68 results on '"P., Canitrot"'
Search Results
2. Left anterior descending myocardial bridge: Angiographic prevalence and its association to atherosclerosis
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Anthony Matta, Ronan Canitrot, Vanessa Nader, Stephanie Blanco, Francesco Campelo-Parada, Frederic Bouisset, Thibault Lhermusier, Meyer Elbaz, Didier Carrie, and Jerome Roncalli
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Myocardial bridge ,Left anterior descending coronary artery ,Atherosclerosis ,MINOCA ,Surgery ,RD1-811 ,Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Objective: Left anterior descending Myocardial Bridge (LADMB) is considered a benign condition and actually becomes a forgotten cause of serious cardiac events. This study was conducted to estimate the prevalence of LADMB and its association to atherosclerosis. Methods: An observational retrospective study was conducted on patients referred for coronary angiography between June 2012 and June 2020. Coronary angiography database was revisedand studied population was divided into 2 groups: LADMB group versus Non-LADMB group. Results: LADMB was detected in 510 patients out of 35813 included in the study resulting in a prevalence at 1.42%. The mean age was 66.5 years. Male gender was more common than female (70vs30%). The prevalence of significant atherosclerotic LAD disease was more than two times higher in the non-LADMB group compared to the LADMB group. Statistical analysis revealed a significant negative association between LADMB and atherosclerosis (p
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- 2021
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3. Surfing the clinical trials of mesenchymal stem cell therapy in ischemic cardiomyopathy
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Iman Razeghian-Jahromi, Anthony G. Matta, Ronan Canitrot, Mohammad Javad Zibaeenezhad, Mahboobeh Razmkhah, Anahid Safari, Vanessa Nader, and Jerome Roncalli
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Mesenchymal stem cells ,Ischemic cardiomyopathy ,Clinical trials ,Medicine (General) ,R5-920 ,Biochemistry ,QD415-436 - Abstract
Abstract While existing remedies failed to fully address the consequences of heart failure, stem cell therapy has been introduced as a promising approach. The present review is a comprehensive appraisal of the impacts of using mesenchymal stem cells (MSCs) in clinical trials mainly conducted on ischemic cardiomyopathy. The benefits of MSC therapy for dysfunctional myocardium are likely attributed to numerous secreted paracrine factors and immunomodulatory effects. The positive outcomes associated with MSC therapy are scar size reduction, reverse remodeling, and angiogenesis. Also, a decreasing in the level of chronic inflammatory markers of heart failure progression like TNF-α is observed. The intense inflammatory reaction in the injured myocardial micro-environment predicts a poor response of scar tissue to MSC therapy. Subsequently, the interval delay between myocardial injury and MSC therapy is not yet determined. The optimal requested dose of cells ranges between 100 to 150 million cells. Allogenic MSCs have different advantages compared to autogenic cells and intra-myocardial injection is the preferred delivery route. The safety and efficacy of MSCs-based therapy have been confirmed in numerous studies, however several undefined parameters like route of administration, optimal timing, source of stem cells, and necessary dose are limiting the routine use of MSCs therapeutic approach in clinical practice. Lastly, pre-conditioning of MSCs and using of exosomes mediated MSCs or genetically modified MSCs may improve the overall therapeutic effect. Future prospective studies establishing a constant procedure for MSCs transplantation are required in order to apply MSC therapy in our daily clinical practice and subsequently improving the overall prognosis of ischemic heart failure patients.
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- 2021
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4. Model-Based and Model-Free Replay Mechanisms for Reinforcement Learning in Neurorobotics
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Elisa Massi, Jeanne Barthélemy, Juliane Mailly, Rémi Dromnelle, Julien Canitrot, Esther Poniatowski, Benoît Girard, and Mehdi Khamassi
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hippocampal replay ,reinforcement learning ,neurorobotics ,model-based ,model-free ,Neurosciences. Biological psychiatry. Neuropsychiatry ,RC321-571 - Abstract
Experience replay is widely used in AI to bootstrap reinforcement learning (RL) by enabling an agent to remember and reuse past experiences. Classical techniques include shuffled-, reversed-ordered- and prioritized-memory buffers, which have different properties and advantages depending on the nature of the data and problem. Interestingly, recent computational neuroscience work has shown that these techniques are relevant to model hippocampal reactivations recorded during rodent navigation. Nevertheless, the brain mechanisms for orchestrating hippocampal replay are still unclear. In this paper, we present recent neurorobotics research aiming to endow a navigating robot with a neuro-inspired RL architecture (including different learning strategies, such as model-based (MB) and model-free (MF), and different replay techniques). We illustrate through a series of numerical simulations how the specificities of robotic experimentation (e.g., autonomous state decomposition by the robot, noisy perception, state transition uncertainty, non-stationarity) can shed new lights on which replay techniques turn out to be more efficient in different situations. Finally, we close the loop by raising new hypotheses for neuroscience from such robotic models of hippocampal replay.
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- 2022
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5. Surfing the clinical trials of mesenchymal stem cell therapy in ischemic cardiomyopathy
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Razeghian-Jahromi, Iman, Matta, Anthony G., Canitrot, Ronan, Zibaeenezhad, Mohammad Javad, Razmkhah, Mahboobeh, Safari, Anahid, Nader, Vanessa, and Roncalli, Jerome
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- 2021
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6. Impact of Coronary Artery Disease and Percutaneous Coronary Intervention on Transcatheter Aortic Valve Implantation
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Anthony G. Matta, Thibault Lhermusier, Francisco Campelo Parada, Frederic Bouisset, Ronan Canitrot, Vanessa Nader, Stéphanie Blanco, Meyer Elbaz, Jerome Roncalli, and Didier Carrié
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Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Introduction. The prevalence of coronary artery disease (CAD) detected in preoperative work-up for transcatheter aortic valve implantation (TAVI) is high. Instead, the management of a concomitant CAD remains unclear. We evaluate the impact of CAD and percutaneous coronary intervention (PCI) on TAVI procedures. Materials and Methods. A retrospective study was conducted on 1336 consecutive patients who underwent TAVI in Toulouse University Hospital, Rangueil, France. The studied population was divided into 2 groups: CAD-TAVI group and No CAD-TAVI group. Then, the CAD-TAVI group was segregated into 2 subgroups: PCI-TAVI group and No PCI-TAVI group. In-hospital adverse clinical outcomes were assessed in each group. Results. Pre-TAVI work-up revealed significant CAD in 36% of 1030 patients eligible for inclusion in the study. The overall prevalence of in-hospital death, stroke, major or life-threatening bleeding, minor bleeding, major vascular complications, minor vascular complications, pacemaker implantation, and acute kidney injury was 2.7%, 2.4%, 2.8%, 3.6%, 3.9%, 7.5%, 12.5%, and 2.7%, respectively. Among the studied population, 55% were admitted to the cardiac care unit. No significant statistical difference was observed between groups. Discussion. CAD-TAVI population was not more likely to develop in-hospital adverse clinical outcomes post-TAVI procedure compared to others. Also, no significant difference regarding in-hospital death was observed. In parallel, performing PCI prior to TAVI did not increase the risk of in-hospital death and complications. The difference in terms of the distribution of antithrombotic regimen may explain the higher prevalence of bleeding events in the PCI-TAVI group. Conclusion. This study provides direct clinical relevance useful in daily practice. No negative impact has been attributed to the presence of a concomitant CAD and/or preoperative PCI on the TAVI hospitalization period.
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- 2021
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7. Prevalence of Posttranscatheter Aortic Valve Implantation Vascular Complications in Real Life
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Anthony Matta, Ronan Canitrot, Vanessa Nader, Frederic Bouisset, Thibault Lhermusier, Francisco Campelo-Parada, Etienne Grunenwald, Bertrand Marcheix, Meyer Elbaz, Didier Carrie, and Jerome Roncalli
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Diseases of the circulatory (Cardiovascular) system ,RC666-701 - Abstract
Background. Vascular complications (VCs) are commonly observed after transfemoral transcatheter aortic valve implantation (TAVI) procedures. Closure devices for the access site were developed to reduce their incidence. We aim to evaluate the prevalence, predictors, and outcomes of the occurrence of post-TAVI VCs. Materials and Methods. A retrospective study was conducted on 1336 consecutive patients who underwent TAVI at the University Hospital of Toulouse, France, between January 2016 and March 2020. All included procedures were performed through the common femoral artery, and ProGlide® was the used closure device. The studied population was divided into two groups depending on the occurrence of VCs defined according to Valve Academic Research Consortium-2 criteria. Results. The mean age of the studied population was 84.4 ± 6.9, and 48% were male. 90% of TAVI interventions were performed through the right femoral artery. The prevalence of VCs was 18.8%, and 3.7% were major. Prolonged procedure duration was an independent predictor of VCs. Using the right access site and smaller introducer size (14 Fr) were preventive factors. No significant difference in mortality rate was detected between the two groups. Conclusion. This study showed a low prevalence for post-TAVI VCs, especially for the major type. An increase in bleeding events and prolonged cardiac care unit stay were the common adverse outcomes.
