stra...

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Main Authors: Assaf Amitai, Andrew Seeber, Susan M. Gasser, David Holcman
Format: Article
Language:English
Published: Elsevier 2017-01-01
Series:Cell Reports
Subjects:
Online Access:http://www.sciencedirect.com/science/article/pii/S2211124717300542
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spelling doaj-78c65dd2255c43b4bbc593c2c27ac8ee2020-11-25T01:13:26ZengElsevierCell Reports2211-12472017-01-011851200121410.1016/j.celrep.2017.01.018Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus TrajectoriesAssaf Amitai0Andrew Seeber1Susan M. Gasser2David Holcman3Institut de Biologie de l’École Normale Supérieure, Ecole Normale Supérieure, 46 rue d’Ulm, 75005 Paris, FranceFriedrich Miescher Institute for Biomedical Research, Maulbeerstrasse 66, 4058 Basel, SwitzerlandFriedrich Miescher Institute for Biomedical Research, Maulbeerstrasse 66, 4058 Basel, SwitzerlandInstitut de Biologie de l’École Normale Supérieure, Ecole Normale Supérieure, 46 rue d’Ulm, 75005 Paris, FranceChromatin moves with subdiffusive and spatially constrained dynamics within the cell nucleus. Here, we use single-locus tracking by time-lapse fluorescence microscopy to uncover information regarding the forces that influence chromatin movement following the induction of a persistent DNA double-strand break (DSB). Using improved time-lapse imaging regimens, we monitor trajectories of tagged DNA loci at a high temporal resolution, which allows us to extract biophysical parameters through robust statistical analysis. Polymer modeling based on these parameters predicts chromatin domain expansion near a DSB and damage extrusion from the domain. Both phenomena are confirmed by live imaging in budding yeast. Calculation of the anomalous exponent of locus movement allows us to differentiate forces imposed on the nucleus through the actin cytoskeleton from those that arise from INO80 remodeler-dependent changes in nucleosome organization. Our analytical approach can be applied to high-density single-locus trajectories obtained in any cell type.http://www.sciencedirect.com/science/article/pii/S2211124717300542chromatin dynamicsnucleosome compactionpolymer modeldouble-strand breakactin cytoskeletonmicrotubulestime-lapse imagingDNA damageDNA mobilitynumerical stimulations
collection DOAJ
language English
format Article
sources DOAJ
author Assaf Amitai
Andrew Seeber
Susan M. Gasser
David Holcman
spellingShingle Assaf Amitai
Andrew Seeber
Susan M. Gasser
David Holcman
Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
Cell Reports
chromatin dynamics
nucleosome compaction
polymer model
double-strand break
actin cytoskeleton
microtubules
time-lapse imaging
DNA damage
DNA mobility
numerical stimulations
author_facet Assaf Amitai
Andrew Seeber
Susan M. Gasser
David Holcman
author_sort Assaf Amitai
title Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
title_short Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
title_full Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
title_fullStr Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
title_full_unstemmed Visualization of Chromatin Decompaction and Break Site Extrusion as Predicted by Statistical Polymer Modeling of Single-Locus Trajectories
title_sort visualization of chromatin decompaction and break site extrusion as predicted by statistical polymer modeling of single-locus trajectories
publisher Elsevier
series Cell Reports
issn 2211-1247
publishDate 2017-01-01
description Chromatin moves with subdiffusive and spatially constrained dynamics within the cell nucleus. Here, we use single-locus tracking by time-lapse fluorescence microscopy to uncover information regarding the forces that influence chromatin movement following the induction of a persistent DNA double-strand break (DSB). Using improved time-lapse imaging regimens, we monitor trajectories of tagged DNA loci at a high temporal resolution, which allows us to extract biophysical parameters through robust statistical analysis. Polymer modeling based on these parameters predicts chromatin domain expansion near a DSB and damage extrusion from the domain. Both phenomena are confirmed by live imaging in budding yeast. Calculation of the anomalous exponent of locus movement allows us to differentiate forces imposed on the nucleus through the actin cytoskeleton from those that arise from INO80 remodeler-dependent changes in nucleosome organization. Our analytical approach can be applied to high-density single-locus trajectories obtained in any cell type.
topic chromatin dynamics
nucleosome compaction
polymer model
double-strand break
actin cytoskeleton
microtubules
time-lapse imaging
DNA damage
DNA mobility
numerical stimulations
url http://www.sciencedirect.com/science/article/pii/S2211124717300542
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