Role of the <i>Saccharomyces cerevisiae</i> Rad51 Paralogs in Sister Chromatid Recombination

Mozlin, Amy M.; Fung, Cindy W.; Symington, Lorraine S.

doi:10.1534/genetics.107.082677

Cited by 64 publications

(104 citation statements)

References 71 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These results suggest that each of these Rad51 paralogs has a nonredundant function in HR. Interestingly, although overexpression of S. cerevisiae RAD51 reverses a defect in DSB-induced HR in rad55 and rad57 mutants, RAD51 overexpression was not able to suppress the spontaneous SCR defect in rad57 mutants, suggesting a specialized role for Rad51 paralogs in the repair of daughter strand gaps that arise as a result of stalled replication forks (43). In this regard, mammalian XRCC3 has been shown to be required for replication fork progression in cells treated with DNA replication inhibitors (23).…”

Section: Discussionmentioning

confidence: 99%

XRCC2 and XRCC3 Regulate the Balance between Short- and Long-Tract Gene Conversions between Sister Chromatids

Nagaraju

Hartlerode

Kwok

et al. 2009

Molecular and Cellular Biology

View full text Add to dashboard Cite

Sister chromatid recombination (SCR) is a potentially error-free pathway for the repair of DNA lesions associated with replication and is thought to be important for suppressing genomic instability. The mechanisms regulating the initiation and termination of SCR in mammalian cells are poorly understood. Previous work has implicated all the Rad51 paralogs in the initiation of gene conversion and the Rad51C/XRCC3 complex in its termination. Here, we show that hamster cells deficient in the Rad51 paralog XRCC2, a component of the Rad51B/Rad51C/Rad51D/XRCC2 complex, reveal a bias in favor of long-tract gene conversion (LTGC) during SCR. This defect is corrected by expression of wild-type XRCC2 and also by XRCC2 mutants defective in ATP binding and hydrolysis. In contrast, XRCC3-mediated homologous recombination and suppression of LTGC are dependent on ATP binding and hydrolysis. These results reveal an unexpectedly general role for Rad51 paralogs in the control of the termination of gene conversion between sister chromatids.

show abstract

Section: Discussionmentioning

confidence: 99%

XRCC2 and XRCC3 Regulate the Balance between Short- and Long-Tract Gene Conversions between Sister Chromatids

Nagaraju

Hartlerode

Kwok

et al. 2009

Molecular and Cellular Biology

View full text Add to dashboard Cite

show abstract

“…Replication of nicked DNA molecules can give rise to a recombinogenic DSB (22,30). In addition, nicked or gapped DNA molecules can stimulate conversion directly, without being converted to a DSB (31)(32)(33).…”

Section: Effect Of Gamma Irradiation On Cell Viability and The Frequementioning

confidence: 99%

Mitotic gene conversion events induced in G1-synchronized yeast cells by gamma rays are similar to spontaneous conversion events

Lee

Petes

2010

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

In a previous study, we mapped spontaneous mitotic reciprocal crossovers (RCOs) in a 120-kb interval of chromosome V of Saccharomyces cerevisiae. About three-quarters of the crossovers were associated with gene conversion tracts. About 40% of these conversion tracts had the pattern expected as a consequence of repair of a double-stranded DNA break (DSB) of an unreplicated chromosome. We test this hypothesis by examining the crossovers and gene conversion events induced by gamma irradiation in G1-and G2-arrested diploid yeast cells. The gene conversion patterns of G1-irradiated cells (but not G2-irradiated cells) mimic conversion events associated with spontaneous RCOs, confirming our previous conclusion that many spontaneous crossovers are initiated by a DSB on an unreplicated chromosome.homologous recombination | DNA breaks | Saccharomyces cerevisae | loss of heterozygosity H omologous mitotic recombination is an efficient method of repairing double-stranded breaks (DSBs) in the yeast Saccharomyces cerevisiae and other organisms (1). Although mitotic recombination was described in Drosophila more than 70 years ago (2), many of the basic properties of mitotic recombination are not understood. The chromosomes resulting from a mitotic recombination event are segregated into two daughter cells and one problem is that most analytic methods select for only one of the cells containing the recombinant chromosomes.A method for selecting both daughter cells with the products expected from reciprocal crossing over (RCO) is shown in Fig. 1. A diploid yeast strain is constructed in which one copy of chromosome V has an ochre mutation in the CAN1 gene (can1-100); in the absence of an ochre suppressor, such strains are resistant to canavanine. On the other homologue, the CAN1 gene has been replaced by SUP4-o, a gene encoding an ochre-suppressing tRNA. The diploid is also homozygous for the ade2-1 ochre mutation. Yeast strains containing the ade2-1 allele without a nonsense suppressor are Ade − and form red colonies as a result of accumulation of red precursor to adenine (3). In the diploid depicted in Fig. 1, because of the presence of the SUP4-o gene, the cells are canavanine-sensitive, Ade + , and form white colonies.A RCO between the centromere of chromosome V and the can1-100/SUP4-o markers will result in two Can R daughter cells that will subsequently grow to form a red/white sectored Can R colony (4). As a consequence of the RCO, polymorphisms distal to the crossover point become homozygous in the two sectors, whereas polymorphisms proximal to the exchange retain heterozygosity ( Fig.