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- 2021
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8. Detection in coincidence of gravitational wave bursts with a network of interferometric detectors (I): Geometric acceptance and timing
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Arnaud, Nicolas, Barsuglia, Matteo, Bizouard, Marie-Anne, Canitrot, Philippe, Cavalier, Fabien, Davier, Michel, Hello, Patrice, and Pradier, Thierry
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General Relativity and Quantum Cosmology - Abstract
Detecting gravitational wave bursts (characterised by short durations and poorly modelled waveforms) requires to have coincidences between several interferometric detectors in order to reject non-stationary noise events. As the wave amplitude seen in a detector depends on its location with respect to the source direction and as the signal to noise ratio of these bursts are expected to be low, coincidences between antennas may not be so likely. This paper investigates this question from a statistical point of view by using a simple model of a network of detectors; it also estimates the timing precision of a detection in an interferometer which is an important issue for the reconstruction of the source location, based on time delays., Comment: low resolution figure 1 due to file size problems
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- 2001
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9. JMJD6 participates in the maintenance of ribosomal DNA integrity in response to DNA damage.
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Jérémie Fages, Catherine Chailleux, Jonathan Humbert, Suk-Min Jang, Jérémy Loehr, Jean-Philippe Lambert, Jacques Côté, Didier Trouche, and Yvan Canitrot
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Genetics ,QH426-470 - Abstract
Ribosomal DNA (rDNA) is the most transcribed genomic region and contains hundreds of tandem repeats. Maintaining these rDNA repeats as well as the level of rDNA transcription is essential for cellular homeostasis. DNA damages generated in rDNA need to be efficiently and accurately repaired and rDNA repeats instability has been reported in cancer, aging and neurological diseases. Here, we describe that the histone demethylase JMJD6 is rapidly recruited to nucleolar DNA damage and is crucial for the relocalisation of rDNA in nucleolar caps. Yet, JMJD6 is dispensable for rDNA transcription inhibition. Mass spectrometry analysis revealed that JMJD6 interacts with the nucleolar protein Treacle and modulates its interaction with NBS1. Moreover, cells deficient for JMJD6 show increased sensitivity to nucleolar DNA damage as well as loss and rearrangements of rDNA repeats upon irradiation. Altogether our data reveal that rDNA transcription inhibition is uncoupled from rDNA relocalisation into nucleolar caps and that JMJD6 is required for rDNA stability through its role in nucleolar caps formation.
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- 2020
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10. A Convenient Route to New (Radio)Fluorinated and (Radio)Iodinated Cyclic Tyrosine Analogs
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Maria Noelia Chao, Jean-Michel Chezal, Eric Debiton, Damien Canitrot, Tiffany Witkowski, Sophie Levesque, Françoise Degoul, Sébastien Tarrit, Barbara Wenzel, Elisabeth Miot-Noirault, Audrey Serre, and Aurélie Maisonial-Besset
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radioiodination ,radiofluorination ,tyrosine analogs ,TIC(OH) ,PET/SPECT imaging ,Medicine ,Pharmacy and materia medica ,RS1-441 - Abstract
The use of radiolabeled non-natural amino acids can provide high contrast SPECT/PET metabolic imaging of solid tumors. Among them, radiohalogenated tyrosine analogs (i.e., [123I]IMT, [18F]FET, [18F]FDOPA, [123I]8-iodo-L-TIC(OH), etc.) are of particular interest. While radioiodinated derivatives, such as [123I]IMT, are easily available via electrophilic aromatic substitutions, the production of radiofluorinated aryl tyrosine analogs was a long-standing challenge for radiochemists before the development of innovative radiofluorination processes using arylboronate, arylstannane or iodoniums salts as precursors. Surprisingly, despite these methodological advances, no radiofluorinated analogs have been reported for [123I]8-iodo-L-TIC(OH), a very promising radiotracer for SPECT imaging of prostatic tumors. This work describes a convenient synthetic pathway to obtain new radioiodinated and radiofluorinated derivatives of TIC(OH), as well as their non-radiolabeled counterparts. Using organotin compounds as key intermediates, [125I]5-iodo-L-TIC(OH), [125I]6-iodo-L-TIC(OH) and [125I]8-iodo-L-TIC(OH) were efficiently prepared with good radiochemical yield (RCY, 51–78%), high radiochemical purity (RCP, >98%), molar activity (Am, >1.5–2.9 GBq/µmol) and enantiomeric excess (e.e. >99%). The corresponding [18F]fluoro-L-TIC(OH) derivatives were also successfully obtained by radiofluorination of the organotin precursors in the presence of tetrakis(pyridine)copper(II) triflate and nucleophilic [18F]F− with 19–28% RCY d.c., high RCP (>98.9%), Am (20–107 GBq/µmol) and e.e. (>99%).
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- 2022
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11. Senataxin resolves RNA:DNA hybrids forming at DNA double-strand breaks to prevent translocations
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Sarah Cohen, Nadine Puget, Yea-Lih Lin, Thomas Clouaire, Marion Aguirrebengoa, Vincent Rocher, Philippe Pasero, Yvan Canitrot, and Gaëlle Legube
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Science - Abstract
Recent studies suggest key roles of RNA in DNA double-strand breaks repair. Here the authors identify the helicase senataxin to be involved in DNA repair and resolve RNA:DNA hybrids forming at DNA double-strand breaks.
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- 2018
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12. Consequences of Disregarding Metric Invariance on Diagnosis and Prognosis Using Psychological Tests
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David Blanco-Canitrot, Jesús M. Alvarado, and Daniel Ondé
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invariance ,differential item functioning ,predictive value of tests ,reliability and validity ,Psychology ,BF1-990 - Published
- 2018
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13. Homologous Recombination Assay
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Yvan Canitrot and Didier Trouche
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Biology (General) ,QH301-705.5 - Abstract
Repair of double strand break by homologous recombination was examined using U2OS cells or RG37 cells harbouring specific substrate developed by Puget et al. (2005) and Dumay et al. (2006), respectively, to measure the repair of DNA double strand breaks by homologous recombination. The substrate is composed of two inactive copies of the GFP gene. The upstream copy is inactive due to the absence of promoter, the downstream copy present a promoter but is inactivated by the insertion of the sequence coding for the recognition site of the I-SceI enzyme. The substrate is stably expressed in cells after its insertion in the genome and present as a unique copy. The unique DNA double strand break is then induced by the expression of the I-SceI enzyme after cell transfection with a plasmid coding for the I-SceI enzyme.
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- 2013
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14. Neutral Comet Assay
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Elisa Boutet-Robinet, Didier Trouche, and Yvan Canitrot
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Biology (General) ,QH301-705.5 - Abstract
The Comet assay (or Single Cell Gel Electrophoresis assay) is a sensitive technique to detect DNA damage at the level of an individual cell. This technique is based on micro-electrophoresis of cells DNA content. Briefly, cells are embedded in agarose, lysed and submitted to an electric field, before the staining step with a fluorescent DNA binding dye. Damaged DNA (charged DNA) migrates in this field, forming the tail of a “comet”, while undamaged DNA remained in the head of the “comet”. The following document describes the protocol to realize a neutral comet assay. This assay can be applied to different cell types and has been useful for numerous applications in fields of toxicology or DNA damage and repair.
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- 2013
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15. Electric urban light vehicles structural integrity and occupant protection validation through experimental crash tests
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Eichinger, Barbara, Dullnig, Sabine, Perlo, Pietro, Biasiotto, Marco, Romo, Javier, El-Baraka, Khadija, Canitrot, Didier, Faedo, Walter, Baron, Filippo, Skigin, Leonid, Karasikov, Nir, Tavernini, Davide, Sorniotti, Aldo, Catona, Giuseppe, Tanzi, Carlo, and Verhulst, Eric
- Abstract
Multi-Moby project, funded under H2020 n° 101006953, aims at developing technology for safe, efficient and affordable urban electric vehicles. The objective of the paper is to show the results achieved in relation to structural integrity and occupant protection in the first year of the project. In a first stage simulation tools have been used to optimise the vehicle structure crashworthiness at different crash configuration based on smart use of High Strength Steels focused to simplified and affordable manufacturing processes. Once the structural behaviour met requirements and expectations, the restraint system has been developed. After design optimisation, three vehicles have been prototyped to perform three crash tests, two of them frontal, corresponding to Regulation 137 and Regulation 94, and one lateral, corresponding to Regulation 95.
