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1. GPATCH11 variants cause mis-splicing and early-onset retinal dystrophy with neurological impairment

Author

Zanetti, Andrea, Dujardin, Gwendal, Fares-Taie, Lucas, Amiel, Jeanne, Roger, Jérôme E., Audo, Isabelle, Robert, Matthieu P., David, Pierre, Jung, Vincent, Goudin, Nicolas, Guerrera, Ida Chiara, Moriceau, Stéphanie, Amana, Danielle, Assia Batzir, Nurit, Bachar-Zipori, Anat, Basel Salmon, Lina, Boddaert, Nathalie, Briault, Sylvain, Bruel, Ange-Line, Costet-Fighiera, Christine, Coutinho Santos, Luisa, Gitiaux, Cyril, Kaminska, Karolina, Kuentz, Paul, Orenstein, Naama, Philip-Sarles, Nicole, Plutino, Morgane, Quinodoz, Mathieu, Santos, Cristina, Sigaudy, Sabine, Soeiro e Sá, Mariana, Sofrin, Efrat, Sousa, Ana Berta, Sousa-Luis, Rui, Thauvin-Robinet, Christel, van Dijk, Erwin L., Zaafrane-Khachnaoui, Khaoula, Zur, Dinah, Kaplan, Josseline, Rivolta, Carlo, Rozet, Jean-Michel, and Perrault, Isabelle

Published
2024
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3. Anti–IL-4R versus anti–IL-5/5R after anti–IL-5/5R failure in asthma: An emulated target trial

Author

Devouassoux, G., Taillé, C., Chanez, P., Bonniaud, P., Bourdin, A., Saint Raymond, C., Maurer, C., Beurnier, A., Roux, P., Margelidon, V., Boudjemaa, A., Mangiapan, G., Freymond, N., Didi, T., Russier, M., Garcia, G., Meyer, E. Popin, Dupin, C., Fouquet, F., Jouveshomme, S., Gaspard, W., Dury, S., Maillard, S. Habib, Izadifar, A., Cuvillon, E., Deslée, G., Barnig, C., Perotin, J.M., Gamez, A.S., Oster, J.P., Khayat, N., Chenivesse, C., Li, X., Appere de Vecchi, C., Gicquello, A., Rami, H., Vignal, G., Just, N., Blanc, X., Leroyer, C., Wemeau, L., Achkar, A., Sattler, C., Catherinot, E., Guilleminault, L., Gaillot-Drevon, M., Rochefort-Morel, C., Couturaud, F., Martin, P., Chabrol, A., Pegliasco, H., Sése, L., Romanet, S., Caverstri, B., Tcherakian, C., Magnan, A., Ahmed, E., Allibe, F., Beltramo, G., Michaux, K., Paleiron, N., Martinez, S., Begne, C., Tummino, C., Givel, C., Mourin, G., Salvator, H., Volpato, M., Drucbert, M., Rossignoli, N., Keddache, S., Justet, A., Andrejak, C., Valcke, J., Perrin, J., Mercy, M., Jouvenot, M., Soumagne, T., Elharrar, X., Douvry, B., Godbert, B., Maitre, B., Goyard, C., Didier, A., Cadet, E., Chabot, F., Gonzalez, J., Mattei, L., Gouitaa, M., Chauveau, S., Raymond, S., Dirou, S., Fry, S., Briault, A., Moui, A., Paris, A., NoelSavina, E., Olivier, C., Caradec, E., Roche, N., Picart, G., Belmont, L., Portel, L., Serra, M. Rocca, Guibert, N., Jean, R., Hadjadj, S., Guillo, S., Gauquelin, L., Estellat, C., Prigent, A., Larrousse, M., Jaffuel, D., Bourayou, Karima, Klising, Eve, Yelles, Nessima, Pochon, Sarra, Gouider, Amal, Medina, Hadj