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Open AccessJournal ArticleDOI

Differences in the localization and morphology of chromosomes in the human nucleus

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TLDR
It is demonstrated that the distribution of genomic sequences between chromosomes has implications for nuclear structure and the findings are discussed in relation to a model of the human nucleus that is functionally compartmentalized.
Abstract
Using fluorescence in situ hybridization we show striking differences in nuclear position, chromosome morphology, and interactions with nuclear substructure for human chromosomes 18 and 19. Human chromosome 19 is shown to adopt a more internal position in the nucleus than chromosome 18 and to be more extensively associated with the nuclear matrix. The more peripheral localization of chromosome 18 is established early in the cell cycle and is maintained thereafter. We show that the preferential localization of chromosomes 18 and 19 in the nucleus is reflected in the orientation of translocation chromosomes in the nucleus. Lastly, we show that the inhibition of transcription can have gross, but reversible, effects on chromosome architecture. Our data demonstrate that the distribution of genomic sequences between chromosomes has implications for nuclear structure and we discuss our findings in relation to a model of the human nucleus that is functionally compartmentalized.

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Posted ContentDOI

Impact of chromosome fusions on 3D genome organization and gene expression in budding yeast

TL;DR: It is found that chromosome fusions dramatically alter 3D nuclear organization without leading to strong genome-wide changes in transcription, and a mild but significant and reproducible increase in expression of genes near fusion sites is observed.
Proceedings Article

Analysis of biomathematically predicted Scaffold / Matrix Attached Regions (S/MARs) by three different approaches.

TL;DR: Teilergebnisse aus dieser Arbeit wurden mit Genehmigung der Gemeinsamen Naturwissen-schaftlichen Fakultät vertreten durch den Mentor der Arbeit veröffentlicht.
Book ChapterDOI

Quantitative Approaches to Nuclear Architecture Analysis and Modelling

TL;DR: A brief introduction will be given into quantitative experimental and modelling approaches to large scale nuclear genome architecture in human cells, and two novel examples for quantitative computer modelling are presented.
Posted ContentDOI

Dynamic nuclear lamina-chromatin interactions during G1 progression

TL;DR: In this paper, a modified version of the Tyramide-Signal Amplification sequencing (TSA-seq) was used to uncover a dynamic NL-chromatin interaction as cells progress through G1.
Journal ArticleDOI

Spatial arrangement of the human genome and its possible functional role

TL;DR: In eukaryotic cell nuclei genomic DNA interacts with histones to form nucleosome; arrays of nucleosomes are packaged into chromatin fibers that constitute chromatin in interphase celluclei, chromatides and chromosomes in mitotic cells.
References
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Journal ArticleDOI

Organization of the higher-order chromatin loop: specific DNA attachment sites on nuclear scaffold

TL;DR: Data are presented for sequence-specific chromatin-loop organization in histone-depleted nuclei from Drosophila melanogaster Kc cells and a family of attachment sites related by hybridization to those of the hsp70 genes was discovered.
Journal ArticleDOI

Replicon clusters are stable units of chromosome structure: evidence that nuclear organization contributes to the efficient activation and propagation of S phase in human cells.

TL;DR: It is proposed that the coordinated replication of related groups of replicons, that form stable replicon clusters, contributes to the efficient activation and propagation of S phase in mammalian cells.
Journal ArticleDOI

Association of Transcriptionally Silent Genes with Ikaros Complexes at Centromeric Heterochromatin

TL;DR: It is shown that transcriptionally inactive but not transcriptionally active genes associate with Ikaros-heterochromatin foci, which support a model of organization of the nucleus in which repressed genes are selectively recruited into centromeric domains.
Journal ArticleDOI

The inactive X chromosome in female mammals is distinguished by a lack of histone H4 acetylation, a cytogenetic marker for gene expression

TL;DR: In this paper, immunolabeled human and mouse metaphase chromosomes with antibodies specific for the acetylated isoforms of histone H4 were labeled in regions corresponding to conventional R bands (regions enriched in coding DNA), except for a single chromosome in female cells.
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