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- 2023
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16. Multi-Moby – Smart solutions for safe, efficient and affordable light electric vehicles
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Eichinger, Barbara, Dullnig, Sabine, Perlo, Pietro, Biasiotto, Marco, Garcia, Javier Romo, El-Baraka, Khadija, Canitrot, Didier, Jugovic, Svetislav, Faedo, Walter, Mioni, Andrea, Skigin, Leonid, Karasikov, Nir, So, Kai Man, Tavolo, Gaetano, Tavernini, Davide, Sorniotti, Aldo, Catona, Giuseppe, Tanzi, Carlo, and Verhulst, Eric
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Multi-Moby is an ambitious project aiming at quickly finalising the results of a cluster of ongoing and past European projects, addressing the development of technologies for safe, efficient and affordable urban electric vehicles (EVs). This paper presents the developments that have been implemented in the first half of Multi-Moby, which deals with low-cost M1 and N1 EVs, to be manufactured via low-investment and lean processes and plants. The Multi-Moby EVs have excellent passive safety characteristics, enhanced by pre-emptive active safety controllers. The vehicles can be coupled with efficient 100 V or 48 V powertrains. Fast charging is enabled by the integrated design of hybrid supercapacitor-battery cells and wall box chargers. The project will also consider low-cost automated driving solutions, with focus on gimbal-based camera systems for environmental sensing and detection.
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- 2023
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17. Msl2 is a novel component of the vertebrate DNA damage response.
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Zheng Lai, Simona Moravcová, Yvan Canitrot, Lukasz P Andrzejewski, Dervla M Walshe, and Stephen Rea
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Medicine ,Science - Abstract
hMSL2 (male-specific lethal 2, human) is a RING finger protein with ubiquitin ligase activity. Although it has been shown to target histone H2B at lysine 34 and p53 at lysine 351, suggesting roles in transcription regulation and apoptosis, its function in these and other processes remains poorly defined. To further characterize this protein, we have disrupted the Msl2 gene in chicken DT40 cells. Msl2(-/-) cells are viable, with minor growth defects. Biochemical analysis of the chromatin in these cells revealed aberrations in the levels of several histone modifications involved in DNA damage response pathways. DNA repair assays show that both Msl2(-/-) chicken cells and hMSL2-depleted human cells have defects in non-homologous end joining (NHEJ) repair. DNA damage assays also demonstrate that both Msl2 and hMSL2 proteins are modified and stabilized shortly after induction of DNA damage. Moreover, hMSL2 mediates modification, presumably ubiquitylation, of a key DNA repair mediator 53BP1 at lysine 1690. Similarly, hMSL1 and hMOF (males absent on the first) are modified in the presence of hMSL2 shortly after DNA damage. These data identify a novel role for Msl2/hMSL2 in the cellular response to DNA damage. The kinetics of its stabilization suggests a function early in the NHEJ repair pathway. Moreover, Msl2 plays a role in maintaining normal histone modification profiles, which may also contribute to the DNA damage response.
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- 2013
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18. Differential Expression of Cerebellar Metabotropic Glutamate Receptors mGLUR2/3 and mGLUR4a after the Administration of a Convulsant Drug and the Adenosine Analogue Cyclopentyladenosine
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Girardi, Elena Silvia, Canitrot, Juan, Antonelli, Marta, González, Nélida N., and Coirini, Héctor
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- 2007
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19. Cohesin protects genes against γH2AX Induced by DNA double-strand breaks.
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Pierre Caron, Francois Aymard, Jason S Iacovoni, Sébastien Briois, Yvan Canitrot, Beatrix Bugler, Laurent Massip, Ana Losada, and Gaëlle Legube
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Genetics ,QH426-470 - Abstract
Chromatin undergoes major remodeling around DNA double-strand breaks (DSB) to promote repair and DNA damage response (DDR) activation. We recently reported a high-resolution map of γH2AX around multiple breaks on the human genome, using a new cell-based DSB inducible system. In an attempt to further characterize the chromatin landscape induced around DSBs, we now report the profile of SMC3, a subunit of the cohesin complex, previously characterized as required for repair by homologous recombination. We found that recruitment of cohesin is moderate and restricted to the immediate vicinity of DSBs in human cells. In addition, we show that cohesin controls γH2AX distribution within domains. Indeed, as we reported previously for transcription, cohesin binding antagonizes γH2AX spreading. Remarkably, depletion of cohesin leads to an increase of γH2AX at cohesin-bound genes, associated with a decrease in their expression level after DSB induction. We propose that, in agreement with their function in chromosome architecture, cohesin could also help to isolate active genes from some chromatin remodelling and modifications such as the ones that occur when a DSB is detected on the genome.
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- 2012
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20. Correction: The E1A-Associated p400 Protein Modulates Cell Fate Decisions by the Regulation of ROS Homeostasis.
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Lise Mattera, Céline Courilleau, Gaëlle Legube, Takeshi Ueda, Rikiro Fukunaga, Martine Chevillard-Briet, Yvan Canitrot, Fabrice Escaffit, and Didier Trouche
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Genetics ,QH426-470 - Published
- 2010
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21. The E1A-associated p400 protein modulates cell fate decisions by the regulation of ROS homeostasis.
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Lise Mattera, Céline Courilleau, Gaëlle Legube, Takeshi Ueda, Rikiro Fukunaga, Martine Chevillard-Briet, Yvan Canitrot, Fabrice Escaffit, and Didier Trouche
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Genetics ,QH426-470 - Abstract
The p400 E1A-associated protein, which mediates H2A.Z incorporation at specific promoters, plays a major role in cell fate decisions: it promotes cell cycle progression and inhibits induction of apoptosis or senescence. Here, we show that p400 expression is required for the correct control of ROS metabolism. Depletion of p400 indeed increases intracellular ROS levels and causes the appearance of DNA damage, indicating that p400 maintains oxidative stress below a threshold at which DNA damages occur. Suppression of the DNA damage response using a siRNA against ATM inhibits the effects of p400 on cell cycle progression, apoptosis, or senescence, demonstrating the importance of ATM-dependent DDR pathways in cell fates control by p400. Finally, we show that these effects of p400 are dependent on direct transcriptional regulation of specific promoters and may also involve a positive feedback loop between oxidative stress and DNA breaks since we found that persistent DNA breaks are sufficient to increase ROS levels. Altogether, our results uncover an unexpected link between p400 and ROS metabolism and allow deciphering the molecular mechanisms largely responsible for cell proliferation control by p400.
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- 2010
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22. Characterization of a natural mutator variant of human DNA polymerase lambda which promotes chromosomal instability by compromising NHEJ.
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Gloria Terrados, Jean-Pascal Capp, Yvan Canitrot, Miguel García-Díaz, Katarzyna Bebenek, Tomas Kirchhoff, Alberto Villanueva, François Boudsocq, Valérie Bergoglio, Christophe Cazaux, Thomas A Kunkel, Jean-Sébastien Hoffmann, and Luis Blanco
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Medicine ,Science - Abstract
BACKGROUND:DNA polymerase lambda (Pollambda) is a DNA repair polymerase, which likely plays a role in base excision repair (BER) and in non-homologous end joining (NHEJ) of DNA double-strand breaks (DSB). PRINCIPAL FINDINGS:Here, we described a novel natural allelic variant of human Pollambda (hPollambda) characterized by a single nucleotide polymorphism (SNP), C/T variation in the first base of codon 438, resulting in the amino acid change Arg to Trp. In vitro enzyme activity assays of the purified W438 Pollambda variant revealed that it retained both DNA polymerization and deoxyribose phosphate (dRP) lyase activities, but had reduced base substitution fidelity. Ectopic expression of the W438 hPollambda variant in mammalian cells increases mutation frequency, affects the DSB repair NHEJ pathway, and generates chromosome aberrations. All these phenotypes are dependent upon the catalytic activity of the W438 hPollambda. CONCLUSIONS:The expression of a cancer-related natural variant of one specialized DNA polymerase can be associated to generic instability at the cromosomal level, probably due a defective NHEJ. These results establish that chromosomal aberrations can result from mutations in specialized DNA repair polymerases.
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- 2009
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23. Correction: Characterization of a Natural Mutator Variant of Human DNA Polymerase λ which Promotes Chromosomal Instability by Compromising NHEJ.
