Hpz1 Modulates the G1-S Transition in Fission Yeast

Bøe, Cathrine Arnason; Knutsen, Jon Halvor Jonsrud; Boye, Erik; Grallert, Beáta

doi:10.1371/journal.pone.0044539

Cited by 1 publication

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References 56 publications

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“…We recently identified Hpz1 in fission yeast as a potential functional partner of Rad3, which is the fission yeast homologue of ATR 21 . Interestingly we found no evidence for Hpz1 participating in the checkpoint functions of Rad3.…”

Section: Introductionmentioning

confidence: 99%

A novel role for ATR/Rad3 in G1 phase

Bøe

Håland

Boye

et al. 2018

Sci Rep

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Checkpoint kinases are important in cellular surveillance pathways that help cells to cope with DNA damage and protect their genomes. In cycling cells, DNA replication is one of the most sensitive processes and therefore all organisms carefully regulate replication initiation and progression. The checkpoint kinase ATR plays important roles both in response to DNA damage and replication stress, and ATR inhibitors are currently in clinical trials for cancer treatment. Therefore, it is important to understand the roles of ATR in detail. Here we show that the fission yeast homologue Rad3 and the human ATR regulate events also in G1 phase in an unperturbed cell cycle. Rad3Δ mutants or human cells exposed to ATR inhibitor in G1 enter S phase prematurely, which results in increased DNA damage. Furthermore, ATR inhibition in a single G1 reduces clonogenic survival, demonstrating that long-term effects of ATR inhibition during G1 are deleterious for the cell. Interestingly, ATR inhibition through G1 and S phase reduces survival in an additive manner, strongly arguing that different functions of ATR are targeted in the different cell-cycle phases. We propose that potential effects of ATR inhibitors in G1 should be considered when designing future treatment protocols with such inhibitors.

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Section: Introductionmentioning

confidence: 99%