Kaci, Yasmine, Sellali, Djouher, Dahmani, Ndao, Diakhou, Vacher, Yannick, Achkar, Antoine, Ahmed, Engi, Alain, Didier, Allibe, Flora, Andrejak, Claire, De Vecchi, Corinne Appere, Barnig, Cindy, Begne, Camille, Belmont, Laure, Beltramo, Guillaume, Blanc, Xavier, Briault, Amandine, Cadet, Emmanuelle, Caradec, Emmanuela, Catherinot, Émilie, Cavestri, Beatrice, Chabrol, Alexandre, Chanez, Pascal, Chauveau, Simon, Couturaud, Francis, Cuvillon, Édouard, Deslee, Gaëtan, Didi, Toufik, Dirou, Stéphanie, Douvry, benoît, Drucbert, Mélanie, Dupin, Clairelyne, Dury, Sandra, Elharrar, Xavier, Fouquet, Helen, Freymond, Nathalie, Fry, Stéphanie, Gaillot-Drevon, Maud, Gamez, Anne Sophie, Garcia, Gilles, Gaspard, Wanda, Gicquello, Alice, Givel, Claire, Godbert, benoit, Gonzalez, Jésus, Gouitaa, Marion, Goupil, François, Goyard, Céline, Guibert, Nicolas, Guilleminault, Laurent, Habib-Maillard, Stéphanie, Hadjadj, Samra, Izadifar, Armine, Jean, Romain, Jouvenot, marie, Jouveshomme, Stéphane, Just, Nicolas, Justet, Aurélien, Keddache, Sophia, Khayath, Naji, Lemaire, Bertrand, Leroyer, Christophe, Li, Xing, Magnan, Antoine, Maitre, Bernard, Mangiapan, Gilles, Margelidon, Victor, Martin, Pascale, Martinez, Stéphanie, Mattei, Laura, Maurer, Cyril, Mercy, Magalie, Michaux, Karine, Moui, Antoine, Mourin, Gisèle, Noel-Savina, Elisa, Olivier, Cécile, Oster, Jean-Philippe, Paleiron, Nicolas, Paris, Audrey, Pegliasco, Hervé, Perotin Collard, Jeanne-Marie, Perrin, Julie, Picart, Gaël, Pison, Christophe, Popin-Meyer, Élisabeth, Portel, Laurent, Rami, Hassina, Raymond, Stéphane, Serra, Mireille Rocca, Rochefort-Morel, Cécile, Romanet, Stéphanie, Rossignoli, Nadine, Roux, Pauline, Russier, Maud, Saint-Raymond, Christel, Salmeron, Sergio, Salvator, Helene, Sattler, Caroline, Sese, Lucile, Soumagne, Thibaud, Tcherakian, Colas, Tiotiu, Angélica, Tummino, Céline, Valcke-Brossollet, Judith, Vignal, Guillaume, Volpato, Mathilde, Wemeau, Lidwine, Valery, Solène, Simon-Tillaux, Noémie, Devouassoux, Gilles, Bonniaud, Philippe, Beurnier, Antoine, Boudjemaa, Amel, Chenivesse, Cécile, Bourdin, Arnaud, Gauquelin, Lisa, Guillo, Sylvie, Taillé, Camille, and Estellat, Candice