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Gloria Terrados, Jean-Pascal Capp, Yvan Canitrot, Miguel García-Díaz, Katarzyna Bebenek, Tomas Kirchhoff, Alberto Villanueva, François Boudsocq, Valérie Bergoglio, Christophe Cazaux, Thomas A. Kunkel, Jean-Sébastien Hoffmann, and Luis Blanco
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Medicine ,Science - Published
- 2009
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24. Deregulated DNA polymerase β strengthens ionizing radiation-induced nucleotidic and chromosomal instabilities
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Fréchet, Mathilde, Canitrot, Yvan, Bieth, Anne, Dogliotti, Eugenia, Cazaux, Christophe, and Hoffmann, Jean-Sébastien
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- 2002
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25. Enhanced expression and activity of DNA polymerase β in human ovarian tumor cells: impact on sensitivity towards antitumor agents
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Bergoglio, Valérie, Canitrot, Yvan, Hogarth, Linda, Minto, Lynne, Howell, Stephen B, Cazaux, Christophe, and Hoffmann, Jean-Sébastien
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- 2001
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26. Endovascular hypothermia after cardiac arrest in a Chilean ICU
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Canitrot, M and Ugarte, S
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- 2014
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27. Arterial-jugular bulb differences in pCO2, lactate, serum sodium and C-reactive protein in neurocritical patients
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Canitrot, M and Ugarte, S
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- 2014
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28. Mutator phenotype of BCR – ABL transfected Ba/F3 cell lines and its association with enhanced expression of DNA polymerase β
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Canitrot, Y, Lautier, D, Laurent, G, Fréchet, M, Ahmed, A, Turhan, AG, Salles, B, Cazaux, C, and Hoffmann, JS
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- 1999
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29. Myocardial bridging is significantly associated to myocardial infarction with non-obstructive coronary arteries
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Matta, Anthony, Nader, Vanessa, Canitrot, Ronan, Delmas, Clement, Bouisset, Frederic, Lhermusier, Thibault, Blanco, Stephanie, Campelo-Parada, Francisco, Elbaz, Meyer, Carrie, Didier, Galinier, Michel, and Roncalli, Jerome
- Abstract
Graphical AbstractIllustration of the importance to search for MB in MINOCA patients. MB, myocardial bridging; MINOCA, myocardial infarction with no obstructive coronary artery.
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- 2022
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30. The present status of the VIRGO Central Interferometer*
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E. Turri, Giancarlo Cella, D. Passuello, S. Mataguez, C. N. Man, J. Y. Vinet, F. Garufi, F. Fidecaro, R. De Rosa, Fausto Acernese, A. Errico, G. M. Guidi, C. Bradaschia, M. De Rosa, H. Trinquet, Thierry Pradier, Sergio Cavaliere, Ettore Majorana, J. C. Lacotte, O. Veziant, Ruggero Stanga, B. Lagrange, H. Fang, G. Giordano, Fabrizio Barone, A. Eleuteri, C. Girard, G. Gennaro, P. Tourrenc, G. Calamai, Rosa Poggiani, P. Marin, C. Eder, T. Regimbau, R. Chiche, L. Milano, Alban Remillieux, J. P. Scheidecker, D. Verkindt, E. Cuoco, P. Mugnier, L. Fournier, François Bondu, R. Hermel, S. Braccini, P. Rivoirard, S. Cuzon, J. Ramonet, F. Frasconi, M. Taurigna, G. Losurdo, Ketevan Qipiani, Salvatore Solimeno, C. Palomba, L. Di Fiore, A. Giazotto, R. Flaminio, I. Ferrante, M. Iannarelli, R. Passaquieti, D. Babusci, A. Pasqualetti, L. Giacobone, J. M. Teuler, L. Nicolosi, V Dattilo, H. Vocca, F. Martelli, R. Taddei, R. Cavalieri, B. Mansoux, C. Michel, A. Brillet, M. Loupias, F. Cavalier, M. Varvella, R. Sottile, J. M. Innocent, A. Masserot, F. Ricci, Luisa Bracci, O. Lodygenski, F. Richard, J.-P. Coulon, V. Brisson, L. Fabbroni, F. Cleva, R. Bilhaut, M. Barsuglia, J.-D. Fournier, Zhenyu Zhang, L. Holloway, C. Bourgoin, V. Loriette, J. C. Marrucho, F. Vetrano, Samuele Cortese, C. Casciano, F. Chollet, J.-M. Mackowski, L. Massonnet, Ph. Heusse, F. Paoletti, P. N. Y. David, J. L. Montorio, Fabio Marchesoni, P. Hello, A. Di Virgilio, M. Perciballi, M. A. Bizouard, A. Reboux, P. Canitrot, N. Arnaud, D. Dufournaud, Enrico Calloni, P. Puppo, Maurizio Ripepe, D. Boget, P. Rapagnani, J. P. Roger, A. Bozzi, P. La Penna, Claude Boccara, Gianpaolo Evangelista, B. Lieunard, José Pacheco, A. Viceré, Roberto Cecchi, M. Mazzoni, E. Jules, G. Ballardin, M. Dehamme, P. Dominici, D. Buskulic, Luca Gammaitoni, J. Cachenaut, S. Frasca, M. Davier, V. Reita, P. Ganau, P. Amico, P. Popolizio, Thomas Cokelaer, M. Yvert, B. Mours, M. Punturo, M. Mencik, L. Pinard, F. Bellachia, M. Gaspard, Angela Delli Paoli, Ciro Cattuto, C. Arnault, N. Morgado, J. L. Beney, M. Leliboux, H. Heitmann, T. Lomtadze, F. Marion, B. Caron, D. Enard, F., Acernese, P., Amico, N., Arnaud, C., Arnault, D., Babusci, G., Ballardin, F., Barone, M., Barsuglia, F., Bellachia, J. L., Beney, R., Bilhaut, M. A., Bizouard, C., Boccara, D., Boget, F., Bondu, C., Bourgoin, A., Bozzi, L., Bracci, S., Braccini, C., Bradaschia, A., Brillet, V., Brisson, D., Buskulic, J., Cachenaut, G., Calamai, Calloni, Enrico, P., Canitrot, B., Caron, C., Casciano, C., Cattuto, F., Cavalier, S., Cavaliere, R., Cavalieri, R., Cecchi, G., Cella, R., Chiche, F., Chollet, F., Cleva, T., Cokelaer, S., Cortese, J. P., Coulon, E., Cuoco, S., Cuzon, V., Dattilo, P. Y., David, M., Davier, M., DE ROSA, DE ROSA, Rosario, M., Dehamme, L., DI FIORE, A., DI VIRGILIO, P., Dominici, D., Dufournaud, C., Eder, A., Eleuteri, D., Enard, A., Errico, G., Evangelista, L., Fabbroni, H., Fang, I., Ferrante, F., Fidecaro, R., Flaminio, J. D., Fournier, L., Fournier, S., Frasca, F., Frasconi, L., Gammaitoni, P., Ganau, Garufi, Fabio, M., Gaspard, G., Gennaro, L., Giacobone, A., Giazotto, G., Giordano, C., Girard, G., Guidi, H., Heitmann, P., Hello, R., Hermel, P., Heusse, L., Holloway, M., Iannarelli, J. M., Innocent, E., Jule, P., LA PENNA, J. C., Lacotte, B., Lagrange, M., Leliboux, B., Lieunard, O., Lodygensky, T., Lomtadze, V., Loriette, G., Losurdo, M., Loupia, J. M., Mackowski, E., Majorana, C. N., Man, B., Mansoux, F., Marchesoni, P., Marin, F., Marion, J. C., Marrucho, F., Martelli, A., Masserot, L., Massonnet, S., Mataguez, M., Mazzoni, M., Mencik, C., Michel, Milano, Leopoldo, J. L., Montorio, N., Morgado, B., Mour, P., Mugnier, L., Nicolosi, J., Pacheco, C., Palomba, F., Paoletti, A., Paoli, A., Pasqualetti, R., Passaquieti, D., Passuello, M., Perciballi, L., Pinard, R., Poggiani, P., Popolizio, T., Pradier, M., Punturo, P., Puppo, K., Qipiani, J., Ramonet, P., Rapagnani, A., Reboux, T., Regimbau, V., Reita, A., Remillieux, F., Ricci, F., Richard, M., Ripepe, P., Rivoirard, J. P., Roger, J. P., Scheidecker, Solimeno, Salvatore, R., Sottile, R., Stanga, R., Taddei, M., Taurigna, J. M., Teuler, P., Tourrenc, H., Trinquet, E., Turri, M., Varvella, D., Verkindt, F., Vetrano, O., Veziant, A., Vicere, J. Y., Vinet, H., Vocca, M., Yvert, and Z., Zhang
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Physics ,Interferometry ,Detection of gravitational waves ,Gravitational wave detectors and experiments ,Physics and Astronomy (miscellaneous) ,Debugging ,Onde gravitazionali ,interferometri ,astrofisica ,media_common.quotation_subject ,Detector ,Astronomy ,Antenna (radio) ,gravitational wave ,media_common - Abstract
The VIRGO Central Interferometer (CITF) is a short suspended interferometer operated with the central area elements of the VIRGO detector. The main motivation behind the CITF is to allow the integration and debugging of a large part of the subsystems of VIRGO while the construction of the long arms of the antenna is being completed. This will permit a faster commissioning of the full-size antenna. In fact, almost all the main components of the CITF, with the exception of the large mirrors and a few other details, are the same as those to be used for the full-size detector. In this paper the present status of the VIRGO CITF is reported.
