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374 results on '"Gounon, P."'

1. A filter at the entrance of the Golgi that selects vesicles according to size and bulk lipid composition

Author

Maud Magdeleine, Romain Gautier, Pierre Gounon, Hélène Barelli, Stefano Vanni, and Bruno Antonny

Subjects
ALPS motif, membrane curvature, golgin, Golgi, transport vesicle, perforated cell, Medicine, Science, Biology (General), QH301-705.5
Abstract

When small phosphatidylcholine liposomes are added to perforated cells, they bind preferentially to the Golgi suggesting an exceptional avidity of this organelle for curved membranes without stereospecific interactions. We show that the cis golgin GMAP-210 accounts for this property. First, the liposome tethering properties of the Golgi resembles that of the amphipathic lipid-packing sensor (ALPS) motif of GMAP-210: both preferred small (radius < 40 nm) liposomes made of monounsaturated but not saturated lipids. Second, reducing GMAP-210 levels or redirecting its ALPS motif to mitochondria decreased liposome capture by the Golgi. Extensive mutagenesis analysis suggests that GMAP-210 tethers authentic transport vesicles via the same mechanism whereby the ALPS motif senses lipid-packing defects at the vesicle surface through its regularly spaced hydrophobic residues. We conclude that the Golgi uses GMAP-210 as a filter to select transport vesicles according to their size and bulk lipid composition.

Published
2016
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5. A Transcriptional Regulator of the LuxR-UhpA Family, FlcA, Controls Flocculation and Wheat Root Surface Colonization by Azospirillum brasilense Sp7

Author

Lily Pereg-Gerk, Annick Paquelin, Pierre Gounon, Ivan R. Kennedy, and Claudine Elmerich

Subjects
Microbiology, QR1-502, Botany, QK1-989
Abstract

Genetic complementation of a spontaneous mutant, impaired in flocculation, Congo red binding, and colonization of root surface, led to the identification of a new regulatory gene in Azospirillum brasilense Sp7, designated flcA. The deduced amino acid sequence of flcA shared high similarity with a family of transcriptional activators of the LuxR-UhpA family. The most significant match was with the AgmR protein, an activator for glycerol metabolism in Pseudomonas aeruginosa. Derivatives of Sp7 resulting from site-directed Tn5 mutagenesis in the flcA coding sequence were constructed by marker exchange. Characterization of the resulting mutant strains showed that flcA controls the production of capsular polysaccharides, the flocculation process in culture, and the colonization of the root surface of wheat. This study provides new information on the genetic control of the mechanism of plant root colonization by Azospirillum.

Published
1998
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8. Inflammatory monocytes and neutrophils are licensed to kill during memory responses in vivo.

Author

Emilie Narni-Mancinelli, Saidi M'Homa Soudja, Karine Crozat, Marc Dalod, Pierre Gounon, Frédéric Geissmann, and Grégoire Lauvau

Subjects
Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5
Abstract

Immunological memory is a hallmark of B and T lymphocytes that have undergone a previous encounter with a given antigen. It is assumed that memory cells mediate better protection of the host upon re-infection because of improved effector functions such as antibody production, cytotoxic activity and cytokine secretion. In contrast to cells of the adaptive immune system, innate immune cells are believed to exhibit a comparable functional effector response each time the same pathogen is encountered. Here, using mice infected by the intracellular bacterium Listeria monocytogenes, we show that during a recall bacterial infection, the chemokine CCL3 secreted by memory CD8+ T cells drives drastic modifications of the functional properties of several populations of phagocytes. We found that inflammatory ly6C+ monocytes and neutrophils largely mediated memory CD8+ T cell bacteriocidal activity by producing increased levels of reactive oxygen species (ROS), augmenting the pH of their phagosomes and inducing antimicrobial autophagy. These events allowed an extremely rapid control of bacterial growth in vivo and accounted for protective immunity. Therefore, our results provide evidence that cytotoxic memory CD8+ T cells can license distinct antimicrobial effector mechanisms of innate cells to efficiently clear pathogens.

Published
2011
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9. Bacillus sphaericus binary toxin elicits host cell autophagy as a response to intoxication.

Author

Onya Opota, Nils C Gauthier, Anne Doye, Colin Berry, Pierre Gounon, Emmanuel Lemichez, and David Pauron

Subjects
Medicine, Science
Abstract

Bacillus sphaericus strains that produce the binary toxin (Bin) are highly toxic to Culex and Anopheles mosquitoes, and have been used since the late 1980s as a biopesticide for the control of these vectors of infectious disease agents. The Bin toxin produced by these strains targets mosquito larval midgut epithelial cells where it binds to Cpm1 (Culex pipiens maltase 1) a digestive enzyme, and causes severe intracellular damage, including a dramatic cytoplasmic vacuolation. The intoxication of mammalian epithelial MDCK cells engineered to express Cpm1 mimics the cytopathologies observed in mosquito enterocytes following Bin ingestion: pore formation and vacuolation. In this study we demonstrate that Bin-induced vacuolisation is a transient phenomenon that affects autolysosomes. In addition, we show that this vacuolisation is associated with induction of autophagy in intoxicated cells. Furthermore, we report that after internalization, Bin reaches the recycling endosomes but is not localized either within the vacuolating autolysosomes or within any other degradative compartment. Our observations reveal that Bin elicits autophagy as the cell's response to intoxication while protecting itself from degradation through trafficking towards the recycling pathways.

