Gad8 Protein Is Found in the Nucleus Where It Interacts with the MluI Cell Cycle Box-binding Factor (MBF) Transcriptional Complex to Regulate the Response to DNA Replication Stress

Timely down-regulation of the evolutionarily conserved protein kinase Swe1 plays an important role in cell cycle control, as Swe1 can block nuclear division through inhibitory phosphorylation of the catalytic subunit of cyclin-dependent kinase. In particular, Swe1 degradation is important for budding yeast cell survival in case of DNA replication stress, whereas it is inhibited by the morphogenesis checkpoint in response to alterations in actin cytoskeleton or septin structure. We show that the lack of the Dma1 and Dma2 ubiquitin ligases, which moderately affects Swe1 localization and degradation during an unperturbed cell cycle with no apparent phenotypic effects, is toxic for cells that are partially defective in Swe1 down-regulation. Moreover, Swe1 is stabilized, restrained at the bud neck, and hyperphosphorylated in dma1Δ dma2Δ cells subjected to DNA replication stress, indicating that the mechanism stabilizing Swe1 under these conditions is different from the one triggered by the morphogenesis checkpoint. Finally, the Dma proteins are required for proper Swe1 ubiquitylation. Taken together, the data highlight a previously unknown role of these proteins in the complex regulation of Swe1 and suggest that they might contribute to control, directly or indirectly, Swe1 ubiquitylation.

Download Full-text

E2F1: Cause and Consequence of DNA Replication Stress

Frontiers in Molecular Biosciences ◽

10.3389/fmolb.2020.599332 ◽

2021 ◽

Vol 7 ◽

Author(s):

Shahd Fouad ◽

David Hauton ◽

Vincenzo D'Angiolella

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Tumor Suppressor ◽

Signaling Pathways ◽

Mammalian Cells ◽

Replication Stress ◽

Checkpoint Control ◽

Oncogenic Signaling ◽

Dna Replication Stress ◽

Oncogenic Signaling Pathways

In mammalian cells, cell cycle entry occurs in response to the correct stimuli and is promoted by the transcriptional activity of E2F family members. E2F proteins regulate the transcription of S phase cyclins and genes required for DNA replication, DNA repair, and apoptosis. The activity of E2F1, the archetypal and most heavily studied E2F family member, is tightly controlled by the DNA damage checkpoints to modulate cell cycle progression and initiate programmed cell death, when required. Altered tumor suppressor and oncogenic signaling pathways often result in direct or indirect interference with E2F1 regulation to ensure higher rates of cell proliferation independently of external cues. Despite a clear link between dysregulated E2F1 activity and cancer progression, literature on the contribution of E2F1 to DNA replication stress phenotypes is somewhat scarce. This review discusses how dysfunctional tumor suppressor and oncogenic signaling pathways promote the disruption of E2F1 transcription and hence of its transcriptional targets, and how such events have the potential to drive DNA replication stress. In addition to the involvement of E2F1 upstream of DNA replication stress, this manuscript also considers the role of E2F1 as a downstream effector of the response to this type of cellular stress. Lastly, the review introduces some reflections on how E2F1 activity is integrated with checkpoint control through post-translational regulation, and proposes an exploitable tumor weakness based on this axis.

Download Full-text

Protein phosphatase 2A (PP2A) promotes anaphase entry after DNA replication stress in budding yeast

Molecular Biology of the Cell ◽

10.1091/mbc.e21-04-0222 ◽

2021 ◽

Author(s):

