García-Rubio M, et al. (2003)

Reference: García-Rubio M, et al. (2003) Recombinogenic effects of DNA-damaging agents are synergistically increased by transcription in Saccharomyces cerevisiae. New insights into transcription-associated recombination. Genetics 165(2):457-66

Reference Help

Abstract

Homologous recombination of a particular DNA sequence is strongly stimulated by transcription, a phenomenon observed from bacteria to mammals, which we refer to as transcription-associated recombination (TAR). TAR might be an accidental feature of DNA chemistry with important consequences for genetic stability. However, it is also essential for developmentally regulated processes such as class switching of immunoglobulin genes. Consequently, it is likely that TAR embraces more than one mechanism. In this study we tested the possibility that transcription induces recombination by making DNA more susceptible to recombinogenic DNA damage. Using different plasmid-chromosome and direct-repeat recombination constructs in which transcription is driven from either the P(GAL1)- or the P(tet)-regulated promoters, we have shown that either 4-nitroquinoline-N-oxide (4-NQO) or methyl methanesulfonate (MMS) produces a synergistic increase of recombination when combined with transcription. 4-NQO and MMS stimulated recombination of a transcriptionally active DNA sequence up to 12,800- and 130-fold above the spontaneous levels observed in the absence of transcription, whereas 4-NQO and MMS alone increased recombination 193- and 4.5-fold, respectively. Our results provide evidence that TAR is due, at least in part, to the ability of transcription to enhance the accessibility of DNA to exogenous chemicals and internal metabolites responsible for recombinogenic lesions. We discuss possible parallelisms between the mechanisms of induction of recombination and mutation by transcription.

Download Citation (.nbib)

Reference Type: Journal Article | Research Support, Non-U.S. Gov't
Authors: García-Rubio M, Huertas P, González-Barrera S, Aguilera A
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