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DNA replication stress

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DNA replication stress refers to the cellular condition characterized by the slowing or stalling of DNA replication forks, which can lead to genomic instability, increased mutation rates, and potential cell death. It is often triggered by various factors, including DNA damage, nucleotide depletion, and the presence of DNA-binding proteins.
lightbulbAbout this topic
DNA replication stress refers to the cellular condition characterized by the slowing or stalling of DNA replication forks, which can lead to genomic instability, increased mutation rates, and potential cell death. It is often triggered by various factors, including DNA damage, nucleotide depletion, and the presence of DNA-binding proteins.
Modification with UFM1 (UFMylation) has recently emerged as a versatile signaling system regulating diverse cellular processes, from endoplasmic reticulum homeostasis to genome stability. Recent studies have expanded this landscape by... more
REV3, the catalytic subunit of translesion polymerase zeta (polζ), is commonly associated with DNA damage bypass and repair. Despite sharing accessory subunits with replicative polymerase δ, very little is known about the role of polζ in... more
Geminin, a DNA replication licensing inhibitor, ensures faithful DNA replication in vertebrates. Several studies have shown that Geminin depletion in vitro results in rereplication and DNA damage, while increased expression of Geminin has... more
Ethanol is a ubiquitous environmental stressor that is toxic to all lifeforms. Here, we use the model eukaryote Saccharomyces cerevisiae to show that exposure to sublethal ethanol concentrations causes DNA replication stress and an... more
POLθ promotes repair of DNA double-strand breaks (DSBs) resulting from collapsed forks in homologous recombination (HR) defective tumors. Inactivation of POLθ results in synthetic lethality with the loss of HR genes BRCA1/2, which induces... more
DNA replication timing (RT), reflecting the temporal order of origin activation, is known as a robust and conserved cell-type specific process. Upon low replication stress, the slowing of replication forks induces well-documented RT... more
Aneuploidy and overexpression of hsa-miR-155-5p (miR-155) characterize most solid and hematological malignancies. We recently demonstrated that miR-155 sustains aneuploidy at early stages of in vitro cellular transformation. During in... more
Key Points UBE2T is frequently amplified and/or overexpressed and is required for homologous recombination activity in multiple myeloma cells. UBE2T is a potential therapeutic target to increase chemosensitivity in multiple myeloma cells.
Ultraviolet (UV)-induced DNA damage causes an efficient block of elongating replication forks. The checkpoint kinase, CHK1 has been shown to stabilize replication forks following hydroxyurea treatment. Therefore, we wanted to test if the... more
The DNA damage response kinase ATR may be a useful cancer therapeutic target. ATR inhibition synergizes with loss of ERCC1, ATM, XRCC1 and DNA damaging chemotherapy agents. Clinical trials have begun using ATR inhibitors in combination... more
Histone modifications regulate gene expression and chromosomal events, yet how histonemodifying enzymes are targeted is poorly understood. Here we report that a conserved DNA repair protein, SMRC-1, associates with MET-2, the C. elegans... more
We previously reported high expression of RAD51 and increased homologous recombination (HR) rates in multiple myeloma (MM) cells, and showed that genomic instability and disease progression are commensurate with HR levels. Moreover, high... more
The causal role of aneuploidy in cancer initiation remains under debate since mutations of euploidy-controlling genes reduce cell fitness but aneuploidy strongly associates with human cancers. Telomerase activation allows immortal growth... more
Significance One origin of cancer arises from defects in the homologous recombination (HR) DNA repair pathway, which results in oncogenic genomic instability. Normal cells prefer HR for repair of stressed replication forks because it is... more
Ethanol is a ubiquitous environmental stressor that is toxic to all lifeforms. Here, we use the model eukaryote Saccharomyces cerevisiae to show that exposure to sublethal ethanol concentrations causes DNA replication stress and an... more
About 10% of cancer cells employ the "alternative lengthening of telomeres" (ALT) pathway instead of reactivating the hTERT subunit of human telomerase. The hTR RNA subunit is also abnormally silenced in some ALT + cells not expressing... more
The TP53 gene is a key tumor suppressor. Although the tumor suppressor p53 was one of the first to be characterized as a transcription factor, with its main function potentiated by its interaction with DNA, there are still many unresolved... more
Telomerase reverse transcriptase (TERT) and telomerase RNA component (TERC) constitute the core telomerase enzyme that maintains the length of telomeres. Telomere maintenance is affected in a broad range of cancer and degenerative... more
Leukemia cells rely on two nucleotide biosynthetic pathways, de novo and salvage, to produce dNTPs for DNA replication. Here, using metabolomic, proteomic, and phosphoproteomic approaches, we show that inhibition of the replication stress... more
Highlights  Whole-genome RNAi synthetic sickness/lethality screens were performed.  We identified synthetic sickness/lethality interaction of RRM1 with REV3.  HU and iREV3 treatments synergistically induce single-stranded DNA in... more