A transcription factor-based mechanism for mouse heterochromatin formation

Aydan Bulut-Karslioglu; Valentina Perrera; Manuela Scaranaro; Inti Alberto De La Rosa-Velazquez; Suzanne Van De Nobelen; Nicholas Shukeir; Johannes Popow; Borbala Gerle; Susanne Opravil; Michaela Pagani; Simone Meidhof; Thomas Brabletz; Thomas Manke; Monika Lachner; Thomas Jenuwein

doi:10.1038/nsmb.2382

A transcription factor-based mechanism for mouse heterochromatin formation

Aydan Bulut-Karslioglu^*, Valentina Perrera, Manuela Scaranaro, Inti Alberto De La Rosa-Velazquez, Suzanne Van De Nobelen, Nicholas Shukeir, Johannes Popow, Borbala Gerle, Susanne Opravil, Michaela Pagani, Simone Meidhof, Thomas Brabletz, Thomas Manke, Monika Lachner, Thomas Jenuwein

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

140 Citations (Scopus)

Abstract

Heterochromatin is important for genome integrity and stabilization of gene-expression programs. We have identified the transcription factors Pax3 and Pax9 as redundant regulators of mouse heterochromatin, as they repress RNA output from major satellite repeats by associating with DNA within pericentric heterochromatin. Simultaneous depletion of Pax3 and Pax9 resulted in dramatic derepression of major satellite transcripts, persistent impairment of heterochromatic marks and defects in chromosome segregation. Genome-wide analyses of methylated histone H3 at Lys9 showed enrichment at intergenic major satellite repeats only when these sequences retained intact binding sites for Pax and other transcription factors. Additionally, bioinformatic interrogation of all histone methyltransferase Suv39h-dependent heterochromatic repeat regions in the mouse genome revealed a high concordance with the presence of transcription factor binding sites. These data define a general model in which reiterated arrangement of transcription factor binding sites within repeat sequences is an intrinsic mechanism of the formation of heterochromatin.

Original language	English
Pages (from-to)	1023-1032
Number of pages	10
Journal	Nature Structural and Molecular Biology
Volume	19
Issue number	10
DOIs	https://doi.org/10.1038/nsmb.2382
Publication status	Published - Oct 2012
Externally published	Yes

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Bulut-Karslioglu, A., Perrera, V., Scaranaro, M., De La Rosa-Velazquez, I. A., Van De Nobelen, S., Shukeir, N., Popow, J., Gerle, B., Opravil, S., Pagani, M., Meidhof, S., Brabletz, T., Manke, T., Lachner, M., & Jenuwein, T. (2012). A transcription factor-based mechanism for mouse heterochromatin formation. Nature Structural and Molecular Biology, 19(10), 1023-1032. https://doi.org/10.1038/nsmb.2382

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title = "A transcription factor-based mechanism for mouse heterochromatin formation",

abstract = "Heterochromatin is important for genome integrity and stabilization of gene-expression programs. We have identified the transcription factors Pax3 and Pax9 as redundant regulators of mouse heterochromatin, as they repress RNA output from major satellite repeats by associating with DNA within pericentric heterochromatin. Simultaneous depletion of Pax3 and Pax9 resulted in dramatic derepression of major satellite transcripts, persistent impairment of heterochromatic marks and defects in chromosome segregation. Genome-wide analyses of methylated histone H3 at Lys9 showed enrichment at intergenic major satellite repeats only when these sequences retained intact binding sites for Pax and other transcription factors. Additionally, bioinformatic interrogation of all histone methyltransferase Suv39h-dependent heterochromatic repeat regions in the mouse genome revealed a high concordance with the presence of transcription factor binding sites. These data define a general model in which reiterated arrangement of transcription factor binding sites within repeat sequences is an intrinsic mechanism of the formation of heterochromatin.",

author = "Aydan Bulut-Karslioglu and Valentina Perrera and Manuela Scaranaro and {De La Rosa-Velazquez}, {Inti Alberto} and {Van De Nobelen}, Suzanne and Nicholas Shukeir and Johannes Popow and Borbala Gerle and Susanne Opravil and Michaela Pagani and Simone Meidhof and Thomas Brabletz and Thomas Manke and Monika Lachner and Thomas Jenuwein",

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Bulut-Karslioglu, A, Perrera, V, Scaranaro, M, De La Rosa-Velazquez, IA, Van De Nobelen, S, Shukeir, N, Popow, J, Gerle, B, Opravil, S, Pagani, M, Meidhof, S, Brabletz, T, Manke, T, Lachner, M & Jenuwein, T 2012, 'A transcription factor-based mechanism for mouse heterochromatin formation', Nature Structural and Molecular Biology, vol. 19, no. 10, pp. 1023-1032. https://doi.org/10.1038/nsmb.2382

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AU - Bulut-Karslioglu, Aydan

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AU - Van De Nobelen, Suzanne

AU - Shukeir, Nicholas

AU - Popow, Johannes

AU - Gerle, Borbala

AU - Opravil, Susanne

AU - Pagani, Michaela

AU - Meidhof, Simone

AU - Brabletz, Thomas

AU - Manke, Thomas

AU - Lachner, Monika

AU - Jenuwein, Thomas

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AB - Heterochromatin is important for genome integrity and stabilization of gene-expression programs. We have identified the transcription factors Pax3 and Pax9 as redundant regulators of mouse heterochromatin, as they repress RNA output from major satellite repeats by associating with DNA within pericentric heterochromatin. Simultaneous depletion of Pax3 and Pax9 resulted in dramatic derepression of major satellite transcripts, persistent impairment of heterochromatic marks and defects in chromosome segregation. Genome-wide analyses of methylated histone H3 at Lys9 showed enrichment at intergenic major satellite repeats only when these sequences retained intact binding sites for Pax and other transcription factors. Additionally, bioinformatic interrogation of all histone methyltransferase Suv39h-dependent heterochromatic repeat regions in the mouse genome revealed a high concordance with the presence of transcription factor binding sites. These data define a general model in which reiterated arrangement of transcription factor binding sites within repeat sequences is an intrinsic mechanism of the formation of heterochromatin.

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A transcription factor-based mechanism for mouse heterochromatin formation

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