Published
2011
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10. Direct visualization of peptide/MHC complexes at the surface and in the intracellular compartments of cells infected in vivo by Leishmania major.

Author

Eric Muraille, Pierre Gounon, Julie Cazareth, Johan Hoebeke, Christoph Lippuner, Ana Davalos-Misslitz, Toni Aebischer, Sylviane Muller, Nicolas Glaichenhaus, and Evelyne Mougneau

Subjects
Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5
Abstract

Protozoa and bacteria infect various types of phagocytic cells including macrophages, monocytes, dendritic cells and eosinophils. However, it is not clear which of these cells process and present microbial antigens in vivo and in which cellular compartments parasite peptides are loaded onto Major Histocompatibility Complex molecules. To address these issues, we have infected susceptible BALB/c (H-2d) mice with a recombinant Leishmania major parasite expressing a fluorescent tracer. To directly visualize the antigen presenting cells that present parasite-derived peptides to CD4+ T cells, we have generated a monoclonal antibody that reacts to an antigenic peptide derived from the parasite LACK antigen bound to I-Ad Major Histocompatibility Complex class II molecule. Immunogold electron microscopic analysis of in vivo infected cells showed that intracellular I-Ad/LACK complexes were present in the membrane of amastigote-containing phagosomes in dendritic cells, eosinophils and macrophages/monocytes. In both dendritic cells and macrophages, these complexes were also present in smaller vesicles that did not contain amastigote. The presence of I-Ad/LACK complexes at the surface of dendritic cells, but neither on the plasma membrane of macrophages nor eosinophils was independently confirmed by flow cytometry and by incubating sorted phagocytes with highly sensitive LACK-specific hybridomas. Altogether, our results suggest that peptides derived from Leishmania proteins are loaded onto Major Histocompatibility Complex class II molecules in the phagosomes of infected phagocytes. Although these complexes are transported to the cell surface in dendritic cells, therefore allowing the stimulation of parasite-specific CD4+ T cells, this does not occur in other phagocytic cells. To our knowledge, this is the first study in which Major Histocompatibility Complex class II molecules bound to peptides derived from a parasite protein have been visualized within and at the surface of cells that were infected in vivo.

Published
2010
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13. Acadesine kills chronic myelogenous leukemia (CML) cells through PKC-dependent induction of autophagic cell death.

Author

Guillaume Robert, Issam Ben Sahra, Alexandre Puissant, Pascal Colosetti, Nathalie Belhacene, Pierre Gounon, Paul Hofman, Fréderic Bost, Jill-Patrice Cassuto, and Patrick Auberger

Subjects
Medicine, Science
Abstract

CML is an hematopoietic stem cell disease characterized by the t(9;22) (q34;q11) translocation encoding the oncoprotein p210BCR-ABL. The effect of acadesine (AICAR, 5-Aminoimidazole-4-carboxamide-1-beta-D-ribofuranoside) a compound with known antileukemic effect on B cell chronic lymphoblastic leukemia (B-CLL) was investigated in different CML cell lines. Acadesine triggered loss of cell metabolism in K562, LAMA-84 and JURL-MK1 and was also effective in killing imatinib-resistant K562 cells and Ba/F3 cells carrying the T315I-BCR-ABL mutation. The anti-leukemic effect of acadesine did not involve apoptosis but required rather induction of autophagic cell death. AMPK knock-down by Sh-RNA failed to prevent the effect of acadesine, indicating an AMPK-independent mechanism. The effect of acadesine was abrogated by GF109203X and Ro-32-0432, both inhibitor of classical and new PKCs and accordingly, acadesine triggered relocation and activation of several PKC isoforms in K562 cells. In addition, this compound exhibited a potent anti-leukemic effect in clonogenic assays of CML cells in methyl cellulose and in a xenograft model of K562 cells in nude mice. In conclusion, our work identifies an original and unexpected mechanism by which acadesine triggers autophagic cell death through PKC activation. Therefore, in addition to its promising effects in B-CLL, acadesine might also be beneficial for Imatinib-resistant CML patients.

Published
2009
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21. P2-8 - Infections sexuellement transmissibles chez les travailleuses du sexe au Togo - Prévalence et prise en charge syndromique

Author

Youa, Y.F., Bitty-Anderson, A., Gounon, K.H., Junior Sadio, A., Dagnra, A., and Ekouevi, K.

