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Reference - PMID:19546237 - TOR complex 2 controls gene silencing, telomere length maintenance, and survival under DNA-damaging conditions.

Reference summary

PubMed ID
PMID:19546237
Title
TOR complex 2 controls gene silencing, telomere length maintenance, and survival under DNA-damaging conditions.
Authors
Schonbrun M, Laor D, López-Maury L, Bähler J, Kupiec M, Weisman R
Citation
Mol Cell Biol 2009 Aug;29(16):4584-94
Publication year
2009
Abstract
The Target Of Rapamycin (TOR) kinase belongs to the highly conserved eukaryotic family of phosphatidylinositol-3-kinase-related kinases (PIKKs). TOR proteins are found at the core of two distinct evolutionarily conserved complexes, TORC1 and TORC2. Disruption of TORC1 or TORC2 results in characteristically dissimilar phenotypes. TORC1 is a major cell growth regulator, while the cellular roles of TORC2 are not well understood. In the fission yeast Schizosaccharomyces pombe, Tor1 is a component of the TORC2 complex, which is particularly required during starvation and various stress conditions. Our genome-wide gene expression analysis of Deltator1 mutants indicates an extensive similarity with chromatin structure mutants. Consistently, TORC2 regulates several chromatin-mediated functions, including gene silencing, telomere length maintenance, and tolerance to DNA damage. These novel cellular roles of TORC2 are rapamycin insensitive. Cells lacking Tor1 are highly sensitive to the DNA-damaging drugs hydroxyurea (HU) and methyl methanesulfonate, similar to mutants of the checkpoint kinase Rad3 (ATR). Unlike Rad3, Tor1 is not required for the cell cycle arrest in the presence of damaged DNA. Instead, Tor1 becomes essential for dephosphorylation and reactivation of the cyclin-dependent kinase Cdc2, thus allowing reentry into mitosis following recovery from DNA replication arrest. Taken together, our data highlight critical roles for TORC2 in chromatin metabolism and in promoting mitotic entry, most notably after recovery from DNA-damaging conditions. These data place TOR proteins in line with other PIKK members, such as ATM and ATR, as guardians of genome stability.

Annotation

GO biological process

GO:0010971 - positive regulation of G2/M transition of mitotic cell cycle

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Multi-locus phenotype

FYPO:0002019 - elongated telomeres during vegetative growth

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FYPO:0001122 - elongated vegetative cell

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FYPO:0001490 - inviable elongated vegetative cell

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FYPO:0002061 - inviable vegetative cell population

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FYPO:0000088 - sensitive to hydroxyurea

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FYPO:0000089 - sensitive to methyl methanesulfonate

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FYPO:0000091 - sensitive to thiabendazole

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FYPO:0002239 - shortened telomeres during vegetative growth

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FYPO:0003481 - viable elongated vegetative cell, elongated upon mitotic entry

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FYPO:0006822 - viable small vegetative cell with normal cell growth rate

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FYPO:0002060 - viable vegetative cell population

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Single locus phenotype

FYPO:0005189 - abnormal re-entry into mitotic cell cycle after arrest in response to hydroxyurea

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FYPO:0002827 - decreased chromatin silencing at silent mating-type cassette

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FYPO:0005187 - decreased level of transport gene mRNA during vegetative growth

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FYPO:0005188 - delayed onset of mitotic cell cycle arrest during cellular response to hydroxyurea

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FYPO:0002019 - elongated telomeres during vegetative growth

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FYPO:0005917 - increased subtelomeric heterochromatin RNA level

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FYPO:0004343 - increased wtf-derived RNA level

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FYPO:0000963 - normal growth on hydroxyurea

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FYPO:0000957 - normal growth on methyl methanesulfonate

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FYPO:0002899 - normal protein phosphorylation during cellular response to DNA damage

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FYPO:0002687 - normal telomere length during vegetative growth

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FYPO:0000088 - sensitive to hydroxyurea

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FYPO:0000089 - sensitive to methyl methanesulfonate

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FYPO:0000091 - sensitive to thiabendazole

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FYPO:0000268 - sensitive to UV during vegetative growth

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FYPO:0002239 - shortened telomeres during vegetative growth

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FYPO:0003481 - viable elongated vegetative cell, elongated upon mitotic entry

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FYPO:0006822 - viable small vegetative cell with normal cell growth rate

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