Published
2024
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9. Tracheobronchopathia osteochondroplastica: clinical, bronchoscopic, and comorbid features in a case series

Author

Antoine Dumazet, Claire Launois, Francois Lebargy, Romain Kessler, Hervé Vallerand, Pierre Schmitt, Christophe Hermant, Sandra Dury, Maxime Dewolf, Julien Dutilh, Maher Abouda, Marion Ferreira, Ihab Atallah, Samy Lachkar, Jérémy Charriot, Stéphane Jouneau, Yurdagul Uzunhan, Stéphane Chouabe, Benjamin Coiffard, Hervé Dutau, Jean Hagenburg, Amandine Briault, Valérian Dormoy, Marion Lirsac, Jean-Michel Vergnon, Gaetan Deslee, and Jeanne-Marie Perotin

Subjects
Tracheobronchopathia osteochondroplastica, Bronchoscopy, Tracheal stenosis, Case report, Diseases of the respiratory system, RC705-779
Abstract

Abstract Background Tracheobronchopathia osteochondroplastica (TO) is a rare condition of unknown etiology. TO is characterized by submucosal nodules, with or without calcifications, protruding in the anterolateral walls of the trachea and proximal bronchi. The objective of this study was to describe TO features and associated comorbidities in a series of patients. Methods Patients suffering from TO were retrospectively included by investigators from the Groupe d’Endoscopie Thoracique et Interventionnelle Francophone (GETIF). Demographic, clinical, comorbidities, bronchoscopic, functional, and radiological characteristics, and outcomes were recorded and analyzed. Results Thirty-six patients were included (69% male with a mean of 65 ± 12 years). Chronic symptoms were described by 81% of patients including cough (74%) and dyspnea on exertion (74%). TO was associated with COPD in 19% of the cases and gastroesophageal reflux disease in 6%. A mild to severe airflow obstruction was present in 55% of the cases. CT scan showed tracheal submucosal nodules in 93% of patients and tracheal stenosis in 17%. Bronchoscopy identified TO lesions in the trachea in 65% of the cases, and 66% of them were scattered. A bronchoscopic reevaluation was performed in 7 cases, 9 ± 14 months [1–56] after initial diagnosis, and showed the stability of lesions in all cases. Three patients underwent interventional bronchoscopic treatment. Conclusion The diagnosis of TO relies on typical bronchoscopic findings and can be evoked on a CT scan. Histologic diagnosis can be useful in atypical cases for differential diagnosis. Given its low consequences in terms of symptoms, lung functions, and evolution, no treatment is usually required.

Published
2022
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10. Large-conductance calcium-activated potassium channel haploinsufficiency leads to sensory deficits in the visual system: a case report

Author

Olivier Perche, Fabien Lesne, Alain Patat, Susanne Raab, Roy Twyman, Robert H. Ring, and Sylvain Briault

Subjects
BKCa, KCNMA1, Electroretinography, Contrast sensitivity, Case report, Medicine
Abstract

Abstract Background Mutations in the genes encoding the large-conductance calcium-activated potassium channel, especially KCNMA1 encoding its α-subunit, have been linked to several neurological features, including intellectual disability or autism. Associated with neurodevelopmental phenotypes, sensory function disturbances are considered to be important clinical features contributing to a variety of behavioral impairments. Large-conductance calcium-activated potassium channels are important in regulating neurotransmission in sensory circuits, including visual pathways. Deficits in visual function can contribute substantially to poor quality of life, while therapeutic approaches aimed at addressing such visual deficits represent opportunities to improve neurocognitive and neurobehavioral outcomes. Case presentation We describe the case of a 25-year-old Caucasian male with autism spectrum disorder and severe intellectual disability presenting large-conductance calcium-activated potassium channel haploinsufficiency due to a de novo balanced translocation (46, XY, t [9; 10] [q23;q22]) disrupting the KCNMA1 gene. The visual processing pathway of the subject was evaluated using both electroretinography and visual contrast sensitivity, indicating that both retinal bipolar cell function and contrast discrimination performance were reduced by approximately 60% compared with normative control values. These findings imply a direct link between KCNMA1 gene disruption and visual dysfunction in humans. In addition, the subject reported photophobia but did not exhibit strabismus, nystagmus, or other visual findings on physical examination. Conclusions This case study of a subject with large-conductance calcium-activated potassium channel haploinsufficiency and photophobia revealed a visual pathway deficit at least at the retinal level, with diminished retinal light capture likely due to bipolar cell dysfunction and an associated loss of contrast sensitivity. The data suggest that large-conductance calcium-activated potassium channels play an important role in the normal functioning of the visual pathway in humans, and that their disruption may play a role in visual and other sensory system symptomatology in large-conductance calcium-activated potassium channelopathies or conditions where disruption of large-conductance calcium-activated potassium channel function is a relevant feature of the pathophysiology, such as fragile X syndrome. This work suggests that the combined use of physiological (electroretinography) and functional (contrast sensitivity) approaches may have utility as a biomarker strategy for identifying and characterizing visual processing deficits in individuals with large-conductance calcium-activated potassium channelopathy. Trial registration ID-RCB number 2019-A01015-52, registered 17/05/2019.

Published
2022
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11. STING agonist diABZI induces PANoptosis and DNA mediated acute respiratory distress syndrome (ARDS)

Author

Yasmine Messaoud-Nacer, Elodie Culerier, Stéphanie Rose, Isabelle Maillet, Nathalie Rouxel, Sylvain Briault, Bernhard Ryffel, Valerie F. J. Quesniaux, and Dieudonnée Togbe

