Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.

Studies of higher-order chromatin arrangements are an essential part of ongoing attempts to explore changes in epigenome structure and their functional implications during development and cell differentiation. However, the extent and cell-type-specificity of three-dimensional (3D) chromosome arrange...

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Main Authors: Andreas Bolzer, Gregor Kreth, Irina Solovei, Daniela Koehler, Kaan Saracoglu, Christine Fauth, Stefan Müller, Roland Eils, Christoph Cremer, Michael R Speicher, Thomas Cremer
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2005-05-01
Series:PLoS Biology
Online Access:https://doi.org/10.1371/journal.pbio.0030157
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spelling doaj-65a0712be0d3411c9e4e3ac04635aea92021-07-02T17:09:54ZengPublic Library of Science (PLoS)PLoS Biology1544-91731545-78852005-05-0135e15710.1371/journal.pbio.0030157Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.Andreas BolzerGregor KrethIrina SoloveiDaniela KoehlerKaan SaracogluChristine FauthStefan MüllerRoland EilsChristoph CremerMichael R SpeicherThomas CremerStudies of higher-order chromatin arrangements are an essential part of ongoing attempts to explore changes in epigenome structure and their functional implications during development and cell differentiation. However, the extent and cell-type-specificity of three-dimensional (3D) chromosome arrangements has remained controversial. In order to overcome technical limitations of previous studies, we have developed tools that allow the quantitative 3D positional mapping of all chromosomes simultaneously. We present unequivocal evidence for a probabilistic 3D order of prometaphase chromosomes, as well as of chromosome territories (CTs) in nuclei of quiescent (G0) and cycling (early S-phase) human diploid fibroblasts (46, XY). Radial distance measurements showed a probabilistic, highly nonrandom correlation with chromosome size: small chromosomes-independently of their gene density-were distributed significantly closer to the center of the nucleus or prometaphase rosette, while large chromosomes were located closer to the nuclear or rosette rim. This arrangement was independently confirmed in both human fibroblast and amniotic fluid cell nuclei. Notably, these cell types exhibit flat-ellipsoidal cell nuclei, in contrast to the spherical nuclei of lymphocytes and several other human cell types, for which we and others previously demonstrated gene-density-correlated radial 3D CT arrangements. Modeling of 3D CT arrangements suggests that cell-type-specific differences in radial CT arrangements are not solely due to geometrical constraints that result from nuclear shape differences. We also found gene-density-correlated arrangements of higher-order chromatin shared by all human cell types studied so far. Chromatin domains, which are gene-poor, form a layer beneath the nuclear envelope, while gene-dense chromatin is enriched in the nuclear interior. We discuss the possible functional implications of this finding.https://doi.org/10.1371/journal.pbio.0030157
collection DOAJ
language English
format Article
sources DOAJ
author Andreas Bolzer
Gregor Kreth
Irina Solovei
Daniela Koehler
Kaan Saracoglu
Christine Fauth
Stefan Müller
Roland Eils
Christoph Cremer
Michael R Speicher
Thomas Cremer
spellingShingle Andreas Bolzer
Gregor Kreth
Irina Solovei
Daniela Koehler
Kaan Saracoglu
Christine Fauth
Stefan Müller
Roland Eils
Christoph Cremer
Michael R Speicher
Thomas Cremer
Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
PLoS Biology
author_facet Andreas Bolzer
Gregor Kreth
Irina Solovei
Daniela Koehler
Kaan Saracoglu
Christine Fauth
Stefan Müller
Roland Eils
Christoph Cremer
Michael R Speicher
Thomas Cremer
author_sort Andreas Bolzer
title Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
title_short Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
title_full Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
title_fullStr Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
title_full_unstemmed Three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
title_sort three-dimensional maps of all chromosomes in human male fibroblast nuclei and prometaphase rosettes.
publisher Public Library of Science (PLoS)
series PLoS Biology
issn 1544-9173
1545-7885
publishDate 2005-05-01
description Studies of higher-order chromatin arrangements are an essential part of ongoing attempts to explore changes in epigenome structure and their functional implications during development and cell differentiation. However, the extent and cell-type-specificity of three-dimensional (3D) chromosome arrangements has remained controversial. In order to overcome technical limitations of previous studies, we have developed tools that allow the quantitative 3D positional mapping of all chromosomes simultaneously. We present unequivocal evidence for a probabilistic 3D order of prometaphase chromosomes, as well as of chromosome territories (CTs) in nuclei of quiescent (G0) and cycling (early S-phase) human diploid fibroblasts (46, XY). Radial distance measurements showed a probabilistic, highly nonrandom correlation with chromosome size: small chromosomes-independently of their gene density-were distributed significantly closer to the center of the nucleus or prometaphase rosette, while large chromosomes were located closer to the nuclear or rosette rim. This arrangement was independently confirmed in both human fibroblast and amniotic fluid cell nuclei. Notably, these cell types exhibit flat-ellipsoidal cell nuclei, in contrast to the spherical nuclei of lymphocytes and several other human cell types, for which we and others previously demonstrated gene-density-correlated radial 3D CT arrangements. Modeling of 3D CT arrangements suggests that cell-type-specific differences in radial CT arrangements are not solely due to geometrical constraints that result from nuclear shape differences. We also found gene-density-correlated arrangements of higher-order chromatin shared by all human cell types studied so far. Chromatin domains, which are gene-poor, form a layer beneath the nuclear envelope, while gene-dense chromatin is enriched in the nuclear interior. We discuss the possible functional implications of this finding.
url https://doi.org/10.1371/journal.pbio.0030157
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