Abstract

L'approche syndromique est une recommandation de l'Organisation mondiale de la santé (OMS) pour le traitement des infections sexuellement transmissibles (IST) dans les pays à faibles capacités de diagnostic biologique. Peu de données sont disponibles sur cette approche au Togo. L'objectif de cette étude était de décrire la prise en charge des IST basée sur l'approche syndromique chez les travailleuses du sexe (TS) au Togo en 2023.

Published
2024
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22. 1-6 - Rétention dans les soins VIH pédiatriques au Togo en 2022 et analyse des facteurs associés par estimation des temps de survie moyens restreints ajustés

Author

Sadio, A.J., Gbeasor-Komlanvi, F.A., Bakoubayi, A.W., Gounon, H.K., Dagnra, A.C., and Ekouevi, D.

Abstract

La faible rétention dans les soins VIH constitue un obstacle à la réalisation des objectifs 3X95 de l'ONUSIDA. L'objectif de cette étude était de décrire la rétention dans les soins des enfants vivant avec le VIH (EVVIH) et ses facteurs associés au Togo en 2022.

Published
2024
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27. Proposition d’un modèle de tutorat pour la conception de dispositifs d’accompagnement en formation en ligne

Author

Patricia Gounon, Pascal Leroux, and Xavier Dubourg

Subjects
Education, Special aspects of education, LC8-6691
Abstract

Nous avons constaté dans la littérature le manque de prise en compte de l’accompagnement des apprenants dans la conception des dispositifs de formation en ligne. Ce manque nous semble très préjudiciable dans le cycle de vie d’une formation. C’est pourquoi, après avoir identifié les besoins d’accompagnement des apprenants dans une formation en ligne, nous proposons un modèle descriptif d’une activité de tutorat. Ce modèle sert de fondement pour guider la définition des spécifications du dispositif d’accompagnement des apprenants en matière de tâches et d’outils supports de leurs activités. Dans la dernière partie de l’article, nous présentons la méthodologie d’application de ce modèle au cours du cycle de vie d’une formation.

Published
2004
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30. Dev Cell

Author

Al-Hasani K, Pfeifer A, Courtney M, Ben-Othman N, Gjernes E, Vieira A, Druelle N, Avolio F, Ravassard P, Leuckx G, Lacas-Gervais S, Ambrosetti D, Benizri E, Hecksher-Sorensen J, Gounon P, Ferrer J, Gradwohl G, Heimberg H, Mansouri A, and Collombat P.

Published
2013

34. Décrire l'accompagnement des apprenants - Proposition d'une extension du langage de modélisation pédagogique IMS-Learning Design

Author

Gounon, P., Leroux, P., Dubourg, X., meignier, sylvain, Laboratoire d'Informatique de l'Université du Maine (LIUM), and Le Mans Université (UM)-Centre National de la Recherche Scientifique (CNRS)

Subjects
dispositif d'accompagnement des apprenants, IMS-Learning Design, [INFO.EIAH]Computer Science [cs]/Technology for Human Learning, [INFO] Computer Science [cs], modèle de tutorat, ComputingMilieux_MISCELLANEOUS, langage de modélisation pédagogique, EML
Abstract

L'objectif de cet article est de proposer une modification du langage de modélisation pédagogique IMS-Learning Design en termes de description d'une activité d'accompagnement des apprenants et de la spécification des rôles des acteurs participant à cette activité. Les modifications apportées s'appuient sur un modèle d'organisation du tutorat que nous avons défini. Ce modèle a pour objectifs (1) d'organiser les tâches entre les acteurs tuteur et apprenants, (2) d'assurer auprès des apprenants un accompagnement adapté à la situation d'apprentissage et (3) de spécifier les outils support à l'activité des acteurs de la formation.

Published
2005

36. False alarm reduction for the buried mine detection

Author

Ginolhac, Guillaume, Gounon, P., Ioan, S., Hetet, A., Groupe d'Electromagnétisme Appliqué (GEA), Université Paris Nanterre (UPN), and Ginolhac, Guillaume

Subjects
Alarm, ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2003

38. Interaction between the protein InIB of Listeria monocytogenes and lipoteichoic acid: a novel mechanism of protein association at the surface of gram-positive bacteria

Author

Jonquières, R., Helene Bierne, Fiedler, F., Gounon, P., Pascale Cossart, Unité de recherche Génétique Microbienne (UGM), Institut National de la Recherche Agronomique (INRA), and ProdInra, Migration

Subjects
[SDV.MP]Life Sciences [q-bio]/Microbiology and Parasitology, [SDV.MP] Life Sciences [q-bio]/Microbiology and Parasitology
Published
1999

41. Influence of Viscous Lubricant on Nucleation and Propagation of Frictional Ruptures

Author

Paglialunga, F., Passelègue, F., Latour, S., Gounon, A., and Violay, M.

