9 results on '"Laurent Morel"'
Search Results
2. Characterization of Tensile Stress-Dependent Directional Magnetic Incremental Permeability in Iron-Cobalt Magnetic Sheet: Towards Internal Stress Estimation through Non-Destructive Testing
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Borel Toutsop, Benjamin Ducharne, Mickael Lallart, Laurent Morel, and Pierre Tsafack
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magnetic control ,internal stress ,local characterization ,domain wall bulging ,multi-axis magnetization ,Chemical technology ,TP1-1185 - Abstract
Iron-Cobalt ferromagnetic alloys are promoted for electrical energy conversion in aeronautic applications, but their high magnetostrictive coefficients may result in undesired behaviors. Internal stresses can be tuned to limit magnetostriction but must be adequately assessed in a non-destructive way during production. For this, directional magnetic incremental permeability is proposed in this work. For academic purposes, internal stresses have been replaced by homogenous external stress, which is easier to control using traction/compression testbench and results in similar effects. Tests have been limited to tensile stress stimuli, the worst-case scenario for magnetic stress observation on positive magnetostriction coefficient materials. Hysteresis cycles have been reconstructed from the incremental permeability measurement for stability and reproducibility of the measured quantities. The directionality of the sensor provides an additional degree of freedom in the magnetic response observation. The study reveals that an angle of π/2 between the DC (Hsurf DC) and the AC (Hsurf AC) magnetic excitations with a flux density Ba at HsurfDC = 10 kA·m−1 constitute the ideal experimental situation and the highest correlated parameter to a homogeneous imposed tensile stress. Magnetic incremental permeability is linked to the magnetic domain wall bulging magnetization mechanism; this study thus provides insights for understanding such a mechanism.
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- 2022
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3. Absence of nuclear receptors LXRs impairs immune response to androgen deprivation and leads to prostate neoplasia.
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Laura Bousset, Amandine Septier, Julio Bunay, Allison Voisin, Rachel Guiton, Christelle Damon-Soubeyrant, Yoan Renaud, Angélique De Haze, Vincent Sapin, Anne Fogli, Amandine Rambur, Cyrille De Joussineau, Ayhan Kocer, Amalia Trousson, Joëlle Henry-Berger, Marcus Höring, Gerhard Liebisch, Silke Matysik, Jean-Marc A Lobaccaro, Laurent Morel, and Silvère Baron
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Biology (General) ,QH301-705.5 - Abstract
Chronic inflammation is now a well-known precursor for cancer development. Infectious prostatitis are the most common causes of prostate inflammation, but emerging evidence points the role of metabolic disorders as a potential source of cancer-related inflammation. Although the widely used treatment for prostate cancer based on androgen deprivation therapy (ADT) effectively decreases tumor size, it also causes profound alterations in immune tumor microenvironment within the prostate. Here, we demonstrate that prostates of a mouse model invalidated for nuclear receptors liver X receptors (LXRs), crucial lipid metabolism and inflammation integrators, respond in an unexpected way to androgen deprivation. Indeed, we observed profound alterations in immune cells composition, which was associated with chronic inflammation of the prostate. This was explained by the recruitment of phagocytosis-deficient macrophages leading to aberrant hyporesponse to castration. This phenotypic alteration was sufficient to allow prostatic neoplasia. Altogether, these data suggest that ADT and inflammation resulting from metabolic alterations interact to promote aberrant proliferation of epithelial prostate cells and development of neoplasia. This raises the question of the benefit of ADT for patients with metabolic disorders.
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- 2020
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4. Drosophila Accessory Gland: A Complementary In Vivo Model to Bring New Insight to Prostate Cancer
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Amandine Rambur, Marine Vialat, Claude Beaudoin, Corinne Lours-Calet, Jean-Marc Lobaccaro, Silvère Baron, Laurent Morel, and Cyrille de Joussineau
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prostate cancer ,Drosophila ,early tumorigenesis ,late tumorigenesis ,in vivo model ,Cytology ,QH573-671 - Abstract
Prostate cancer is the most common cancer in aging men. Despite recent progress, there are still few effective treatments to cure its aggressive and metastatic stages. A better understanding of the molecular mechanisms driving disease initiation and progression appears essential to support the development of more efficient therapies and improve patient care. To do so, multiple research models, such as cell culture and mouse models, have been developed over the years and have improved our comprehension of the biology of the disease. Recently, a new model has been added with the use of the Drosophila accessory gland. With a high level of conservation of major signaling pathways implicated in human disease, this functional equivalent of the prostate represents a powerful, inexpensive, and rapid in vivo model to study epithelial carcinogenesis. The purpose of this review is to quickly overview the existing prostate cancer models, including their strengths and limitations. In particular, we discuss how the Drosophila accessory gland can be integrated as a convenient complementary model by bringing new understanding in the mechanisms driving prostate epithelial tumorigenesis, from initiation to metastatic formation.