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- 2002
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31. THE PRESENT STATUS OF THE VIRGO CENTRAL INTERFEROMETER
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F. ACERNESE, P. AMICO, N. ARNAUD, C. ARNAULT, D. BABUSCI, G. BALLARDIN, F. BARONE, M. BARSUGLIA, F. BELLACHIA, J. L. BENEY, R. BILHAUT, M. A. BIZOUARD, C. BOCCARA, D. BOGET, F. BONDU, C. BOURGOIN, A. BOZZI, L. BRACCI, S. BRACCINI, C. BRADASCHIA, A. BRILLET, V. BRISSON, D. BUSKULIC, J. CACHENAUT, G. CALAMAI, CALLONI, ENRICO, P. CANITROT, B. CARON, C. CASCIANO, C. CATTUTO, F. CAVALIER, S. CAVALIERE, R. CAVALIERI, R. CECCHI, G. CELLA, R. CHICHE, F. CHOLLET, F. CLEVA, T. COKELAER, S. CORTESE, J. P. COULON, E. CUOCO, S. CUZON, V. DATTILO, P. Y. DAVID, M. DAVIER, R. D. ROSA, M. DEHAMME, L. D. FIORE, A. D. VIRGILIO, P. DOMINICI, D. DUFOURNAUD, C. EDER, A. ELEUTERI, D. ENARD, A. ERRICO, G. EVANGELITA, L. FABBRONI, H. FANG, I. FERRANTE, F. FIDECARO, R. FLAMINIO, J. D. FOURNIER, L. FOURNIER, S. FRASCA, F. FRASCONI, L. GAMMAITONI, P. GANAU, M. GASPARD, G. GENNARO, L. GIACOBONE, A. GIAZOTTO, G. GIORDANO, C. GIRARD, G. GUIDI, H. HEITMANN, P. HELLO, R. HERMEL, P. HEUSSE, L. HOLLOWAY, M. IANNARELLI, J. M. INNOCENT, E. JULES, P. L. PENNA, J. C. LACOTTE, B. LAGRANGE, DE ROSA, ROSARIO, GARUFI, FABIO, MILANO, LEOPOLDO, F., Acernese, P., Amico, N., Arnaud, C., Arnault, D., Babusci, G., Ballardin, F., Barone, M., Barsuglia, F., Bellachia, J. L., Beney, R., Bilhaut, M. A., Bizouard, C., Boccara, D., Boget, F., Bondu, C., Bourgoin, A., Bozzi, L., Bracci, S., Braccini, C., Bradaschia, A., Brillet, V., Brisson, D., Buskulic, J., Cachenaut, G., Calamai, Calloni, Enrico, P., Canitrot, B., Caron, C., Casciano, C., Cattuto, F., Cavalier, S., Cavaliere, R., Cavalieri, R., Cecchi, G., Cella, R., Chiche, F., Chollet, F., Cleva, T., Cokelaer, S., Cortese, J. P., Coulon, E., Cuoco, S., Cuzon, V., Dattilo, P. Y., David, M., Davier, DE ROSA, Rosario, R. D., Rosa, M., Dehamme, L. D., Fiore, A. D., Virgilio, P., Dominici, D., Dufournaud, C., Eder, A., Eleuteri, D., Enard, A., Errico, G., Evangelita, L., Fabbroni, H., Fang, I., Ferrante, F., Fidecaro, R., Flaminio, J. D., Fournier, L., Fournier, S., Frasca, F., Frasconi, L., Gammaitoni, P., Ganau, Garufi, Fabio, M., Gaspard, G., Gennaro, L., Giacobone, A., Giazotto, G., Giordano, C., Girard, G., Guidi, H., Heitmann, P., Hello, R., Hermel, P., Heusse, L., Holloway, M., Iannarelli, J. M., Innocent, E., Jule, P. L., Penna, J. C., Lacotte, B., Lagrange, and Milano, Leopoldo
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- 2002
32. Last stage control and mechanical transfer function measurement of the VIRGO suspensions
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R. De Rosa, G. Ballardin, R. Hermel, R. Cavalieri, Gianpaolo Evangelista, R. Passaquieti, B. Lieunard, J.-P. Coulon, A. Giazotto, J.-D. Fournier, M. Davier, I. Ferrante, J. Ramonet, C. Arnault, A. Di Virgilio, Luca Gammaitoni, L. Pinard, F. Bellachia, M. Leliboux, C. Girard, M. Loupias, F. Vetrano, C. Palomba, S. Frasca, P. N. Y. David, M. Varella, Angela Delli Paoli, Ciro Cattuto, C. N. Man, J. Y. Vinet, H. Vocca, F. Martelli, Marina Mazzoni, Claude Boccara, Zhenyu Zhang, F. Fidecaro, G. M. Guidi, P. Puppo, Maurizio Ripepe, F. Richard, H. Heitmann, M. Mencik, L. Giacobone, F. Paoletti, José Pacheco, A. Bozzi, F. Garufi, F. Ricci, J. C. Lacotte, S. Mataguez, L. Di Fiore, Roberto Cecchi, M. Iannarelli, N. Morgado, M. Barsuglia, Rosa Poggiani, R. Chiche, D. Buskulic, E. Jules, Teimuraz Lomtadze, H. Fang, F. Chollet, J.-M. Mackowski, R. Sottile, B. Mours, M. Punturo, F. Cavalier, G. Cella, Sergio Cavaliere, B. Mansoux, A. Masserot, J. M. Innocent, Thierry Pradier, A. Eleuteri, V. Loriette, J. P. Scheidecker, D. Enard, M. Perciballi, O. Veziant, G. Gennaro, P. Marin, C. Eder, M. Yvert, L. Massonnet, Ketevan Qipiani, Ruggero Stanga, J. L. Montorio, E. Cuoco, B. Lagrange, R. Bilhaut, L. Holloway, D. Passuello, J. L. Beney, F. Marion, M. A. Bizouard, B. Caron, M. Gaspard, A. Viceré, P. Amico, P. La Penna, A. Reboux, Thomas Cokelaer, Fabio Marchesoni, P. Hello, D. Boget, J. P. Roger, M. De Rosa, Fabrizio Barone, R. Taddei, H. Trinquet, Salvatore Solimeno, G. Giordano, P. Ganau, D. Babusci, P. Tourrenc, G. Calamai, L. Fabbroni, G. Losurdo, Alban Remillieux, L. Milano, S. Cuzon, Ettore Majorana, D. Verkindt, Samuele Cortese, M. Taurigna, J. Cachenaut, P. Mugnier, V. Reita, L. Fournier, A. Pasqualetti, F. Frasconi, François Bondu, P. Rivoirard, R. Flaminio, Fausto Acernese, A. Errico, T. Regimbau, Ph. Heusse, M. Maiorino, V. Brisson, P. Canitrot, N. Arnaud, P. Rapagnani, J. M. Teuler, L. Nicolosi, C. Michel, Luisa Bracci, P. Popolizio, O. Lodygenski, F. Cleva, C. Bourgoin, M. Dehamme, P. Dominici, J. C. Marrucho, C. Bradaschia, D. Dufournaud, Enrico Calloni, E. Turri, S. Braccini, V. Dattilo, A. Brillet, C. Casciano, A., Bozzi, C., Bourgoin, S., Cortese, A., Errico, D., Enard, S., Mataguez, A., Paoli, A., Pasqualetti, P., Popolizio, F., Richard, J. M., Teuler, Z., Zhang, C., Boccara, M., Leliboux, V., Loriette, V., Reita, J. P., Roger, P., Ganau, B., Lagrange, J. M., Mackowski, C., Michel, J. L., Montorio, N., Morgado, L., Pinard, A., Remillieux, L., Bracci, G., Calamai, E., Cuoco, P., Dominici, L., Fabbroni, G., Guidi, G., Losurdo, F., Martelli, M., Mazzoni, M., Ripepe, R., Stanga, F., Vetrano, F., Acernese, F., Barone, Calloni, Enrico, S., Cavaliere, M., DE ROSA, DE ROSA, Rosario, L., DI FIORE, A., Eleuteri, G., Evangelista, Garufi, Fabio, M., Maiorino, L., Milano, K., Qipiani, S., Solimeno, M., Varvella, P., Amico, C., Cattuto, L., Gammaitoni, F., Marchesoni, M., Punturo, H., Vocca, G., Ballardin, S., Braccini, C., Bradaschia, C., Casciano, R., Cavalieri, R., Cecchi, G., Cella, V., Dattilo, A., DI VIRGILIO, I., Ferrante, F., Fidecaro, F., Frasconi, G., Gennaro, A., Giazotto, L., Holloway, P., LA PENNA, T., Lomtadze, L., Nicolosi, F., Paoletti, R., Passaquieti, D., Passuello, R., Poggiani, R., Taddei, A., Vicere, S., Frasca, E., Majorana, C., Palomba, M., Perciballi, P., Puppo, P., Rapagnani, F., Ricci, N., Arnaud, C., Arnault, M., Barsuglia, J. L., Beney, R., Bilhaut, M. A., Bizouard, V., Brisson, P., Canitrot, F., Cavalier, R., Chiche, S., Cuzon, M., Davier, M., Dehamme, C., Eder, M., Gaspard, P., Hello, P., Heusse, E., Jule, O., Lodygensky, B., Mansoux, J. C., Marrucho, M., Mencik, P., Marin, T., Pradier, A., Reboux, P., Rivoirard, M., Taurigna, F., Bellachia, D., Boget, D., Buskulic, B., Caron, F., Chollet, P. Y., David, D., Dufournaud, R., Flaminio, L., Fournier, L., Giacobone, C., Girard, R., Hermel, J. C., Lacotte, B., Lieunard, F., Marion, A., Masserot, L., Massonnet, B., Mour, P., Mugnier, J., Ramonet, R., Sottile, D., Verkindt, O., Veziant, M., Yvert, D., Babusci, H., Fang, G., Giordano, M., Iannarelli, E., Turri, F., Bondu, A., Brillet, J., Cachenaut, F., Cleva, T., Cokelaer, J. P., Coulon, J. D., Fournier, H., Heitmann, J. M., Innocent, M., Loupia, C. N., Man, J., Pacheco, T., Regimbau, J. P., Scheidecker, H., Trinquet, P., Tourrenc, J. Y., Vinet, Cavaliere, Sergio, and Virgo, Collaboration
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Physics ,Onde gravitazionali ,interferometri ,sospensioni ,Automatic control ,Gravitational wave ,business.industry ,Detector ,Astrophysics::Instrumentation and Methods for Astrophysics ,Pendulum ,Transfer function ,Optics ,Control theory ,Control system ,Sensitivity (control systems) ,Suspension (vehicle) ,business ,Instrumentation - Abstract
The automatic control of the suspended mirrors is a major task in operating an interferometric gravitational wave antenna. To reach the extreme sensitivity required for this kind of detector, an accurate alignment and a stable locking of the interferometer on its working point are crucial. The solution of this problem is particularly complex in the case of a multistage pendulum, such as the suspension system for seismic isolation adopted in VIRGO. A precise knowledge of the suspension mechanical transfer functions (TFs) for different forces applied in the control servo-loops represents essential information to reach the goal. In this article, we describe the apparatus we developed to measure the VIRGO suspension TF and we report the results thus obtained on full-scale suspensions at the VIRGO site. Preliminary results for the implemented control system of the last suspension stage are also presented.