Subjects
Cytology, QH573-671
Abstract

Abstract Stimulator of interferon genes (STING) contributes to immune responses against tumors and may control viral infection including SARS-CoV-2 infection. However, activation of the STING pathway by airway silica or smoke exposure leads to cell death, self-dsDNA release, and STING/type I IFN dependent acute lung inflammation/ARDS. The inflammatory response induced by a synthetic non-nucleotide-based diABZI STING agonist, in comparison to the natural cyclic dinucleotide cGAMP, is unknown. A low dose of diABZI (1 µg by endotracheal route for 3 consecutive days) triggered an acute neutrophilic inflammation, disruption of the respiratory barrier, DNA release with NET formation, PANoptosis cell death, and inflammatory cytokines with type I IFN dependent acute lung inflammation. Downstream upregulation of DNA sensors including cGAS, DDX41, IFI204, as well as NLRP3 and AIM2 inflammasomes, suggested a secondary inflammatory response to dsDNA as a danger signal. DNase I treatment, inhibition of NET formation together with an investigation in gene-deficient mice highlighted extracellular DNA and TLR9, but not cGAS, as central to diABZI-induced neutrophilic response. Therefore, activation of acute cell death with DNA release may lead to ARDS which may be modeled by diABZI. These results show that airway targeting by STING activator as a therapeutic strategy for infection may enhance lung inflammation with severe ARDS. STING agonist diABZI induces neutrophilic lung inflammation and PANoptosis A, Airway STING priming induce a neutrophilic lung inflammation with epithelial barrier damage, double-stranded DNA release in the bronchoalvelolar space, cell death, NETosis and type I interferon release. B, 1. The diamidobenzimidazole (diABZI), a STING agonist is internalized into the cytoplasm through unknown receptor and induce the activation and dimerization of STING followed by TBK1/IRF3 phosporylation leading to type I IFN response. STING activation also leads to NF-kB activation and the production of pro-inflammatory cytokines TNFα and IL-6. 2. The activation of TNFR1 and IFNAR1 signaling pathway results in ZBP1 and RIPK3/ASC/CASP8 activation leading to MLKL phosphorylation and necroptosis induction. 3. This can also leads to Caspase-3 cleavage and apoptosis induction. 4. Self-dsDNA or mtDNA sensing by NLRP3 or AIM2 induces inflammsome formation leading to Gasdermin D cleavage enabling Gasdermin D pore formation and the release mature IL-1β and pyroptosis. NLRP3 inflammasome formation can be enhanced by the ZBP1/RIPK3/CASP8 complex. 5. A second signal of STING activation with diABZI induces cell death and the release of self-DNA which is sensed by cGAS and form 2′3′-cGAMP leading to STING hyper activation, the amplification of TBK1/IRF3 and NF-kB pathway and the subsequent production of IFN-I and inflammatory TNFα and IL-6. This also leads to IFI204 and DDX41 upregulation thus, amplifying the inflammatory loop. The upregulation of apoptosis, pyroptosis and necroptosis is indicative of STING-dependent PANoptosis.

Published
2022
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12. Anti-IL-4R versus Anti-IL-5/5R after Anti-IL-5/5R failure in asthma: an emulated target trial

