Literature DB >> 21685366

Analysis of protein dynamics at active, stalled, and collapsed replication forks.

Bianca M Sirbu1, Frank B Couch, Jordan T Feigerle, Srividya Bhaskara, Scott W Hiebert, David Cortez.   

Abstract

Successful DNA replication and packaging of newly synthesized DNA into chromatin are essential to maintain genome integrity. Defects in the DNA template challenge genetic and epigenetic inheritance. Unfortunately, tracking DNA damage responses (DDRs), histone deposition, and chromatin maturation at replication forks is difficult in mammalian cells. Here we describe a technology called iPOND (isolation of proteins on nascent DNA) to analyze proteins at active and damaged replication forks at high resolution. Using this methodology, we define the timing of histone deposition and chromatin maturation. Class 1 histone deacetylases are enriched at replisomes and remove predeposition marks on histone H4. Chromatin maturation continues even when decoupled from replisome movement. Furthermore, fork stalling causes changes in the recruitment and phosphorylation of proteins at the damaged fork. Checkpoint kinases catalyze H2AX phosphorylation, which spreads from the stalled fork to include a large chromatin domain even prior to fork collapse and double-strand break formation. Finally, we demonstrate a switch in the DDR at persistently stalled forks that includes MRE11-dependent RAD51 assembly. These data reveal a dynamic recruitment of proteins and post-translational modifications at damaged forks and surrounding chromatin. Furthermore, our studies establish iPOND as a useful methodology to study DNA replication and chromatin maturation.

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Year:  2011        PMID: 21685366      PMCID: PMC3127432          DOI: 10.1101/gad.2053211

Source DB:  PubMed          Journal:  Genes Dev        ISSN: 0890-9369            Impact factor:   11.361


  43 in total

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2.  FK228 (depsipeptide) as a natural prodrug that inhibits class I histone deacetylases.

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3.  Hdac3 is essential for the maintenance of chromatin structure and genome stability.

Authors:  Srividya Bhaskara; Sarah K Knutson; Guochun Jiang; Mahesh B Chandrasekharan; Andrew J Wilson; Siyuan Zheng; Ashwini Yenamandra; Kimberly Locke; Jia-Ling Yuan; Alyssa R Bonine-Summers; Christina E Wells; Jonathan F Kaiser; M Kay Washington; Zhongming Zhao; Florence F Wagner; Zu-Wen Sun; Fen Xia; Edward B Holson; Dineo Khabele; Scott W Hiebert
Journal:  Cancer Cell       Date:  2010-11-16       Impact factor: 31.743

4.  Combining ATR suppression with oncogenic Ras synergistically increases genomic instability, causing synthetic lethality or tumorigenesis in a dosage-dependent manner.

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6.  Histone H2AX is phosphorylated in an ATR-dependent manner in response to replicational stress.

Authors:  I M Ward; J Chen
Journal:  J Biol Chem       Date:  2001-10-22       Impact factor: 5.157

Review 7.  Epigenetic modifications in double-strand break DNA damage signaling and repair.

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Journal:  Clin Cancer Res       Date:  2010-09-07       Impact factor: 12.531

Review 8.  Differences in the DNA replication of unicellular eukaryotes and metazoans: known unknowns.

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9.  MDC1 collaborates with TopBP1 in DNA replication checkpoint control.

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10.  Duplication and maintenance of heterochromatin domains.

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  226 in total

1.  RAD51 mutants cause replication defects and chromosomal instability.

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2.  Schizosaccharomyces pombe Hat1 (Kat1) is associated with Mis16 and is required for telomeric silencing.

Authors:  Kevin Tong; Thomas Keller; Charles S Hoffman; Anthony T Annunziato
Journal:  Eukaryot Cell       Date:  2012-07-06

Review 3.  Viral and cellular interactions during adenovirus DNA replication.

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4.  SMARCAL1 catalyzes fork regression and Holliday junction migration to maintain genome stability during DNA replication.

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5.  ATR phosphorylates SMARCAL1 to prevent replication fork collapse.

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6.  The SNM1B/APOLLO DNA nuclease functions in resolution of replication stress and maintenance of common fragile site stability.

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7.  Identification of proteins at active, stalled, and collapsed replication forks using isolation of proteins on nascent DNA (iPOND) coupled with mass spectrometry.

Authors:  Bianca M Sirbu; W Hayes McDonald; Huzefa Dungrawala; Akosua Badu-Nkansah; Gina M Kavanaugh; Yaoyi Chen; David L Tabb; David Cortez
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8.  Single-Molecule Imaging Reveals How Mre11-Rad50-Nbs1 Initiates DNA Break Repair.

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Review 9.  DNA Damage Response Assessments in Human Tumor Samples Provide Functional Biomarkers of Radiosensitivity.

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Review 10.  WEE1 tyrosine kinase, a novel epigenetic modifier.

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