Abstract

Fluids are pervasive in the Earth's crust and saturate fractures and faults. The combination of fluids and gouge layers developing along faults can generate fluids of different viscosities. Such viscous fluids were found to influence the reactivation, frictional stability of faults, and eventually the dynamics of propagating earthquake ruptures. We reproduced laboratory earthquakes on analog material (PMMA) to study the influence of viscous lubricant on fault frictional stability, rupture nucleation, and propagation under mixed lubrication conditions. Experiments were conducted in dry conditions, and with fluids presenting a viscosity ranging from 1 to 1,000 mPa.s. Through photoelasticity, high‐frequency strain gauge sensors, and accelerometer measurements, we obtained new insights about the influence of lubricant on a characteristic nucleation length, rupture propagation velocity, and local slip and slip rate evolution during the reproduced frictional ruptures. Our experiments show that the presence of a lubricant generating mixed lubricated conditions along the fault induces, (a) a reduction of the frictional resistance, (b) an increase in nucleation length, (c) a decrease in the fracture energy. In addition, the larger the viscosity of the fluids, the larger the reduction of frictional strength and the increase in the nucleation length. Moreover, ruptures occurring under mixed lubricated conditions showed a pulse‐like rather than crack‐like behavior, suggesting that viscous lubrication can induce the transition from crack‐like to pulse‐like rupture along natural faults. We demonstrate, supported by existing theory, that this transition is mainly governed by the stress acting on the fault at the onset of nucleation, which is drastically reduced in presence of a lubricant. Fluids naturally permeating the Earth's crust or being injected for reservoir stimulation can promote fault reactivation, resulting in natural or so‐called induced earthquakes. It is important to comprehend how the presence of these fluids, as well as their properties, affect the activation and magnitude of seismic events. In particular, we investigated the role of fluid viscosity under controlled experimental conditions through laboratory experiments on analog material. We show that for the same applied normal stress, faults under lubricated conditions (i.e., where a thin film of viscous lubricant had been spread) can be activated at much lower shear stresses than dry faults. At the same time, the generated events will be much smaller in magnitude (i.e., smaller stress drop) and propagate more stably. Frictional strength of lubricated artificial interfaces is dramatically reduced under mixed lubrication conditionsNucleation length of rupture under lubricated conditions is larger than the one of ruptures under dry conditionsViscous lubrication (under mixed conditions) can affect the nature of ruptures that would propagated pulse‐like rather than crack‐like Frictional strength of lubricated artificial interfaces is dramatically reduced under mixed lubrication conditions Nucleation length of rupture under lubricated conditions is larger than the one of ruptures under dry conditions Viscous lubrication (under mixed conditions) can affect the nature of ruptures that would propagated pulse‐like rather than crack‐like

Published
2023
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42. Metformin inhibits melanoma development through autophagy and apoptosis mechanisms

Author

Tomic, T, primary, Botton, T, additional, Cerezo, M, additional, Robert, G, additional, Luciano, F, additional, Puissant, A, additional, Gounon, P, additional, Allegra, M, additional, Bertolotto, C, additional, Bereder, J-M, additional, Tartare-Deckert, S, additional, Bahadoran, P, additional, Auberger, P, additional, Ballotti, R, additional, and Rocchi, S, additional

Published
2011
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44. miR-210 is overexpressed in late stages of lung cancer and mediates mitochondrial alterations associated with modulation of HIF-1 activity

Author

Puisségur, M-P, primary, Mazure, N M, additional, Bertero, T, additional, Pradelli, L, additional, Grosso, S, additional, Robbe-Sermesant, K, additional, Maurin, T, additional, Lebrigand, K, additional, Cardinaud, B, additional, Hofman, V, additional, Fourre, S, additional, Magnone, V, additional, Ricci, J E, additional, Pouysségur, J, additional, Gounon, P, additional, Hofman, P, additional, Barbry, P, additional, and Mari, B, additional

Published
2010
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45. 789 ROLE OF THE AUTOPHAGY IN HEPATOCYTE DEATH IN NONALCOHOLIC FATTY LIVER DISEASE (NAFLD): STUDY IN VITRO, IN MICE AND IN HUMANS

Author

Lavallard, V., primary, Bonnafous, S., additional, Rousseau, D., additional, Bailly-Maitre, B., additional, Anty, R., additional, Saint-Paul, M.-C., additional, Sadoul, J.-L., additional, Ianelli, A., additional, Deveaux, V., additional, Lotersztajn, S., additional, Gounon, P., additional, Gugenheim, J., additional, Le Marchand-Brustel, Y., additional, Tran, A., additional, and Gual, P., additional

Published
2010
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