Alao JP, et al. (2009)

Reference: Alao JP, et al. (2009) Inhibition of type I histone deacetylase increases resistance of checkpoint-deficient cells to genotoxic agents through mitotic delay. Mol Cancer Ther 8(9):2606-15

Reference Help

Abstract

Histone deacetylase (HDAC) inhibitors potently inhibit tumor growth and are currently being evaluated for their efficacy as chemosensitizers and radiosensitizers. This efficacy is likely to be limited by the fact that HDAC inhibitors also induce cell cycle arrest. Deletion of the class I HDAC Rpd3 has been shown to specifically suppress the sensitivity of Saccharomyces cerevisiae DNA damage checkpoint mutants to UV and hydroxyurea. We show that in the fission yeast Schizosaccharomyces pombe, inhibition of the homologous class I HDAC specifically suppresses the DNA damage sensitivity of checkpoint mutants. Importantly, the prototype HDAC inhibitor Trichostatin A also suppressed the sensitivity of DNA damage checkpoint but not of DNA repair mutants to UV and HU. TSA suppressed DNA damage activity independently of the mitogen-activated protein kinase-dependent and spindle checkpoint pathways. We show that TSA delays progression into mitosis and propose that this is the main mechanism for suppression of the DNA damage sensitivity of S. pombe checkpoint mutants, partially compensating for the loss of the G(2) checkpoint pathway. Our studies also show that the ability of HDAC inhibitors to suppress DNA damage sensitivity is not species specific. Class I HDACs are the major target of HDAC inhibitors and cancer cells are often defective in checkpoint activation. Effective use of these agents as chemosensitizers and radiosensitizers may require specific treatment schedules that circumvent their inhibition of cell cycle progression.

PMID: 19723888
DOI full text
PubMed
PubTator

Download Citation (.nbib)

Reference Type: Journal Article | Research Support, Non-U.S. Gov't
Authors: Alao JP, Olesch J, Sunnerhagen P
Primary Lit For
Additional Lit For
Review For

Gene Ontology Annotations

Evidence ID	Analyze ID	Gene/Complex	Systematic Name/Complex Accession	Qualifier	Gene Ontology Term ID	Gene Ontology Term	Aspect	Annotation Extension	Evidence	Method	Source	Assigned On	Reference

Download (.txt)

Analyze

Phenotype Annotations

Evidence ID	Analyze ID	Gene	Gene Systematic Name	Phenotype	Experiment Type	Experiment Type Category	Mutant Information	Strain Background	Chemical	Details	Reference

Download (.txt)

Analyze

Disease Annotations

Evidence ID	Analyze ID	Gene	Gene Systematic Name	Disease Ontology Term	Disease Ontology Term ID	Qualifier	Evidence	Method	Source	Assigned On		Reference

Download (.txt)

Analyze

Regulation Annotations

Evidence ID	Analyze ID	Regulator	Regulator Systematic Name	Target	Target Systematic Name	Direction	Regulation of	Happens During	Regulator Type	Direction	Regulation Of	Happens During	Method	Evidence	Strain Background	Reference

Download (.txt)

Analyze

Post-translational Modifications

				Site		Modification	Modifier	Source	Reference

Download (.txt)

Analyze

Interaction Annotations

Genetic Interactions

Evidence ID	Analyze ID		Interactor	Interactor Systematic Name	Interactor	Interactor Systematic Name	Allele	Assay	Annotation	Action	Phenotype	SGA score	P-value	Source	Reference	Note

Download (.txt)

Analyze

Physical Interactions

Evidence ID	Analyze ID		Interactor	Interactor Systematic Name	Interactor	Interactor Systematic Name	Assay	Annotation	Action	Modification	Source	Reference	Note

Download (.txt)

Analyze

Functional Complementation Annotations

Complement ID	Locus ID	Gene	Species	Gene ID	Strain background	Direction	Details	Source	Reference

Download (.txt)

Analyze

Published Datasets

Evidence ID	Analyze ID		Dataset	Description	Keywords	Number of Conditions	Reference

Download (.txt)

Analyze

Downloadable Files

Evidence ID	Analyze ID		File	Description

Download (.txt)

Analyze