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- 2002
33. The Virgo Suspensions
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J. Ramonet, Samuele Cortese, L. Milano, H. Vocca, M. Yvert, Teimuraz Lomtadze, D. Passuello, Thierry Pradier, R. Bilhaut, A. Viceré, M. Gaspard, H. Fang, Ph. Heusse, P. Canitrot, N. Arnaud, P. Rapagnani, F. Garufi, R. De Rosa, C. Arnault, J. L. Beney, F. Frasconi, A. Di Virgilio, L. Giacobone, R. Sottile, B. Mansoux, A. Masserot, P. Amico, G. Cella, P. Ganau, Fausto Acernese, R. Flaminio, B. Mours, P. La Penna, M. Leliboux, A. Errico, F. Marion, M. Punturo, M. Varvella, A. Bozzi, C. Girard, B. Caron, V. Loriette, C. N. Man, J. Y. Vinet, L. Pinard, F. Fidecaro, M. Iannarelli, M. Dehamme, L. Holloway, T. Regimbau, P. Dominici, Thomas Cokelaer, F. Bellachia, G. M. Guidi, Angela Delli Paoli, Ciro Cattuto, F. Martelli, C. Bradaschia, Marina Mazzoni, S. Mataguez, F. Paoletti, D. Buskulic, F. Cavalier, J. L. Montorio, J. M. Innocent, Zhenyu Zhang, R. Passaquieti, A. Giazotto, José Pacheco, J. M. Teuler, I. Ferrante, L. Nicolosi, S. Cuzon, C. Michel, G. Ballardin, Sergio Cavaliere, A. Reboux, V. Brisson, H. Heitmann, M. Mencik, S. Braccini, N. Morgado, M. De Rosa, J. P. Roger, R. Hermel, Luisa Bracci, O. Lodygenski, H. Trinquet, F. Chollet, J.-M. Mackowski, F. Cleva, Roberto Cecchi, A. Eleuteri, G. Giordano, C. Bourgoin, J. C. Marrucho, Fabrizio Barone, Ettore Majorana, D. Enard, M. Loupias, D. Dufournaud, E. Jules, E. Turri, P. Puppo, Maurizio Ripepe, Enrico Calloni, M. Davier, P. Tourrenc, G. Calamai, Gianpaolo Evangelista, B. Lieunard, L. Di Fiore, M. Barsuglia, Luca Gammaitoni, G. Losurdo, V. Dattilo, A. Brillet, S. Frasca, M. Taurigna, Alban Remillieux, D. Verkindt, P. Popolizio, L. Massonnet, Fabio Marchesoni, R. Taddei, P. Mugnier, L. Fournier, Patrice Hello, J. Cachenaut, V. Reita, G. Gennaro, François Bondu, P. Rivoirard, M. Perciballi, D. Boget, P. Marin, C. Casciano, C. Eder, L. Fabbroni, Marie-Anne Bizouard, A. Pasqualetti, C. Palomba, F. Ricci, Ketevan Qipiani, E. Cuoco, F. Richard, Claude Boccara, Rosa Poggiani, R. Chiche, F. Vetrano, P. N. Y. David, Salvatore Solimeno, R. Cavalieri, J.-P. Coulon, J.-D. Fournier, D. Babusci, J. C. Lacotte, Ruggero Stanga, J. P. Scheidecker, O. Veziant, and B. Lagrange
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Physics ,business.product_category ,Gravitational wave detectors and experiments ,Physics and Astronomy (miscellaneous) ,business.industry ,Payload ,Seismic noise ,Interferometry ,Optics ,Control system ,Six degrees of freedom ,business ,Suspension (vehicle) ,Beam (structure) ,Digital camera - Abstract
The VIRGO suspensions are chains of passive mechanical filters designed to isolate the interferometer mirrors from seismic noise starting from a few Hz. In order to reduce the low-frequency swing of the mirror along the beam, an active control system, acting at the level of the suspension point, damps the main resonant modes of the system (all below 2.5 Hz). Another control loop, at the level of the optical payload, makes use of a digital camera monitoring the mirror position in all six degrees of freedom. Its main goal is to decrease the rms angular displacements of the mirror, on a time scale of several minutes, down to less than 1 μrad. All the seven suspensions of the VIRGO central interferometer are presently in operation, while the assembly of the last two, for the terminal mirrors, is in progress. The design and performance of the system are described in this paper. PACS number: 0480N (Some figures in this article are in colour only in the electronic version)
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- 2002
34. Productividad y ocupación en la producción de azúcar en Tucumán
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Adolfo Canitrot and Juan Sommer
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Economics as a science ,HB71-74 - Abstract
La ocupación en la producción de azúcar en Tucumán ha decaído considerablemente en la última década. Como la producción de azúcar es la actividad más importante en la región se ha producido una alta tasa de desempleo y una emigración de trabajadores. Este proceso no ha sido continuo, sino sujeto a fluctuaciones debido a la inestabilidad del precio y oferta del producto. Este trabajo analiza las tendencias del mercado y la producción y concluye que la caída del empleo es una consecuencia del estancamiento de la demanda combinado con un rápido aumento del rendimiento de la caña de azúcar. La inestabilidad es por otra parte la consecuencia de los altos costos, la gran proporción de pequeños productores y la existencia de ajustes de tipo telaraña. El artículo finaliza con la proyección de posibles niveles de empleo en los próximos cinco años, de acuerdo a diferentes hipótesis alternativas.
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- 1972
35. Encephalopathy with electrical status epilepticus during sleep: Cognitive and executive improvement after epilepsy surgery.
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Fournier-Del Castillo, Concepción, García-Fernández, Marta, Pérez-Jiménez, María-Ángeles, Ugalde-Canitrot, Arturo, Álvarez-Linera, Juan, Ruiz-Falcó, María-Luz, and Villarejo-Ortega, Francisco
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- 2014
- Full Text
- View/download PDF
36. Interpreting troponin elevation in the setting of infective endocarditis: Causes and prognostic value.
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Canitrot, R., Delmas, C., Delon, C., Biendel, C., Porte, L., Bouisset, F., Laperche, C., Labaste, F., Roncalli, J., Elbaz, M., Carrie, D., Galinier, M., and Lavie Badie, Y.