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- 2021
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5. InSAR tropospheric correction combining GNSS data and a global atmospheric model
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elisabeth simonetto, Frédéric Durand, Laurent Morel, Jean-Luc Froger, and Joëlle Nicolas
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Instruments and machines ,QA71-90 ,Applied optics. Photonics ,TA1501-1820 ,Cellular telephone services industry. Wireless telephone industry ,HE9713-9715 - Abstract
Les mesures issues de l'interférométrie d'images radar (InSAR), notamment satellitales, doivent être corrigées du délai dû à la propagation des ondes dans l'atmosphère. Plusieurs travaux ont déjà montré l'intérêt de cette correction. Cet article présente une méthode d'estimation de la phase troposphérique qui utilise à la fois des mesures GNSS (Global Navigation Satellite System) et un modèle d'atmosphère global (ERA-Interim). Pour évaluer cette méthode, nous comparons alors les mesures de déplacements interférométriques avant et après la correction avec les déplacements mesurés par GNSS, considérés comme référence. Les données utilisées pour les expériences sont acquises sur le Piton de la Fournaise en France.
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- 2018
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6. New Insights in Prostate Cancer Development and Tumor Therapy: Modulation of Nuclear Receptors and the Specific Role of Liver X Receptors
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Laura Bousset, Amandine Rambur, Allan Fouache, Julio Bunay, Laurent Morel, Jean-Marc A. Lobaccaro, Silvère Baron, Amalia Trousson, and Cyrille de Joussineau
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prostate cancer ,metastasis ,LXRs ,androgens ,estrogens ,cholesterol ,oxysterols ,signaling pathway ,Biology (General) ,QH301-705.5 ,Chemistry ,QD1-999 - Abstract
Prostate cancer (PCa) incidence has been dramatically increasing these last years in westernized countries. Though localized PCa is usually treated by radical prostatectomy, androgen deprivation therapy is preferred in locally advanced disease in combination with chemotherapy. Unfortunately, PCa goes into a castration-resistant state in the vast majority of the cases, leading to questions about the molecular mechanisms involving the steroids and their respective nuclear receptors in this relapse. Interestingly, liver X receptors (LXRα/NR1H3 and LXRβ/NR1H2) have emerged as new actors in prostate physiology, beyond their historical roles of cholesterol sensors. More importantly LXRs have been proposed to be good pharmacological targets in PCa. This rational has been based on numerous experiments performed in PCa cell lines and genetic animal models pointing out that using selective liver X receptor modulators (SLiMs) could actually be a good complementary therapy in patients with a castration resistant PCa. Hence, this review is focused on the interaction among the androgen receptors (AR/NR3C4), estrogen receptors (ERα/NR3A1 and ERβ/NR3A2), and LXRs in prostate homeostasis and their putative pharmacological modulations in parallel to the patients’ support.
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- 2018
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7. Chemical composition, antioxidant, anti-inflammatory and anti-proliferative activities of essential oils of plants from Burkina Faso.