show abstract

“…Mutation of RAD51, RAD55, or RAD57 confers sensitivity of ionizing radiation (IR) and defects in mitotic and meiotic recombination, indicating that their functions are not redundant (Symington 2002). rad51 mutants generally exhibit more severe defects than rad55 or rad57 mutants in DSB-induced recombination assays; however, rad55 and rad57 mutants are more defective than rad51 in some assays that measure spontaneous recombination between repeated sequences (Rattray and Symington 1995;Mozlin et al 2008).The molecular details of homologous recombination are largely based on genetic, physical, and cytological studies of DSB repair (DSBR) and on biochemical characterization of purified proteins (Paques and Haber 1999;Sugawara et al 2003;Lisby et al 2004;San Filippo et al 2008). The single-stranded DNA (ssDNA)-binding protein, replication protein A (RPA), initially binds ssDNA that forms by nucleolytic processing of DNA ends at DSBs.…”

mentioning

confidence: 99%

Suppression of the Double-Strand-Break-Repair Defect of the Saccharomyces cerevisiae rad57 Mutant

Fung¹,

Mozlin²,

Symington

2009

Genetics

Self Cite

View full text Add to dashboard Cite

The Rad51 paralogs Rad55 and Rad57 form a heterodimer required to mediate the formation and/or stabilization of the Rad51 filament. To further characterize the function of Rad55-Rad57, we used a combination of rad57 partial suppressors to determine whether the DNA repair and recombination defects of the rad57 mutant could be completely suppressed. The combination of all suppressors, elevated temperature, srs2, rad51-I345T, and mating-type (MAT) heterozygosity resulted in almost complete suppression of the rad57 mutant defect in the recruitment of Rad51 to DNA-damaged sites, as well as survival in response to ionizing radiation and camptothecin. In a physical assay to monitor the kinetics of double-strand-break (DSB)-induced gene conversion, the rad57 mutant defect was effectively suppressed by srs2 and MAT heterozygosity, but these same suppressors failed to suppress the spontaneous recombination defect. Thus the Rad55-Rad57 heterodimer appears to have a unique function in spontaneous recombination that is not essential for DSB repair. Furthermore, we investigated the currently unknown mechanism of rad57 suppression by MAT heterozygosity and found that it is independent of DNL4. H OMOLOGOUS recombination is required forthe faithful repair of DNA double-strand breaks (DSBs) that arise during normal cellular processes or from exposure of cells to DNA-damaging agents. Central to the process of homologous recombination is the Rad51 protein, which facilitates synapsis and strand invasion into homologous duplex DNA (San Filippo et al. 2008). Rad51 belongs to the RecA family of homologous pairing proteins (Aboussekhra et al. 1992;Basile et al. 1992;Shinohara et al. 1992). Yeast and humans have two RecA homologs: Rad51 and the meiosis-specific Dmc1 (Bishop et al. 1992;San Filippo et al. 2008). In addition, the Saccharomyces cerevisiae RAD55 and RAD57 genes encode proteins with sequence similarity to RecA and Rad51 and are considered to be Rad51 paralogs (Kans and Mortimer 1991;Lovett 1994). Mutation of RAD51, RAD55, or RAD57 confers sensitivity of ionizing radiation (IR) and defects in mitotic and meiotic recombination, indicating that their functions are not redundant (Symington 2002). rad51 mutants generally exhibit more severe defects than rad55 or rad57 mutants in DSB-induced recombination assays; however, rad55 and rad57 mutants are more defective than rad51 in some assays that measure spontaneous recombination between repeated sequences (Rattray and Symington 1995;Mozlin et al. 2008).The molecular details of homologous recombination are largely based on genetic, physical, and cytological studies of DSB repair (DSBR) and on biochemical characterization of purified proteins (Paques and Haber 1999;Sugawara et al. 2003;Lisby et al. 2004;San Filippo et al. 2008). The single-stranded DNA (ssDNA)-binding protein, replication protein A (RPA), initially binds ssDNA that forms by nucleolytic processing of DNA ends at DSBs. In vitro, RPA has been shown to be inhibitory to Rad51 binding to ssDNA, but this inhibition c...

show abstract

Role of the Saccharomyces cerevisiae Rad51 Paralogs in Sister Chromatid Recombination

Cited by 64 publications

References 71 publications

XRCC2 and XRCC3 Regulate the Balance between Short- and Long-Tract Gene Conversions between Sister Chromatids

XRCC2 and XRCC3 Regulate the Balance between Short- and Long-Tract Gene Conversions between Sister Chromatids

Mitotic gene conversion events induced in G1-synchronized yeast cells by gamma rays are similar to spontaneous conversion events

Suppression of the Double-Strand-Break-Repair Defect of the Saccharomyces cerevisiae rad57 Mutant

Contact Info

Product

Resources

About