Cory Haluska ◽

Fengzhi Jin ◽

Yanchang Wang

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Dna Synthesis ◽

Protein Phosphatase ◽

Budding Yeast ◽

Replication Stress ◽

S Phase ◽

Viability Loss ◽

Phosphatase 2A ◽

Dna Replication Stress

DNA replication stress activates the S-phase checkpoint that arrests the cell cycle, but it is poorly understood how cells recover from this arrest. Cyclin-dependent kinase (CDK) and Protein Phosphatase 2A (PP2A) are key cell cycle regulators, and Cdc55 is a regulatory subunit of PP2A in budding yeast. We found that yeast cells lacking functional PP2ACdc55 showed slow growth in the presence of hydroxyurea (HU), a DNA synthesis inhibitor, without obvious viability loss. Moreover, PP2A mutants exhibited delayed anaphase entry and sustained levels of anaphase inhibitor Pds1 after HU treatment. A DNA damage checkpoint Chk1 phosphorylates and stabilizes Pds1. We showed that chk1Δ and mutation of the Chk1 phosphorylation sites in Pds1 largely restored efficient anaphase entry in PP2A mutants after HU treatment. In addition, deletion of SWE1 that encodes the inhibitory kinase for CDK or mutation of the Swe1 phosphorylation site in CDK ( cdc28F19) also suppressed the anaphase entry delay in PP2A mutants after HU treatment. Our genetic data suggest that Swe1/CDK acts upstream of Pds1. Surprisingly, cdc55Δ showed significant suppression to the viability loss of S-phase checkpoint mutants during DNA synthesis block. Together, our results uncover a PP2A-Swe1-CDK-Chk1-Pds1 axis that promotes recovery from DNA replication stress.

Download Full-text

Centrosome impairment causes DNA replication stress through MLK3/MK2 signaling and R-loop formation

10.1101/2020.01.09.898684 ◽

2020 ◽

Author(s):

Zainab Tayeh ◽

Kim Stegmann ◽

Antonia Kleeberg ◽

Mascha Friedrich ◽

Josephine Ann Mun Yee Choo ◽

...

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Replication Stress ◽

List Type ◽

Replication Forks ◽

Loop Formation ◽

Animal Cells ◽

Replication Fork Progression ◽

Primordial Dwarfism ◽

Dna Replication Stress

AbstractCentrosomes function as organizing centers of microtubules and support accurate mitosis in many animal cells. However, it remains to be explored whether and how centrosomes also facilitate the progression through different phases of the cell cycle. Here we show that impairing the composition of centrosomes, by depletion of centrosomal components or by inhibition of polo-like kinase 4 (PLK4), reduces the progression of DNA replication forks. This occurs even when the cell cycle is arrested before damaging the centrosomes, thus excluding mitotic failure as the source of replication stress. Mechanistically, the kinase MLK3 associates with centrosomes. When centrosomes are disintegrated, MLK3 activates the kinases p38 and MK2/MAPKAPK2. Transcription-dependent RNA:DNA hybrids (R-loops) are then causing DNA replication stress. Fibroblasts from patients with microcephalic primordial dwarfism (Seckel syndrome) harbouring defective centrosomes showed replication stress and diminished proliferation, which were each alleviated by inhibition of MK2. Thus, centrosomes not only facilitate mitosis, but their integrity is also supportive in DNA replication.HighlightsCentrosome defects cause replication stress independent of mitosis.MLK3, p38 and MK2 (alias MAPKAPK2) are signalling between centrosome defects and DNA replication stress through R-loop formation.Patient-derived cells with defective centrosomes display replication stress, whereas inhibition of MK2 restores their DNA replication fork progression and proliferation.Graphical abstract

Download Full-text

DNA replication stress induces deregulation of the cell cycle events in root meristems of Allium cepa

Annals of Botany ◽

10.1093/aob/mcs215 ◽

2012 ◽

Vol 110 (8) ◽

pp. 1581-1591 ◽

Cited By ~ 12

Author(s):

Aneta Żabka ◽

Justyna Teresa Polit ◽

Janusz Maszewski

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Allium Cepa ◽

Replication Stress ◽

Root Meristems ◽

Dna Replication Stress

Download Full-text

Role of a Candida albicans Nrm1/Whi5 homologue in cell cycle gene expression and DNA replication stress response

Molecular Microbiology ◽

10.1111/j.1365-2958.2012.08056.x ◽

2012 ◽

Vol 84 (4) ◽

pp. 778-794 ◽

Cited By ~ 17

Author(s):

Ayala Ofir ◽

Kay Hofmann ◽

Esther Weindling ◽

Tsvia Gildor ◽

Katherine S. Barker ◽

...

