A ‘DNA replication’ signature of progression and negative outcome in colorectal cancer

Pillaire, Mj; Sèlves, Janick; Gordien, K.; Gouraud, Pierre-Antoine; Gentil, Catherine; Danjoux, Marie; Do, Catherine; Nègre, Vincent; Bieth, Anne; Guimbaud, Rosine; Trouche, Didier; Pasero, Philippe; Méchali, Marcel; Hoffmann, Jean-Sébastien; Cazaux, Christophe

doi:10.1038/onc.2009.378

Cited by 98 publications

(99 citation statements)

References 43 publications

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“…This novel Pol y function may be particularly important within the context of cancer, as high POLQ expression is strongly associated with poor clinical outcome of patients with colon, breast and lung cancers [22][23][24]55,56 . Abnormal temporal control of replication, recently demonstrated in several haematologic malignancies, has been proposed to represent a common mechanism responsible for genomic instability found in cancer cells 57 ; therefore, Pol y overexpression may be of cardinal importance in defining the modified temporal replication programme in cancer cells and may constitute a driving force for chromosomal instability [58][59][60] .…”

Section: Discussionmentioning

confidence: 98%

“…By conducting large-scale studies of the expression of DNA replication factors in patients with colon, breast and lung cancer, we recently uncovered major alterations in the expression pattern of POLQ, the gene encoding Pol y, and discovered that excess POLQ correlates with genetic instability and poor prognosis [22][23][24] . This is, to our knowledge, the strongest link between a negative clinical outcome and the expression of a DNA polymerase 25 .…”

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confidence: 99%

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A role for DNA polymerase θ in the timing of DNA replication

et al. 2014

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Although DNA polymerase θ (Pol θ) is known to carry out translesion synthesis and has been implicated in DNA repair, its physiological function under normal growth conditions remains unclear. Here we present evidence that Pol θ plays a role in determining the timing of replication in human cells. We find that Pol θ binds to chromatin during early G1, interacts with the Orc2 and Orc4 components of the Origin recognition complex and that the association of Mcm proteins with chromatin is enhanced in G1 when Pol θ is downregulated. Pol θ-depleted cells exhibit a normal density of activated origins in S phase, but early-to-late and late-to-early shifts are observed at a number of replication domains. Pol θ overexpression, on the other hand, causes delayed replication. Our results therefore suggest that Pol θ functions during the earliest steps of DNA replication and influences the timing of replication initiation.

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Section: Discussionmentioning

confidence: 98%

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confidence: 99%

A role for DNA polymerase θ in the timing of DNA replication

et al. 2014

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“…MCM7 has been reported to be upregulated in many types of cancer and functions as oncogene in muscle- invasive bladder cancer (22), non-small cell lung cancer (23,24), Hodgkin lymphoma (25), prostate cancer (15), liver cancer (26), meningiomas (27), colorectal cancer (28,29), medulloblastoma (30) and oral squamous cell carcinoma (31). By siRNA-mediated knockdown of MCM7 in GAC cell lines, the cell proliferation and invasion were inhibited, thus MCM7 knockdown exerts anti-oncogenic effect in vitro.…”

Section: Discussionmentioning

confidence: 99%

MCM7 serves as a prognostic marker in diffuse-type gastric adenocarcinoma and siRNA-mediated knockdown suppresses its oncogenic function

et al. 2014

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Abstract. MCM7 (mini-chromosome maintenance protein 7) is essential for the initiation of genomic replication as a component of the pre-replication complex. The present study aimed to analyze its expression, clinical significance and biological functions in gastric adenocarcinoma (GAC). The MCM7 protein was upregulated in all 9 GAC cell lines. In 6 paired primary GACs, MCM7 was upregulated in tumor compared with the corresponding non-tumorous gastric tissues. In normal gastric epithelium tissue, MCM7 was strictly expressed in the proliferative compartment. MCM7 knockdown by siRNA in gastric cancer cell line AGS and NCI-N87 significantly suppressed cell proliferation, inhibited monolayer colony formation, reduced cell invasion and induced late apoptosis. Its nuclear expression correlated with advanced age and poorer disease specific survival in diffuse-type GACs. All the findings supported that MCM7 might play an oncogenic role in gastric tumorigenesis. It serves as a potential prognostic marker and therapeutic target in diffuse-type GACs.

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“…Determining how these bacterial enzymes are regulated will allow a better description of the regulation of TLS polymerase activity in other systems. Furthermore, TLS polymerases have been implicated in the evolution of antibiotic resistance in bacteria and cancer in humans (24)(25)(26)(27). Deregulation of TLS polymerases, therefore, has a variety of deleterious consequences in both prokaryotic and eukaryotic organisms.…”

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confidence: 99%

A Single Residue Unique to DinB-Like Proteins Limits Formation of the Polymerase IV Multiprotein Complex in Escherichia coli

Cafarelli¹,

Rands²,

Benson³

et al. 2013

Journal of Bacteriology

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The activity of DinB is governed by the formation of a multiprotein complex (MPC) with RecA and UmuD. We identified two highly conserved surface residues in DinB, cysteine 66 (C66) and proline 67 (P67). Mapping on the DinB tertiary structure suggests these are noncatalytic, and multiple-sequence alignments indicate that they are unique among DinB-like proteins. To investigate the role of the C66-containing surface in MPC formation, we constructed the dinB(C66A) derivative. We found that DinB(C66A) copurifies with its interacting partners, RecA and UmuD, to a greater extent than DinB. Notably, copurification of RecA with DinB is somewhat enhanced in the absence of UmuD and is further increased for DinB(C66A). In vitro pulldown assays also indicate that DinB(C66A) binds RecA and UmuD better than DinB. We note that the increased affinity of DinB(C66A) for UmuD is RecA dependent. Thus, the C66-containing binding surface appears to be critical to modulate interaction with UmuD, and particularly with RecA. Expression of dinB(C66A) from the chromosome resulted in detectable differences in dinBdependent lesion bypass fidelity and homologous recombination. Study of this DinB derivative has revealed a key surface on DinB, which appears to modulate the strength of MPC binding, and has suggested a binding order of RecA and UmuD to DinB. These findings will ultimately permit the manipulation of these enzymes to deter bacterial antibiotic resistance acquisition and to gain insights into cancer development in humans.

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A ‘DNA replication’ signature of progression and negative outcome in colorectal cancer

Cited by 98 publications

References 43 publications

A role for DNA polymerase θ in the timing of DNA replication

A role for DNA polymerase θ in the timing of DNA replication

MCM7 serves as a prognostic marker in diffuse-type gastric adenocarcinoma and siRNA-mediated knockdown suppresses its oncogenic function

A Single Residue Unique to DinB-Like Proteins Limits Formation of the Polymerase IV Multiprotein Complex in Escherichia coli

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