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Reference - PMID:34608864 - DDK/Hsk1 phosphorylates and targets fission yeast histone deacetylase Hst4 for degradation to stabilize stalled DNA replication forks.

Reference summary

PubMed ID
PMID:34608864
Title
DDK/Hsk1 phosphorylates and targets fission yeast histone deacetylase Hst4 for degradation to stabilize stalled DNA replication forks.
Authors
Aricthota S, Haldar D
Citation
Elife 2021 Oct 05;10
Publication year
2021
Abstract
In eukaryotes, paused replication forks are prone to collapse, which leads to genomic instability, a hallmark of cancer. Dbf4-dependent kinase (DDK)/Hsk1 Cdc7 is a conserved replication initiator kinase with conflicting roles in replication stress response. Here, we show that fission yeast DDK/Hsk1 phosphorylates sirtuin, Hst4 upon replication stress at C-terminal serine residues. Phosphorylation of Hst4 by DDK marks it for degradation via the ubiquitin ligase SCF pof3 . Phosphorylation-defective hst4 mutant ( 4SA-hst4 ) displays defective recovery from replication stress, faulty fork restart, slow S-phase progression and decreased viability. The highly conserved fork protection complex (FPC) stabilizes stalled replication forks. We found that the recruitment of FPC components, Swi1 and Mcl1 to the chromatin is compromised in the 4SA-hst4 mutant, although whole cell levels increased. These defects are dependent upon H3K56ac and independent of intra S-phase checkpoint activation. Finally, we show conservation of H3K56ac-dependent regulation of Timeless, Tipin, and And-1 in human cells. We propose that degradation of Hst4 via DDK increases H3K56ac, changing the chromatin state in the vicinity of stalled forks facilitating recruitment and function of FPC. Overall, this study identified a crucial role of DDK and FPC in the regulation of replication stress response with implications in cancer therapeutics.

Annotation

GO molecular function

GO:0004674 - protein serine/threonine kinase activity

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Modification

MOD:00046 - O-phospho-L-serine

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MOD:01148 - ubiquitinylated lysine

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Multi-locus phenotype

FYPO:0002061 - inviable vegetative cell population

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Qualitative gene expression

PomGeneEx:0000019 - protein level decreased

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PomGeneEx:0000013 - RNA level unchanged

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Single locus phenotype

FYPO:0005268 - abnormal mitotic cell cycle regulation during cellular response to methyl methanesulfonate

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FYPO:0007879 - abolished protein degradation during cellular response to methyl methanesulfonate

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FYPO:0004660 - abolished protein phosphorylation during cellular response to methyl methanesulfonate

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FYPO:0000912 - abolished protein ubiquitination during vegetative growth

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FYPO:0004240 - decreased histone H3-K56 acetylation during vegetative growth

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FYPO:0007878 - decreased protein degradation during cellular response to methyl methanesulfonate

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FYPO:0002909 - decreased protein localization to chromatin during vegetative growth

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FYPO:0007255 - decreased replication fork processing

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FYPO:0001355 - decreased vegetative cell population growth

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FYPO:0007881 - increased duration of histone H2A phosphorylation during cellular response to methyl methanesulfonate

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FYPO:0000614 - increased duration of mitotic S phase

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FYPO:0004189 - increased protein level during cellular response to hydroxyurea

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FYPO:0001327 - increased protein level during vegetative growth

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FYPO:0000957 - normal growth on methyl methanesulfonate

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FYPO:0007880 - normal protein degradation during cellular response to methyl methanesulfonate

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FYPO:0007882 - normal protein kinase activity during cellular response to methyl methanesulfonate

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FYPO:0000838 - normal protein localization to nucleus during vegetative growth

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FYPO:0001357 - normal vegetative cell population growth

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FYPO:0000088 - sensitive to hydroxyurea

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FYPO:0000089 - sensitive to methyl methanesulfonate

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