Author

Valery, Solène, primary, Simon-Tillaux, Noémie, additional, Devouassoux, Gilles, additional, Bonniaud, Philippe, additional, Beurnier, Antoine, additional, Boudjemaa, Amel, additional, Chenivesse, Cécile, additional, Bourdin, Arnaud, additional, Gauquelin, Lisa, additional, Guillo, Sylvie, additional, Taillé, Camille, additional, Estellat, Candice, additional, Devouassoux, G., additional, Taillé, C., additional, Chanez, P., additional, Bonniaud, P., additional, Bourdin, A., additional, Raymond, C.Saint, additional, Maurer, C., additional, Beurnier, A., additional, Roux, P., additional, Margelidon, V., additional, Boudjemaa, A., additional, Mangiapan, G., additional, Freymond, N., additional, Didi, T., additional, Russier, M., additional, Garcia, G., additional, Meyer, E.Popin, additional, Dupin, C., additional, Fouquet, F., additional, Jouveshomme, S., additional, Gaspard, W., additional, Dury, S., additional, Maillard, S.Habib, additional, Izadifar, A., additional, Cuvillon, E., additional, Deslée, G., additional, Barnig, C., additional, Perotin, J.M., additional, Gamez, A.S., additional, Oster, J.P., additional, Khayat, N., additional, Chenivesse, C., additional, Li, X., additional, de Vecchi, C.Appere, additional, Gicquello, A., additional, Rami, H., additional, Vignal, G., additional, Just, N., additional, Blanc, X., additional, Leroyer, C., additional, Wemeau, L., additional, Achkar, A., additional, Sattler, C., additional, Catherinot, E., additional, Guilleminault, L., additional, Gaillot-Drevon, M., additional, Rochefort-Morel, C., additional, Couturaud, F., additional, Martin, P., additional, Chabrol, A., additional, Pegliasco, H., additional, Sése, L., additional, Romanet, S., additional, Caverstri, B., additional, Tcherakian, C., additional, Magnan, A., additional, Ahmed, E., additional, Allibe, F., additional, Beltramo, G., additional, Michaux, K., additional, Paleiron, N., additional, Martinez, S., additional, Begne, C., additional, Tummino, C., additional, Givel, C., additional, Mourin, G., additional, Salvator, H., additional, Volpato, M., additional, Drucbert, M., additional, Rossignoli, N., additional, Keddache, S., additional, Justet, A., additional, Andrejak, C., additional, Valcke, J., additional, Perrin, J., additional, Mercy, M., additional, Jouvenot, M., additional, Soumagne, T., additional, Elharrar, X., additional, Douvry, B., additional, Godbert, B., additional, Maitre, B., additional, Goyard, C., additional, Didier, A., additional, Cadet, E., additional, Chabot, F., additional, Gonzalez, J., additional, Mattei, L., additional, Gouitaa, M., additional, Chauveau, S., additional, Raymond, S., additional, Dirou, S., additional, Fry, S., additional, Briault, A., additional, Moui, A., additional, Paris, A., additional, NoelSavina, E., additional, Olivier, C., additional, Caradec, E., additional, Roche, N., additional, Picart, G., additional, Belmont, L., additional, Portel, L., additional, Serra, M.Rocca, additional, Guibert, N., additional, Jean, R., additional, Hadjadj, S., additional, Guillo, S., additional, Gauquelin, L., additional, Estellat, C., additional, Prigent, A., additional, Larrousse, M., additional, and Jaffuel, D., additional

Published
2024
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14. Electroretinography and contrast sensitivity, complementary translational biomarkers of sensory deficits in the visual system of individuals with fragile X syndrome

Author

Olivier Perche, Fabien Lesne, Alain Patat, Susanne Raab, Roy Twyman, Robert H. Ring, and Sylvain Briault

Subjects
Fragile X syndrome, FMR1, Electroretinography, Biomarker, ERG, Contrast sensitivity, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Abstract Background Disturbances in sensory function are an important clinical feature of neurodevelopmental disorders such as fragile X syndrome (FXS). Evidence also directly connects sensory abnormalities with the clinical expression of behavioral impairments in individuals with FXS; thus, positioning sensory function as a potential clinical target for the development of new therapeutics. Using electroretinography (ERG) and contrast sensitivity (CS), we previously reported the presence of sensory deficits in the visual system of the Fmr1 −/y genetic mouse model of FXS. The goals of the current study were two-folds: (1) to assess the feasibility of measuring ERG and CS as a biomarker of sensory deficits in individuals with FXS, and (2) to investigate whether the deficits revealed by ERG and CS in Fmr1 −/y mice translate to humans with FXS. Methods Both ERG and CS were measured in a cohort of male individuals with FXS (n = 20, 18–45 years) and age-matched healthy controls (n = 20, 18–45 years). Under light-adapted conditions, and using both single flash and flicker (repeated train of flashes) stimulation protocols, retinal function was recorded from individual subjects using a portable, handheld, full-field flash ERG device (RETeval®, LKC Technologies Inc., Gaithersburg, MD, USA). CS was assessed in each subject using the LEA SYMBOLS® low-contrast test (Good-Lite, Elgin, IL, USA). Results Data recording was successfully completed for ERG and assessment of CS in most individuals from both cohorts demonstrating the feasibility of these methods for use in the FXS population. Similar to previously reported findings from the Fmr1 −/y genetic mouse model, individuals with FXS were found to exhibit reduced b-wave and flicker amplitude in ERG and an impaired ability to discriminate contrasts compared to healthy controls. Conclusions This study demonstrates the feasibility of using ERG and CS for assessing visual deficits in FXS and establishes the translational validity of the Fmr1 −/y mice phenotype to individuals with FXS. By including electrophysiological and functional readouts, the results of this study suggest the utility of both ERG and CS (ERG-CS) as complementary translational biomarkers for characterizing sensory abnormalities found in FXS, with potential applications to the clinical development of novel therapeutics that target sensory function abnormalities to treat core symptomatology in FXS. Trial registration ID-RCB number 2019-A01015-52 registered on the 17 May 2019.

