Regulation of HP1–chromatin binding by histone H3 methylation and phosphorylation

Fischle, Wolfgang; Tseng, Boo Shan; Dormann, Holger L.; Ueberheide, Beatrix; Garcia, Benjamin A.; Shabanowitz, Jeffrey; Hunt, Donald F.; Funabiki, Hironori; Allis, C. David

doi:10.1038/nature04219

Cited by 872 publications

(869 citation statements)

References 47 publications

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“…In the case of Aurora B, Sgo appears not to be the only relevant target of the kinase in this prophase pathway. Other possible targets could be condensin, heterochromatin protein 1 (HP1), or some other protein yet to be identified (Fischle et al 2005;Hirota et al 2005;Lipp et al 2007). …”

Section: Discussionmentioning

confidence: 99%

Shugoshin regulates cohesion by driving relocalization of PP2A in Xenopus extracts

Rivera

Losada

2008

Chromosoma

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Section: Discussionmentioning

confidence: 99%

Shugoshin regulates cohesion by driving relocalization of PP2A in Xenopus extracts

Rivera

Losada

2008

Chromosoma

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“…It is intriguing that the amino acids in the histone H3 tail recognized by WDR5, in particular R2 and T3, are known to be methylated and phosphorylated in vivo. Couture et al (16) showed that these PTMs inhibit WDR5 binding, and this lends further credence to the concept of a "phosphomethyl switch" in which the modification status of the histone tail regulates its ability to undergo subsequent PTMs (20).…”

Section: Subsequent Inmentioning

confidence: 87%

MLL Core Components Give the Green Light to Histone Methylation

Crawford

Hess

2006

ACS Chem. Biol.

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“…Further, combinations of multiple modifications result in a context-dependent outcome on transcription (reviewed in . For example, H3K9me3 generally recruits HP1 to repress transcription, but in combination with phosphorylation of the adjacent H3S10, HP1 binding is abrogated and repression may be relieved (Fischle et al, 2005;Mateescu et al, 2008). Thus histone and DNA modifications superimpose a rich layer of information on the underlying DNA sequence.…”

Section: Molecular Mechanism Of Transcriptional Regulation and Epigenmentioning

confidence: 99%

The Epigenetic Landscape of Lineage Choice: Lessons From the Heritability of Cd4 and Cd8 Expression

Gialitakis¹,

Sellars²,

Littman³

2011

Current Topics in Microbiology and Immunology

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Developing αβ T cells choose between the helper and cytotoxic lineages, depending upon the specificity of their T cell receptors for MHC molecules. The expression of the CD4 co-receptor on helper cells and the CD8 co-receptor on cytotoxic cells is intimately linked to this decision, and their regulation at the transcriptional level has been the subject of intense study to better understand lineage choice. Indeed, as the fate of developing T cells is decided, the expression status of these genes is accordingly locked. Genetic models have revealed important transcriptional elements and the ability to manipulate these elements in the framework of development has added a new perspective on the temporal nature of their function and the epigenetic maintenance of gene expression. We examine here the novel insights into epigenetic mechanisms that have arisen through the study of these genes.

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Regulation of HP1–chromatin binding by histone H3 methylation and phosphorylation

Cited by 872 publications

References 47 publications

Shugoshin regulates cohesion by driving relocalization of PP2A in Xenopus extracts

Shugoshin regulates cohesion by driving relocalization of PP2A in Xenopus extracts

MLL Core Components Give the Green Light to Histone Methylation

The Epigenetic Landscape of Lineage Choice: Lessons From the Heritability of Cd4 and Cd8 Expression

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