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Bagora Bayala, Imaël Henri Nestor Bassole, Charlemagne Gnoula, Roger Nebie, Albert Yonli, Laurent Morel, Gilles Figueredo, Jean-Baptiste Nikiema, Jean-Marc A Lobaccaro, and Jacques Simpore
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Medicine ,Science - Abstract
This research highlights the chemical composition, antioxidant, anti-inflammatory and anti-proliferative activities of essential oils from leaves of Ocimum basilicum, Ocimum americanum, Hyptis spicigera, Lippia multiflora, Ageratum conyzoides, Eucalyptus camaldulensis and Zingiber officinale. Essential oils were analyzed by gas chromatography-mass spectrometry and gas chromatography-flame ionization detector. Major constituents were α-terpineol (59.78%) and β-caryophyllene (10.54%) for Ocimum basilicum; 1, 8-cineol (31.22%), camphor (12.730%), α-pinene (6.87%) and trans α-bergamotene (5.32%) for Ocimum americanum; β-caryophyllene (21%), α-pinene (20.11%), sabinene (10.26%), β-pinene (9.22%) and α-phellandrene (7.03%) for Hyptis spicigera; p-cymene (25.27%), β-caryophyllene (12.70%), thymol (11.88), γ-terpinene (9.17%) and thymyle acetate (7.64%) for Lippia multiflora; precocene (82.10%)for Ageratum conyzoides; eucalyptol (59.55%), α-pinene (9.17%) and limonene (8.76%) for Eucalyptus camaldulensis; arcurcumene (16.67%), camphene (12.70%), zingiberene (8.40%), β-bisabolene (7.83%) and β-sesquiphellandrène (5.34%) for Zingiber officinale. Antioxidant activities were examined using 1,1-diphenyl-2-picryl-hydrazyl (DPPH) and 2,2'-azinobis-(3-ethylbenzothiazoline-6-sulfonic acid (ABTS) methods. O. basilicum and L. multiflora exhibited the highest antioxidant activity in DPPH and ABTS tests, respectively. Anti-inflammatory properties were evaluated by measuring the inhibition of lipoxygenase activity and essential oil of Z. officinale was the most active. Anti-proliferative effect was assayed by the measurement of MTT on LNCaP and PC-3 prostate cancer cell lines, and SF-763 and SF-767 glioblastoma cell lines. Essential oils from A. conyzoides and L. multiflora were the most active on LNCaP and PC-3 cell lines, respectively. The SF-767 glioblastoma cell line was the most sensitive to O. basilicum and L. multiflora EOs while essential oil of A. conyzoides showed the highest activity on SF-763 cells. Altogether these results justify the use of these plants in traditional medicine in Burkina Faso and open a new field of investigation in the characterization of the molecules involved in anti-proliferative processes.
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- 2014
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8. NPM1 silencing reduces tumour growth and MAPK signalling in prostate cancer cells.
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Gaëlle Loubeau, Rafik Boudra, Sabrina Maquaire, Corinne Lours-Calet, Claude Beaudoin, Pierre Verrelle, and Laurent Morel
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Medicine ,Science - Abstract
The chaperone nucleophosmin (NPM1) is over-expressed in the epithelial compartment of prostate tumours compared to adjacent healthy epithelium and may represent one of the key actors that support the neoplastic phenotype of prostate adenocarcinoma cells. Yet, the mechanisms that underlie NPM1 mediated phenotype remain elusive in the prostate. To better understand NPM1 functions in prostate cancer cells, we sought to characterize its impact on prostate cancer cells behaviour and decipher the mechanisms by which it may act. Here we show that NPM1 favors prostate tumour cell migration, invasion and colony forming. Furthermore, knockdown of NPM1 leads to a decrease in the growth of LNCaP-derived tumours grafted in Nude mice in vivo. Such oncogenic-like properties are found in conjunction with a positive regulation of NPM1 on the ERK1/2 (Extracellular signal-Regulated Kinases 1/2) kinase phosphorylation in response to EGF (Epidermal Growth Factor) stimulus, which is critical for prostate cancer progression following the setting of an autonomous production of the growth factor. NPM1 could then be a target to switch off specifically ERK1/2 pathway activation in order to decrease or inhibit cancer cell growth and migration.
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- 2014
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9. Metal-NHC complexes: a survey of anti-cancer properties.
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Marie-Laure Teyssot, Anne-Sophie Jarrousse, Michèle Manin, Aurélien Chevry, Stéphane Roche, Frédéric Norre, Claude Beaudoin, Laurent Morel, Damien Boyer, Rachid Mahiou, and Arnaud Gautier
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METAL complexes ,ANTINEOPLASTIC agents ,CANCER chemotherapy ,METAL-ammonia compounds ,HETEROCYCLIC compounds ,CARBENES ,CELL-mediated cytotoxicity ,CISPLATIN - Abstract
New weapons to fight cancer are constantly needed. Among chemotherapeutics, anti-cancer metal-drugs have enjoyed a long and successful history since the discovery of the benchmark cisplatin. Advances in metal-drug discovery have motivated chemists to build plethora of complex structures. Among them, a novel area is emerging. This article presents a survey of the metal-N-Heterocyclic Carbenes (Ag(I), Au(I), Pd(II) and Cu(I)-NHCs) as potential anti-cancer agents. Most of the metal-NHCs considered display higher cytotoxicities than the reference metallo-drug cisplatin. Some of them are even selective for particular cell lines. Their mechanisms of action at the cellular level are further discussed, showing that the nature of the metal is of great importance. All these promising results demonstrate that this approach deserves more attention and work. [ABSTRACT FROM AUTHOR]
- Published
- 2009
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