Published
2021
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15. Case Report: Co-infection with SARS-CoV-2 and influenza H1N1 in a patient with acute respiratory distress syndrome and a pulmonary sarcoidosis [version 2; peer review: 2 approved]

Author

Lekbir Baala, Dalila Benzekri-Lefevre, Laurent Bret, Clémence Guillaume, Laura Courtellemont, Abdelkrim El Khalil, Thomas Guery, Sophie Iquel, Olivier Perche, Khalid Khadre, Thomas Brungs, Julien Decker, Thomas Francia, Julie Bois, Benoit Delamare, Jérôme Guinard, Laurence Got, Sylvain Briault, Thierry Boulain, and Eric Legac

Subjects
Case Report, Articles, Co-infection, SARS-CoV-2, Influenza H1N1, Pulmonary sarcoidosis, Comorbidity
Abstract

Coronavirus disease 2019 (COVID-19) is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and has been a global public health concern. We report coinfection of SARS-CoV-2 and 2009 H1N1 Influenza strain in a French patient with pneumonia leading to acute respiratory distress syndrome. The patient also had a medical history of pulmonary sarcoidosis with a restrictive ventilatory syndrome and obesity, which would be a supplementary risk to develop a poor outcomes. This case highlights the possible coinfection of two severe SARS-CoV-2 and influenza H1N1 viruses in comorbid patient, which presents a higher risk to extend the care duration. The overlapping clinical features of the two respiratory syndromes is a challenge, and awareness is required to recommend an early differential diagnosis and it’s necessary to adopt the vigilant preventive measures and therapeutic strategies to prevent a deleterious impacts in patients with comorbid factors.

Published
2022
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16. Circulating tumour cells as a potential biomarker for lung cancer screening: a prospective cohort study

Author

MARQUETTE, Charles-Hugo, BOUTROS, Jacques, Benzaquen, Jonathan, FERREIRA, Marion, PASTRE, Jean, Pison, Christophe, PADOVANI, Bernard, BETTAYEB, Faiza, FALLET, Vincent, GUIBERT, Nicolas, BASILLE, Damien, ILIE, Marius, HOFMAN, Véronique, HOFMAN, Paul, ISRAEL-BIET, Dominique, CHABOT, François, GUILLAUMOT, Anne, DESLEE, Gaetan, PEROTIN, Jeanne-Marie, DURY, Sandra, MAL, Hervé, MARCEAU, Armelle, Kessler, Romain, Vergnon, Jean-Michel, Pelissier, Carole, Di Palma, Fabrice, Cuvelier, Antoine, PATOUT, Maxime, Bourdin, Arnaud, GAMEZ, Anne Sophie, ANDREJAK, Claire, POULET, Claire, FRANCOIS, Géraldine, Jounieaux, Vincent, Roche, Nicolas, Jouneau, Stéphane, Brinchault, Graziella, Bonniaud, Philippe, ZOUAK, Ayoub, Scherpereel, Arnaud, BALDACCI, Simon, CORTOT, Alexis, Mornex, Jean François, Steenhouwer, François, LEROY, Sylvie, BERTHET, Jean-Philippe, FONTAS, Eric, BULSEI, Julie, CRUZEL, Coralie, Pradelli, Johanna, Fontaine, Maureen, MANIEL, Charlotte, Griffonnet, Jennifer, BUTORI, Catherine, SELVA, Eric, POUDENX, Michel, AguilanIu, Bernard, Ferretti, Gilbert, Arbib, François, Briault, Amandine, Toffart, Anne-Claire, Dahalani, Raissa, Destors, Marie, Chanez, Pascal, GREILLIER, Laurent, ASTOUL, Philippe, BARLESI, Fabrice, GAUBERT, Jean-Yves, Mazières, Julien, Marchand-Adam, Sylvain, Cadranel, Jacques, CHAABANE, Nouha, IZADIFAR, Armine, ROSENCHER, Lise, RUPPERT, Anne-Marie, VIEIRA, Thibault, MATHIOT, Nathalie, Marquette, Charles-Hugo, Boutros, Jacques, Ferreira, Marion, Pastre, Jean, Padovani, Bernard, Bettayeb, Faiza, Fallet, Vincent, Guibert, Nicolas, Basille, Damien, Ilie, Marius, Hofman, Véronique, and Hofman, Paul