- Abstract
Measurement of cardiac troponin (cTn) levels in blood is standard for diagnosis and risk stratification in cardiac emergencies. To investigate the causes, link to underlying coronary artery disease and prognostic value of cTn release in infective endocarditis (IE). Eighty-six consecutive patients hospitalized for acute IE, with at least one cTn drawn and a coronary angiogram performed, were reviewed retrospectively. Factors related to the increase of cTn above the 99th percentile or above 10 times normal (> 10N), as well as their prognostic impact, were assessed. The mean patient age was 63 + 14 years, the majority were men (n = 68, 79%) with staphylococcus IE (n = 34, 40%). Cardiac troponins were elevated above the 99th percentile for 74 (86%) patients and > 10N for 25 (29%) patients. There was no statistically significant correlation between elevated cTn and the presence of an underlying coronary artery disease (Table 1). Cardiac troponin elevation above the 99th percentile was significantly associated with impaired renal function (P = 0.04) and staphylococcus infection (P = 0.02). A rise of cTn > 10N was significantly associated with acute pulmonary edema (P = 0.001), myocardial abscess (P = 0.01), staphylococcus (P = 0.0004), streptococcus (P = 0.008), and renal function (p = 0.0001). The average follow-up period was 919±816 days, and an elevation of cTn > 10 N had a clear prognostic impact (HR 2.38, 95%CI: 1.18–4.84, P = 0.01) (Fig. 1). Troponin elevation in IE is frequent and appears to be related to direct and indirect myocardial injury. It is associated with a poor prognosis. [ABSTRACT FROM AUTHOR]
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- 2021
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37. Epilepsy surgery in children with developmental tumours.
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García-Fernández M, Fournier-Del Castillo C, Ugalde-Canitrot A, Pérez-Jiménez A, Alvarez-Linera J, De Prada-Vicente I, Suárez-Rodríguez J, Bernabeu-Verdú J, and Villarejo-Ortega F
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- 2011
38. Myocardial Bridging is Significantly Related to Myocardial Infarction with Non-Obstructive Coronary Artery Disease.
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Matta, A., Nader, V., Canitrot, R., Delmas, C., Bouisset, F., Lhermusier, T., Blanco, S., Parada, F., Elbaz, M., Carrié, D., Galinier, M., and Roncalli, J.
- Abstract
Myocardial infarction with non obstructive coronary arteries (MINOCA) is a complex working diagnosis including coronary and non-coronary causes, like spontaneous coronary dissection, coronary thrombosis or embolism, myocarditis and cardiomyopathy. The prevalence of MINOCA is increasing, but the underlying etiology remains undetermined in more than 10% of cases. Hypotheses on the potential contributing role of myocardial bridge (MB) in takotsubo cardiomyopathy and coronary artery spasm (CAS) have been raised. We aim to investigate the relationship between MB and MINOCA. An observational retrospective study was conducted on 15,036 patients who had been referred for coronary angiography and who fulfilled the Definition of Myocardial Infarction. The study population was divided into STEMI and Non-STEMI patients, from which we defined two main groups: the MINOCA group and the coronary artery disease (CAD) group. The prevalence of MB was calculated in each group (Fig. 1). The distribution of angiographic MB among the groups was significantly greater in the MINOCA group (2.9% vs. 0.8%, P < 0.001). MINOCA accounted for 14.5% of spontaneous myocardial infarctions, and the clinical presentation was frequently NSTEMI rather than STEMI (84.3% vs. 15.7%, P < 0.001). Adjusted multivariate analyses showed a positive association between MB and MINOCA [OR = 3.28, 95% CI (2.34; 4.61) P < 0.001]. Cardiovascular risk factors were less common in the MINOCA population, which was younger and more often female. The main finding of the present study was that MB is an independent predictor for MINOCA, increasing the corresponding risk by threefold. Because MB prevalence differed significantly between the controls (CAD group) and in the MINOCA group, which was positively correlated to MB, it seems likely that MB would be a potential cause of MINOCA. Future prospective studies are necessary to highlight the physiologic significance of MB in some MINOCA patients. [ABSTRACT FROM AUTHOR]
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- 2022
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39. Functional study of multidrug resistance with fluorescent dyes. Limits of the assay for low levels of resistance and application in clinical samples
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Canitrot, Y., Lahmy, S., Buquen, J.-J., Canitrot, D., and Lautier, D.
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- 1996
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40. Quantifying DNA double-strand breaks induced by site-specific endonucleases in living cells by ligation-mediated purification
- Author
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Chailleux, Catherine, Aymard, François, Caron, Pierre, Daburon, Virginie, Courilleau, Céline, Canitrot, Yvan, Legube, Gaëlle, and Trouche, Didier
- Abstract
Recent advances in our understanding of the management and repair of DNA double-strand breaks (DSBs) rely on the study of targeted DSBs that have been induced in living cells by the controlled activity of site-specific endonucleases, usually recombinant restriction enzymes. Here we describe a protocol for quantifying these endonuclease-induced DSBs; this quantification is essential to an interpretation of how DSBs are managed and repaired. A biotinylated double-stranded oligonucleotide is ligated to enzyme-cleaved genomic DNA, allowing the purification of the cleaved DNA on streptavidin beads. The extent of cleavage is then quantified either by quantitative PCR (qPCR) at a given site or at multiple sites by genome-wide techniques (e.g., microarrays or high-throughput sequencing). This technique, named ligation-mediated purification, can be performed in 2 d. It is more accurate and sensitive than existing alternative methods, and it is compatible with genome-wide analysis. It allows the amount of endonuclease-mediated breaks to be precisely compared between two conditions or across the genome, thereby giving insight into the influence of a given factor or of various chromatin contexts on local repair parameters.
- Published
- 2014
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41. H2A.Z depletion impairs proliferation and viability but not DNA double-strand breaks repair in human immortalized and tumoral cell lines
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Taty-Taty, Gemael-Cedrick, Courilleau, Celine, Quaranta, Muriel, carayon, alexandre, chailleux, catherine, Aymard, Francois, Trouche, Didier, and Canitrot, Yvan
- Abstract
In mammalian cells, DNA double-strand breaks (DSB) can be repaired by 2 main pathways, homologous recombination (HR) and non-homologous end joining (NHEJ). To give access to DNA damage to the repair machinery the chromatin structure needs to be relaxed, and chromatin modifications play major roles in the control of these processes. Among the chromatin modifications, changes in nucleosome composition can influence DNA damage response as observed with the H2A.Z histone variant in yeast. In mammals, p400, an ATPase of the SWI/SNF family able to incorporate H2A.Z in chromatin, was found to be important for histone ubiquitination and BRCA1 recruitment around DSB or for HR in cooperation with Rad51. Recent data with 293T cells showed that mammalian H2A.Z is recruited to DSBs and is important to control DNA resection, therefore participating both in HR and NHEJ. Here we show that depletion of H2A.Z in the osteosarcoma U2OS cell line and in immortalized human fibroblasts does not change parameters of DNA DSB repair while affecting clonogenic ability and cell cycle distribution. In addition, no recruitment of H2A.Z around DSB can be detected in U2OS cells either after local laser irradiation or by chromatin immunoprecipitation. These data suggest that the role of H2A.Z in DSB repair is not ubiquitous in mammals. In addition, given that important cellular parameters, such as cell viability and cell cycle distribution, are more sensitive to H2A.Z depletion than DNA repair, our results underline the difficulty to investigate the role of versatile factors such as H2A.Z.
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- 2014
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42. Modulation of Cellular Response to Cisplatin by a Novel Inhibitor of DNA Polymerase β
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Boudsocq, F., Benaim, P., Canitrot, Y., Knibiehler, M., Ausseil, F., Capp, J. P., Bieth, A., Long, C., David, B., Shevelev, I., Frierich-Heinecken, E., Hübscher, U., Amalric, F., Massiot, G., Hoffmann, J. S., and Cazaux, C.
- Abstract
DNA polymerase β (Pol β) is an error-prone enzyme whose up-regulation has been shown to be a genetic instability enhancer as well as a contributor to cisplatin resistance in tumor cells. In this work, we describe the isolation of new Pol β inhibitors after high throughput screening of 8448 semipurified natural extracts. In vitro, the selected molecules affect specifically Pol β-mediated DNA synthesis compared with replicative extracts from cell nuclei. One of them, masticadienonic acid (MA), is particularly attractive because it perturbs neither the activity of the purified replicative Pol δ nor that of nuclear HeLa cell extracts. With an IC50 value of 8 µM, MA is the most potent of the Pol β inhibitors found so far. Docking simulation revealed that this molecule could substitute for single-strand DNA in the binding site of Pol β by binding Lys35, Lys68, and Lys60, which are the main residues involved in the interaction Pol β/single-strand DNA. Selected inhibitors also affect the Pol β-mediated translesion synthesis (TLS) across cisplatin adducts; MA was still the most efficient. Therefore, masticadienonic acid sensitized the cisplatin-resistant 2008C13*5.25 human tumor cells. Our data suggest that molecules such as masticadienonic acid could be suitable in conjunction with cisplatin to enhance anticancer treatments.
