Literature DB >> 26034280

Histone chaperone Anp32e removes H2A.Z from DNA double-strand breaks and promotes nucleosome reorganization and DNA repair.

Ozge Gursoy-Yuzugullu1, Marina K Ayrapetov1, Brendan D Price2.   

Abstract

The repair of DNA double-strand breaks (DSBs) requires open, flexible chromatin domains. The NuA4-Tip60 complex creates these flexible chromatin structures by exchanging histone H2A.Z onto nucleosomes and promoting acetylation of histone H4. Here, we demonstrate that the accumulation of H2A.Z on nucleosomes at DSBs is transient, and that rapid eviction of H2A.Z is required for DSB repair. Anp32e, an H2A.Z chaperone that interacts with the C-terminal docking domain of H2A.Z, is rapidly recruited to DSBs. Anp32e functions to remove H2A.Z from nucleosomes, so that H2A.Z levels return to basal within 10 min of DNA damage. Further, H2A.Z removal by Anp32e disrupts inhibitory interactions between the histone H4 tail and the nucleosome surface, facilitating increased acetylation of histone H4 following DNA damage. When H2A.Z removal by Anp32e is blocked, nucleosomes at DSBs retain elevated levels of H2A.Z, and assume a more stable, hypoacetylated conformation. Further, loss of Anp32e leads to increased CtIP-dependent end resection, accumulation of single-stranded DNA, and an increase in repair by the alternative nonhomologous end joining pathway. Exchange of H2A.Z onto the chromatin and subsequent rapid removal by Anp32e are therefore critical for creating open, acetylated nucleosome structures and for controlling end resection by CtIP. Dynamic modulation of H2A.Z exchange and removal by Anp32e reveals the importance of the nucleosome surface and nucleosome dynamics in processing the damaged chromatin template during DSB repair.

Entities:  

Keywords:  Anp32e; DSB repair; H2A.Z; NHEJ; genome instability

Mesh:

Substances:

Year:  2015        PMID: 26034280      PMCID: PMC4475971          DOI: 10.1073/pnas.1504868112

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  51 in total

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7.  Heterochromatin protein 1 is recruited to various types of DNA damage.

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9.  Alternative-NHEJ is a mechanistically distinct pathway of mammalian chromosome break repair.

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10.  Histone H3 methylation links DNA damage detection to activation of the tumour suppressor Tip60.

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3.  RPA Phosphorylation Inhibits DNA Resection.

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5.  PARP1-dependent recruitment of the FBXL10-RNF68-RNF2 ubiquitin ligase to sites of DNA damage controls H2A.Z loading.

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Review 7.  The tale of a tail: histone H4 acetylation and the repair of DNA breaks.

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9.  Structural basis of H2A.Z recognition by SRCAP chromatin-remodeling subunit YL1.

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10.  Schizosaccharomyces pombe KAT5 contributes to resection and repair of a DNA double-strand break.

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