Keyword(s):

Gene Expression ◽

Cell Cycle ◽

Candida Albicans ◽

Dna Replication ◽

Stress Response ◽

Replication Stress ◽

Cell Cycle Gene ◽

Dna Replication Stress ◽

Cell Cycle Gene Expression

Download Full-text

LIM Protein Ajuba associates with the RPA complex through direct and cell cycle-dependent interaction with the RPA70 subunit

10.1101/177840 ◽

2017 ◽

Author(s):

Sandy Fowler ◽

Pascal Maguin ◽

Sampada Kalan ◽

Diego Loayza

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Genome Stability ◽

Replication Stress ◽

Cellular Transformation ◽

Early Event ◽

Lim Protein ◽

Show Evidence ◽

Dna Replication Stress ◽

Cycle Dependent

AbstractDNA damage response pathways are essential for genome stability and cell survival. Specifically, the ATR kinase is activated by DNA replication stress. An early event in this activation is the recruitment and phosphorylation of RPA, a single stranded DNA binding complex composed of three subunits, RPA70,RPA32 and RPA14. We have previously shown that the LIM protein Ajuba associates with RPA, and that depletion of Ajuba leads to potent activation of ATR. In this study, we show evidence that the Ajuba-RPA interaction occurs through direct protein contact with RPA70, and that their association is cell cycle-regulated and is reduced upon DNA replication stress. We propose a model in which Ajuba negatively regulates the ATR pathway by directly interacting with RPA70, thereby preventing an inappropriate ATR activation. Our results provide a framework to understand the mechanism of regulation of ATR in human cells, which is important to prevent cellular transformation and tumorigenesis.

Download Full-text

The MluI Cell Cycle Box (MCB) Motifs, but Not Damage-Responsive Elements (DREs), Are Responsible for the Transcriptional Induction of the rhp51+ Gene in Response to DNA Replication Stress

PLoS ONE ◽

10.1371/journal.pone.0111936 ◽

2014 ◽

Vol 9 (11) ◽

pp. e111936 ◽

Cited By ~ 2

Author(s):

Wugangerile Sartagul ◽

Xin Zhou ◽

Yuki Yamada ◽

Ning Ma ◽

Katsunori Tanaka ◽

...

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Replication Stress ◽

Dna Replication Stress ◽

Transcriptional Induction

Download Full-text

Myosin 16 levels fluctuate during the cell cycle and are downregulated in response to DNA replication stress

Cytoskeleton ◽

10.1002/cm.21109 ◽

2013 ◽

Vol 70 (6) ◽

pp. 328-348 ◽

Cited By ~ 16

Author(s):

Richard S. Cameron ◽

Changdan Liu ◽

Jeanene P. S. Pihkala

Keyword(s):

Cell Cycle ◽

Dna Replication ◽

Replication Stress ◽

Dna Replication Stress

Download Full-text

The DNA Replication Stress Hypothesis of Alzheimer’s Disease

The Scientific World JOURNAL ◽

10.1100/2011/625690 ◽

2011 ◽

Vol 11 ◽

pp. 2602-2612 ◽

Cited By ~ 48

Author(s):

Yuri B. Yurov ◽

Svetlana G. Vorsanova ◽

Ivan Y. Iourov

Keyword(s):

Alzheimer’S Disease ◽

Cell Cycle ◽

Alzheimer's Disease ◽

Cell Death ◽

Dna Replication ◽

Cell Cycle Progression ◽

Neuronal Cell ◽

Replication Stress ◽

Mitotic Division ◽

Dna Replication Stress

A well-recognized theory of Alzheimer’s disease (AD) pathogenesis suggests ectopic cell cycle events to mediate neurodegeneration. Vulnerable neurons of the AD brain exhibit biomarkers of cell cycle progression and DNA replication suggesting a reentry into the cell cycle. Chromosome reduplication without proper cell cycle completion and mitotic division probably causes neuronal cell dysfunction and death. However, this theory seems to require some inputs in accordance with the generally recognized amyloid cascade theory as well as to explain causes and consequences of genomic instability (aneuploidy) in the AD brain. We propose that unscheduled and incomplete DNA replication (replication stress) destabilizes (epi)genomic landscape in the brain and leads to DNA replication “catastrophe” causing cell death during the S phase (replicative cell death). DNA replication stress can be a key element of the pathogenetic cascade explaining the interplay between ectopic cell cycle events and genetic instabilities in the AD brain. Abnormal cell cycle reentry and somatic genome variations can be used for updating the cell cycle theory introducing replication stress as a missing link between cell genetics and neurobiology of AD.

Download Full-text