- Published
- 2005
43. p210 BCR/ABL kinase regulates nucleotide excision repair (NER) and resistance to UV radiation
- Author
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Canitrot, Yvan, Falinski, Rafal, Louat, Thierry, Laurent, Guy, Cazaux, Christophe, Hoffmann, Jean-Sébastien, Lautier, Dominique, and Skorski, Tomasz
- Abstract
Both clinical and experimental evidence illustrate that p190 and p210 BCR/ABL oncogenic tyrosine kinases induce resistance to DNA damage and confer an intrinsic genetic instability. Here, we investigated whether BCR/ABL expression could modulate nucleotide excision repair (NER). We found that ectopic expression of p210 BCR/ABL in murine lymphoid BaF3 cell line inhibited NER activity in vitro, promoting hypersensitivity of these cells to ultraviolet (UV) treatment and facilitating a mutator phenotype. However, expression of p210 BCR/ABL in human and murine myeloid cell lines and primary bone marrow cells resulted in the increased NER activity and resistance to UV irradiation. The ABL tyrosine kinase inhibitor STI571 reversed these effects, showing that p210 BCR/ABL tyrosine kinase activity is responsible for deregulation of NER. Hypoactivity of NER in p210 BCR/ABL-positive lymphoid cells was accompanied by the decreased interaction between proliferating cell nuclear antigen (PCNA) and xeroderma pigmentosum group B (XPB); conversely, this interaction was enhanced in p210 BCR/ABL-positive myeloid cells. p190 BCR/ABL did not affect NER in lymphoid and myeloid cells. In summary, our study suggests that p210 BCR/ABL reduced NER activity in lymphoid cells, leading to hypersensitivity to UV and mutagenesis. In contrast, p210 BCR/ABL expression in myeloid cells facilitated NER and induced resistance to UV. (Blood. 2003;102:2632-2637)
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- 2003
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44. DNA polymerase β imbalance increases apoptosis and mutagenesis induced by oxidative stress
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Fréchet, Mathilde, Canitrot, Yvan, Cazaux, Christophe, and Hoffmann, Jean-Sébastien
- Abstract
Oxidative stress has been proposed to be one of the major causes leading to the accumulation of mutation that is associated with the initiation and progression of cancers. Elevated expression of DNA polymerase β, an event found in many human tumors, has been shown to generate a mutator phenotype. Here, we demonstrated that overexpression of DNA polymerase β strengthens the mutagenicity of oxidative damages, concomitantly with a higher cellular sensitivity and increased apoptosis. Deregulated expression of DNA polymerase β could represent a predisposition factor for mutagenic effects of oxidative stress and thus have implication in the generation and/or evolution of cancer.
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- 2001
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45. Nucleotide excision repair DNA synthesis by excess DNA polymerase β: a potential source of genetic instability in cancer cells
- Author
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Canitrot, Yvan, Hoffmann, Jean-Sébastien, Calsou, Patrick, Hayakawa, Hiroshi, Salles, Bernard, and Cazaux, Christophe
- Abstract
The nucleotide excision repair pathway contributes to genetic stability by removing a wide range of DNA damage through an error‐free reaction. When the lesion is located, the altered strand is incised on both sides of the lesion and a damaged oligonucleotide excised. A repair patch is then synthesized and the repaired strand is ligated. It is assumed that only DNA polymerases δ and/or ε participate to the repair DNA synthesis step. Using UV and cisplatin‐modified DNA templates, we measured in vitrothat extracts from cells overexpressing the error‐prone DNA polymerase β exhibited a five‐to sixfold increase of the ultimate DNA synthesis activity compared with control extracts and demonstrated the specific involvement of Pol β in this step. By using a 28 nt gapped, double‐stranded DNA substrate mimicking the product of the incision step, we showed that Pol β is able to catalyze strand displacement downstream of the gap. We discuss these data within the scope of a hypothesis previously presented proposing that excess error‐prone Pol β in cancer cells could perturb the well‐defined specific functions of DNA polymerases during error‐free DNA transactions.—Canitrot, Y., Hoffmann, J.‐S., Calsou, P., Hayakawa, H., Salles, B., Cazaux, C. Nucleotide excision repair DNA synthesis by excess DNA polymerase β: a potential source of genetic instability in cancer cells. FASEB J.14, 1765–1774 (2000)
- Published
- 2000
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46. One-step microsurgery for acquired anterior glottic web.
- Author
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Garrel, R., Amy de La Bretèque, B., Canitrot, L., Frery, A., and Guerrier, B.
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- 2012
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47. Cross-resistance to ionizing radiation in a murine leukemic cell line resistant to cis-dichlorodiammineplatinum(II): role of Ku autoantigen.
- Author
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P, Frit, Y, Canitrot, C, Muller, N, Foray, P, Calsou, E, Marangoni, J, Bourhis, and B, Salles
- Abstract
cis-Dichlorodiammineplatinum(II) (CDDP; cisplatin) is commonly used in combination with ionizing radiation (IR) in the treatment of various malignancies. In vitro, many observations suggest that acquisition of CDDP resistance in cell lines confers cross-resistance to IR, but the molecular mechanisms involved have not been well documented yet. We report here the selection and characterization of a murine CDDP-resistant L1210 cell line (L1210/3R) that exhibits cross-resistance to IR because of an increased capacity to repair double-strand breaks compared with parental cells (L1210/P). In resistant cells, electrophoretic mobility shift assays revealed an increased DNA-end binding activity that could be ascribed, by supershifting the retardation complexes with antibodies, to the autoantigen Ku. The heterodimeric Ku protein, composed of 86-kDa (Ku80) and 70-kDa (Ku70) subunits, is the DNA-targeting component of DNA-dependent protein kinase (DNA-PK), which plays a critical role in mammalian DNA double-strand breaks repair. The increased Ku-binding activity in resistant cells was associated with an overexpression affecting specifically the Ku80 subunit. These data strongly suggest that the increase in Ku activity is responsible for the phenotype of cross-resistance to IR. In addition, these observations, along with previous results from DNA-PK- mutant cells, provide evidence in favor of a role of Ku/DNA-PK in resistance to CDDP. These results suggest that Ku activity may be an important molecular target in cancer therapy at the crossroad between cellular responses to CDDP and IR.
- Published
- 1999
48. Overexpression of DNA polymerase β: a genomic instability enhancer process
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Canitrot, Yvan, Fréchet, Mathilde, Servant, Laurence, Cazaux, Christophe, and Hoffmann, Jean‐Sébastien
- Abstract
DNA polymerase β (Pol β) is the most inaccurate of the six DNA polymerases found in mammalian cells. In a normal situation, it is expressed at a constant low level and its role is believed to be restricted to repair synthesis in the base excision repair pathway participating to the genome stability. However, excess of Pol β, found in some human tumors, could confer an increase in spontaneous mutagenesis and result in a highly mutagenic tolerance phenotype toward bifunctional DNA cross‐linking anticancer drugs. Here, we present a hypothesis on the mechanisms used by Pol β to be a genetic instability enhancer through its overexpression. We hypothesize that an excess of Pol β perturbs the well‐defined specific functions of DNA polymerases developed by the cell and propose Pol β‐mediated gap fillings during DNA transactions like repair, replication, or recombination pathways as key processes to introduce illegitimate deoxyribonucleotides or mutagenic base analogs like those produced by intracellular oxidative processes. These mechanisms may predominate during cellular nonproliferative phases in the absence of DNA replication.—Canitrot, Y., Fréchet, M., Servant, L., Cazaux, C., Hoffmann, J.‐S. Overexpression of DNApolymerase β: a genomic instability enhancer process. FASEB J.13, 1107–1111 (1999)
- Published
- 1999
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49. Pleural effusion, pulmonary embolism and seronegative rheumatoid arthritis.
- Author
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Martinez Muradas, J.A., Gonzalez-Barcala, F.J., Mosquera Martinez, J.A., Rodriguez Real, R., and Canitrot Andion, J.M.
- Subjects
RHEUMATOID arthritis ,AUTOIMMUNE diseases ,BLOOD hyperviscosity syndrome ,ARTHRITIS - Abstract
Summary: We present a case of empyema caused by overinfection of pleural fluid secondary to pulmonary thromboembolism, with negative progress, and the symptoms still persisting after optimum anticoagulant treatment. Given the patient′s negative progress, the possibility of an onset of rheumatoid arthritis (RA) is considered. The diagnosis of onset RA should be considered for unexplained pleural effusion, even though negative rheumatoid factor. [Copyright &y& Elsevier]
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- 2005
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50. Calcium homeostasis in guinea pig type-I vestibular hair cell: possible involvement of an Na^+-Ca^2^+ exchanger
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Chabbert, C., Canitrot, Y., Sans, A., and Lehouelleur, J.
- Published
- 1995
- Full Text
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