A Balance between Tel1 and Rif2 Activities Regulates Nucleolytic Processing and Elongation at Telomeres

Martina, Marina; Clerici, Michela; Baldo, Veronica; Bonetti, Diego; Lucchini, Giovanna; Longhese, Maria Pia

doi:10.1128/mcb.06547-11

Cited by 41 publications

(61 citation statements)

References 52 publications

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“…9a). Although we cannot rule out that SAE2 and RIF2 deletions have additive independent effects, this result is in line with the role of Rif2 in regulating the function of MRX/Sae2 in resection 60 . In this case, premature senescence of the rif2D sae2D est2D triple mutant as compared with the sae2D est2D double mutant would suggest that Sae2 is not the only activity inhibited by Rif2.…”

Section: Nature Communications | Doimentioning

confidence: 50%

Sgs1 and Sae2 promote telomere replication by limiting accumulation of ssDNA

et al. 2014

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In budding yeast, DNA ends are processed by the consecutive action of MRX/Sae2 and two redundant pathways dependent on Sgs1/Dna2 and Exo1, and this processing is counteracted by Ku heterodimer. Here we show that DNA end resection by Sae2 and Sgs1 is dispensable for normal telomere maintenance by telomerase. Instead, these proteins facilitate telomere replication and limit the accumulation of single-strand DNA (ssDNA) at replication fork pause sites. Loss of Sae2 and Sgs1 drives selection for compensatory mutations, notably in Ku, which are responsible for abrupt telomere shortening in cells lacking Sae2 and Sgs1. In telomerase-negative cells, Sae2 and Sgs1 play non-overlapping roles in generating ssDNA at eroded telomeres and are required for the formation of type II survivors. Thus, although their primary function in telomerase-positive cells is to sustain DNA replication over the sites that are prone to fork pausing, Sae2 and Sgs1 contribute to telomere resection in telomerase-deficient cells.

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Section: Nature Communications | Doimentioning

confidence: 50%

Sgs1 and Sae2 promote telomere replication by limiting accumulation of ssDNA

et al. 2014

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“…In S. cerevisiae , MRX is known to interact with Rif2, which is recruited to telomeric DNA ends by Rap1 and negatively regulates telomerase action 39404142. Rif2 was recently found to be recruited also to intrachromosomal DSBs in a manner partially dependent on MRX 43.…”

Section: Functional Dynamics Of the Mrx Complexmentioning

confidence: 99%

Functions and regulation of the MRX complex at DNA double-strand breaks

Gobbini¹,

Cassani²,

Villa³

et al. 2016

Microbial Cell

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DNA double-strand breaks (DSBs) pose a serious threat to genome stability and cell survival. Cells possess mechanisms that recognize DSBs and promote their repair through either homologous recombination (HR) or non-homologous end joining (NHEJ). The evolutionarily conserved Mre11-Rad50-Xrs2 (MRX) complex plays a central role in the cellular response to DSBs, as it is implicated in controlling end resection and in maintaining the DSB ends tethered to each other. Furthermore, it is responsible for DSB signaling by activating the checkpoint kinase Tel1 that, in turn, supports MRX function in a positive feedback loop. The present review focuses mainly on recent works in the budding yeast Saccharomyces cerevisiae to highlight structure and regulation of MRX as well as its interplays with Tel1.

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“…MRX/ MRN is the major responsible for the generation of the G-tail at telomeres, where its activity is stimulated by the PIKK kinase Tel1. 88 Indeed, mrx mutants are defective in G-tail formation in a de novo telomere addition reaction; 89,90 moreover, both mrx mutants and MRN-depleted cells exhibit shorter G-tails. 91,92 Further investigations indicated that MRX and Sae2 act together in the processing the C-strand, even though MRX may give a chromatin remodeler belonging to the Etl1 Snf2 family.…”

Section: Resection In the Telomeric Contextmentioning

confidence: 99%

To trim or not to trim: Progression and control of DSB end resection

Granata

Panigada²,

Galati³

et al. 2013

Cell Cycle

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RepoRt 1848Cell Cycle Volume 12 Issue 12 D NA double-strand breaks (DSBs) are the most cytotoxic form of DNA damage, since they can lead to genome instability and chromosome rearrangements, which are hallmarks of cancer cells. To face this kind of lesion, eukaryotic cells developed two alternative repair pathways, homologous recombination (HR) and non-homologous end joining (NHEJ). Repair pathway choice is influenced by the cell cycle phase and depends upon the 5'-3' nucleolytic processing of the break ends, since the generation of ssDNA tails strongly stimulates HR and inhibits NHEJ. A large amount of work has elucidated the key components of the DSBs repair machinery and how this crucial process is finely regulated. The emerging view suggests that besides endo/exonucleases and helicases activities required for end resection, molecular barrier factors are specifically loaded in the proximity of the break, where they physically or functionally limit DNA degradation, preventing excessive accumulation of ssDNA, which could be threatening for cell survival.

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A Balance between Tel1 and Rif2 Activities Regulates Nucleolytic Processing and Elongation at Telomeres

Cited by 41 publications

References 52 publications

Sgs1 and Sae2 promote telomere replication by limiting accumulation of ssDNA

Sgs1 and Sae2 promote telomere replication by limiting accumulation of ssDNA

Functions and regulation of the MRX complex at DNA double-strand breaks

To trim or not to trim: Progression and control of DSB end resection

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