Mcm2-7 Is an Active Player in the DNA Replication Checkpoint Signaling Cascade via Proposed Modulation of Its DNA Gate

Tsai, Feng-Ling; Vijayraghavan, Sriram; Prinz, Joseph A.; MacAlpine, Heather K.; MacAlpine, David M.; Schwacha, Anthony

doi:10.1128/mcb.01357-14

Cited by 15 publications

(31 citation statements)

References 75 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…e ., HU treatment) [25]. Here, we provide evidence that this mutant is also involved in modulating DNA replication during unchallenged growth, and exhibits unusual replication-dependent DNA damage that is likely linked to an increased frequency of both apoptotic cell death and spontaneous genome rearrangement under this condition.…”

Section: Discussionmentioning

confidence: 75%

A Checkpoint-Related Function of the MCM Replicative Helicase Is Required to Avert Accumulation of RNA:DNA Hybrids during S-phase and Ensuing DSBs during G2/M

2016

Self Cite

View full text Add to dashboard Cite

The Mcm2-7 complex is the catalytic core of the eukaryotic replicative helicase. Here, we identify a new role for this complex in maintaining genome integrity. Using both genetic and cytological approaches, we find that a specific mcm allele (mcm2DENQ) causes elevated genome instability that correlates with the appearance of numerous DNA-damage associated foci of γH2AX and Rad52. We further find that the triggering events for this genome instability are elevated levels of RNA:DNA hybrids and an altered DNA topological state, as over-expression of either RNaseH (an enzyme specific for degradation of RNA in RNA:DNA hybrids) or Topoisomerase 1 (an enzyme that relieves DNA supercoiling) can suppress the mcm2DENQ DNA-damage phenotype. Moreover, the observed DNA damage has several additional unusual properties, in that DNA damage foci appear only after S-phase, in G2/M, and are dependent upon progression into metaphase. In addition, we show that the resultant DNA damage is not due to spontaneous S-phase fork collapse. In total, these unusual mcm2DENQ phenotypes are markedly similar to those of a special previously-studied allele of the checkpoint sensor kinase ATR/MEC1, suggesting a possible regulatory interplay between Mcm2-7 and ATR during unchallenged growth. As RNA:DNA hybrids primarily result from transcription perturbations, we suggest that surveillance-mediated modulation of the Mcm2-7 activity plays an important role in preventing catastrophic conflicts between replication forks and transcription complexes. Possible relationships among these effects and the recently discovered role of Mcm2-7 in the DNA replication checkpoint induced by HU treatment are discussed.

show abstract

Section: Discussionmentioning

confidence: 75%

A Checkpoint-Related Function of the MCM Replicative Helicase Is Required to Avert Accumulation of RNA:DNA Hybrids during S-phase and Ensuing DSBs during G2/M

2016

Self Cite

View full text Add to dashboard Cite

show abstract

“…On average 1,700 proteins per sample (1,296–2,189) were identified. Interestingly, levels of members of the Minichromosome Maintenance (MCM) family ( MCM2 , MCM3 , MCM4 , MCM5 , MCM6 , MCM7 ) [ 23 , 24 ] were found to be highly significantly increased in cervical cancer tissue from early and late stage patients as compared to healthy tissue. A volcano plot illustrates the difference in abundance of proteins in the comparison of both early stage and late stage cervical cancer with the healthy epithelium (Figure 1A and 1B ).…”

Section: Resultsmentioning

confidence: 99%

Proteomic alterations in early stage cervical cancer

et al. 2018

View full text Add to dashboard Cite

Laser capture microdissection (LCM) allows the capture of cell types or well-defined structures in tissue. We compared in a semi-quantitative way the proteomes from an equivalent of 8,000 tumor cells from patients with squamous cell cervical cancer (SCC, n = 22) with healthy epithelial and stromal cells obtained from normal cervical tissue (n = 13). Proteins were enzymatically digested into peptides which were measured by high-resolution mass spectrometry and analyzed by “all-or-nothing” analysis, Bonferroni, and Benjamini-Hochberg correction for multiple testing. By comparing LCM cell type preparations, 31 proteins were exclusively found in early stage cervical cancer (n = 11) when compared with healthy epithelium and stroma, based on criteria that address specificity in a restrictive “all-or-nothing” way. By Bonferroni correction for multiple testing, 30 proteins were significantly up-regulated between early stage cervical cancer and healthy control, including six members of the MCM protein family. MCM proteins are involved in DNA repair and expected to be participating in the early stage of cancer. After a less stringent Benjamini-Hochberg correction for multiple testing, we found that the abundances of 319 proteins were significantly different between early stage cervical cancer and healthy controls. Four proteins were confirmed in digests of whole tissue lysates by Parallel Reaction Monitoring (PRM). Ingenuity Pathway Analysis using correction for multiple testing by permutation resulted in two networks that were differentially regulated in early stage cervical cancer compared with healthy tissue. From these networks, we learned that specific tumor mechanisms become effective during the early stage of cervical cancer.

show abstract

“…For randomized elements, the randomization was repeated 1000 times and the median and [0.01,0.99] percentile interval are shown (red bar). e-f. ECDF of the distance between sporadic (red), clustered (green) and randomly shuffled (black) initiation events, and the center of the closest ORC [25] (e) or Mcm2-7 [27] (f) binding site.…”

Section: Characterisation Of the Sporadic Initiation Eventsmentioning

confidence: 99%

FORK-seq: replication landscape of theSaccharomyces cerevisiaegenome by nanopore sequencing

Hennion

Arbona

Lacroix

et al. 2020

Preprint

View full text Add to dashboard Cite

Genome replication mapping methods profile cell populations, masking cell-tocell heterogeneity. Here, we describe FORK-seq, a nanopore sequencing method to map replication of single DNA molecules at 200 nucleotide resolution. By quantifying BrdU incorporation along pulse-chased replication intermediates from Saccharomyces cerevisiae, we orient 58,651 replication tracks reproducing populationbased replication directionality profiles and map 4,964 and 4,485 individual initiation and termination events, respectively. Although most events cluster at known origins and fork merging zones, 9% and 18% of initiation and termination events, respectively, occur at many locations previously missed. Thus, FORK-seq reveals the full extent of cell-to-cell heterogeneity in DNA replication.

show abstract

Mcm2-7 Is an Active Player in the DNA Replication Checkpoint Signaling Cascade via Proposed Modulation of Its DNA Gate

Cited by 15 publications

References 75 publications

A Checkpoint-Related Function of the MCM Replicative Helicase Is Required to Avert Accumulation of RNA:DNA Hybrids during S-phase and Ensuing DSBs during G2/M

A Checkpoint-Related Function of the MCM Replicative Helicase Is Required to Avert Accumulation of RNA:DNA Hybrids during S-phase and Ensuing DSBs during G2/M

Proteomic alterations in early stage cervical cancer

FORK-seq: replication landscape of theSaccharomyces cerevisiaegenome by nanopore sequencing

Contact Info

Product

Resources

About