2008
DOI: 10.1016/j.abb.2007.11.001
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Interacting proteins Rtt109 and Vps75 affect the efficiency of non-homologous end-joining in Saccharomyces cerevisiae

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Cited by 45 publications
(62 citation statements)
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“…To identify the genes related to the NHEJ pathway, we used an established in vitro plasmid-based DSB repair assay (12) in which the linearized p416 plasmid containing the URA3 selection marker was introduced into a yeast array of target single-gene deletion mutants. The plasmid cleavage site (i.e., an induced DSB) was contained in a region with no homologous sequence available in the genome to repair (Fig.…”
Section: Resultsmentioning
confidence: 99%
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“…To identify the genes related to the NHEJ pathway, we used an established in vitro plasmid-based DSB repair assay (12) in which the linearized p416 plasmid containing the URA3 selection marker was introduced into a yeast array of target single-gene deletion mutants. The plasmid cleavage site (i.e., an induced DSB) was contained in a region with no homologous sequence available in the genome to repair (Fig.…”
Section: Resultsmentioning
confidence: 99%
“…The efficiencies of chromosomal DSBs in yeast for the selected set of strains derived from JKM139 were assayed essentially as described elsewhere (12). Briefly, overnight cultures of wild-type or mutant strains were grown in fresh YPD or YP-raffinose (1% yeast extract, 2% Bacto peptone, 2% raffinose) at 30°C to an optical density at 600 nm (OD 600 ) of ϳ0.5.…”
Section: Methodsmentioning
confidence: 99%
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“…Recent reports also indicate that modulation of H3 K56 acetylation can lead to defects in silencing (Hyland et al 2005;Xu et al 2007), suggesting that ASF1-dependent silencing phenotypes may be related to acetylation of K56 on histone H3 in addition to acetylation of K16 on histone H4. In addition, work from several groups has led to the identification of a pathway involving H3 K56 acetylation, RTT109, and ASF1 in maintaining genome integrity in response to DNA damage (Masumoto et al 2005;Ozdemir et al 2005;Celic et al 2006;Maas et al 2006;Recht et al 2006;Schneider et al 2006;Agez et al 2007;Driscoll et al 2007;Han et al 2007a,b,c;Tsubota et al 2007;Jessulat et al 2008). The findings that (1) acetylation of K56 on histone H3 affects DNA damage sensitivity and silencing, (2) a DNA-damaging agent prevents silent chromatin formation (Kirchmaier and Rine 2006;see also Miller and Nasmyth 1984;Fox et al 1997), and (3) checkpoint activation in response to DNA damage alters Sir localization and silencing (Martin et al 1999;McAinsh et al 1999;Mills et al 1999;Sharp et al 2005) have motivated us to explore the relationship between histone modification, silencing, DNA replication, and responses to DNA damage.…”
mentioning
confidence: 99%
“…Calculation of genetic distance and genetic congruence. Growth-based genetic interactions were measured using a modified BioGRID database derived from version 2.0.60 (51), including the interaction categories "synthetic lethality," "synthetic growth defect," and "haploinsufficiency," as well as "phenotypic enhancement" data specifically derived from E-MAP studies (52)(53)(54)(55). We also added 8,102 and 191,890 E-MAP interactions from additional studies published during the course of this analysis (56,57).…”
Section: Methodsmentioning
confidence: 99%