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Open AccessJournal ArticleDOI

An ectopic human XIST gene can induce chromosome inactivation in postdifferentiation human HT-1080 cells

TLDR
Investigation of four adult male HT-1080 fibrosarcoma cell lines expressing ectopic human XIST demonstrates that these postdifferentiation cells can undergo chromosomal inactivation outside of any normal developmental context, and suggests that autosomal in activation may confer a selective disadvantage.
Abstract
It has been believed that XIST RNA requires a discrete window in early development to initiate the series of chromatin-remodeling events that form the heterochromatic inactive X chromosome. Here we investigate four adult male HT-1080 fibrosarcoma cell lines expressing ectopic human XIST and demonstrate that these postdifferentiation cells can undergo chromosomal inactivation outside of any normal developmental context. All four clonal lines inactivated the transgene-containing autosome to varying degrees and with variable stability. One clone in particular consistently localized the ectopic XIST RNA to a discrete chromosome territory that exhibited striking hallmarks of inactivation, including long-range transcriptional inactivation. Results suggest that some postdifferentiation cell lines are capable of de novo chromosomal inactivation; however, long-term retention of autosomal inactivation was less common, which suggests that autosomal inactivation may confer a selective disadvantage. These results have fundamental significance for understanding genomic programming in early development.

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Accumulation of mutant lamin A causes progressive changes in nuclear architecture in Hutchinson-Gilford progeria syndrome.

TL;DR: It is shown by light and electron microscopy that HGPS is associated with significant changes in nuclear shape, including lobulation of the nuclear envelope, thickening of thenuclear lamina, loss of peripheral heterochromatin, and clustering of nuclear pores.
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Establishment of Histone H3 Methylation on the Inactive X Chromosome Requires Transient Recruitment of Eed-Enx1 Polycomb Group Complexes

TL;DR: Functional analysis demonstrates that Eed-Enx1 is required to establish methylation of histone H3 at lysine 9 and/or lysines 27 on Xi and that this, in turn, is needed to stabilize the Xi chromatin structure.
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Silencing of unsynapsed meiotic chromosomes in the mouse.

TL;DR: It is shown that silencing of unpaired (unsynapsed) chromosome regions also takes place in the mouse during both male and female meiosis, which impacts on the interpretation of the relationship between synaptic errors and sterility in mammals and extends the understanding of the biology of Brca1.
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X chromosome dosage compensation: how mammals keep the balance

TL;DR: Various facets of the ever-expanding field of mammalian dosage compensation are reviewed and its evolutionary, developmental, and mechanistic components are discussed.
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A novel role for Xist RNA in the formation of a repressive nuclear compartment into which genes are recruited when silenced

TL;DR: It is proposed that Xist RNA has multiple functions: A-repeat-independent creation of a transcriptionally silent nuclear compartment; and A- Repeat-dependent induction of gene repression, which is associated with their translocation into this silent domain.
References
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Journal ArticleDOI

Requirement for Xist in X chromosome inactivation

TL;DR: Evidence for gene targeting of Xist, the proposed candidate for the X inactivation centre, is provided, and its absolute requirement in the process of X chromosome inactivation is provided.
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XIST RNA paints the inactive X chromosome at interphase: evidence for a novel RNA involved in nuclear/chromosome structure.

TL;DR: Collective results indicate that XIST RNA may be an architectural element of the interphase chromosome territory, possibly a component of nonchromatin nuclear structure that specifically associates with Xi.
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Characterization of a newly derived human sarcoma cell line (ht-1080)

TL;DR: A tumor cell line was derived from the fibrosarcoma of a 35‐year‐old Caucasian man who died without having received chemotherapy or radiotherapy, and an aberrant karyology with marker chromosomes was present.
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Visualization of focal sites of transcription within human nuclei

TL;DR: Both nucleolar and extra‐nucleolar foci remain after nucleolytic removal of approximately 90% chromatin, suggesting an underlying structure probably organizes groups of transcription units into ‘factories’ where transcripts are both synthesized and processed.
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A Shift from Reversible to Irreversible X Inactivation Is Triggered during ES Cell Differentiation

TL;DR: A full-length mouse Xist cDNA transgene and an inducible expression system facilitating controlled Xist expression in ES cells and differentiated cultures are generated, suggesting that reversible repression by Xist is a required initiation step that might occur during normal X inactivation in female cells.
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