Published
2020
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17. Outcomes of Therapeutic Bronchoscopy in Malignant Airway Obstruction Causing Acute Respiratory Failure

Author

Roy, P., primary, Fournier, C., additional, Barnestein, R., additional, Wallyn, F., additional, Bourinet, V., additional, Briault, A., additional, Camuset, J., additional, Cellerin, L., additional, Crutu, A., additional, Dewolf, M., additional, Egenod, T., additional, Favrolt, N., additional, Héluain, V., additional, Lorut, C., additional, Mangiapan, G., additional, Schlossmacher, P., additional, Toublanc, B., additional, Usturoi, D., additional, Legodec, J., additional, Vergnon, J.-M., additional, Pajiep Chapda, M.-C., additional, Dutau, H., additional, and Guibert, N., additional

Published
2024
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18. Therapeutic Bronchoscopy for Malignant Central Airway Obstruction Complicating Non-bronchogenic Cancers: Results From the Epigetif Registry

Author

Guibert, N., primary, Daigmorte, C., additional, Usturoi, D., additional, Fournier, C., additional, Wallyn, F., additional, Lorut, C., additional, Héluain, V., additional, Legodec, J., additional, Escargue, B., additional, Egenod, T., additional, Cellerin, L., additional, Favrolt, N., additional, Lachkar, S., additional, Crutu, A., additional, Briault, A., additional, Gut-Gobert, C., additional, Bourinet, V., additional, Camuset, J., additional, Perrot, L., additional, Schlossmacher, P., additional, Porzio, M., additional, Luchez, A., additional, Vergnon, J.-M., additional, and Dutau, H., additional

Published
2024
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19. Hippocampal interleukin-33 mediates neuroinflammation-induced cognitive impairments

Author

Flora Reverchon, Vidian de Concini, Vanessa Larrigaldie, Sulayman Benmerzoug, Sylvain Briault, Dieudonnée Togbé, Bernhard Ryffel, Valérie F. J. Quesniaux, and Arnaud Menuet

Subjects
Interleukin-33, Interleukin-1, Microglia, Memory, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Background Interleukin (IL)-33 is expressed in a healthy brain and plays a pivotal role in several neuropathologies, as protective or contributing to the development of cerebral diseases associated with cognitive impairments. However, the role of IL-33 in the brain is poorly understood, raising the question of its involvement in immunoregulatory mechanisms. Methods We administered recombinant IL-33 (rmIL-33) by intra-hippocampal injection to C57BL/6 J (WT) and IL-1αβ deficient mice. Chronic minocycline administration was performed and cognitive functions were examined trough spatial habituation test. Hippocampal inflammatory responses were investigated by RT-qPCR. The microglia activation was assessed using immunohistological staining and fluorescence-activated cell sorting (FACS). Results We showed that IL-33 administration in mice led to a spatial memory performance defect associated with an increase of inflammatory markers in the hippocampus while minocycline administration limited the inflammatory response. Quantitative assessment of glial cell activation in situ demonstrated an increase of proximal intersections per radius in each part of the hippocampus. Moreover, rmIL-33 significantly promoted the outgrowth of microglial processes. Fluorescence-activated cell sorting analysis on isolated microglia, revealed overexpression of IL-1β, 48 h post-rmIL-33 administration. This microglial reactivity was closely related to the onset of cognitive disturbance. Finally, we demonstrated that IL-1αβ deficient mice were resistant to cognitive disorders after intra-hippocampal IL-33 injection. Conclusion Thus, hippocampal IL-33 induced an inflammatory state, including IL-1β overexpression by microglia cells, being causative of the cognitive impairment. These results highlight the pathological role for IL-33 in the central nervous system, independently of a specific neuropathological model.

Published
2020
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20. Lung function in Birt-Hogg-Dubé syndrome: a retrospective analysis of 96 patients

Author

C. Daccord, V. Cottin, G. Prévot, Y. Uzunhan, J. F. Mornex, P. Bonniaud, R. Borie, A. Briault, M. A. Collonge-Rame, B. Crestani, G. Devouassoux, O. Freynet, A. Gondouin, P. A. Hauss, C. Khouatra, S. Leroy, S. Marchand-Adam, C. Marquette, D. Montani, J. M. Naccache, G. Nadeau, N. Poulalhon, M. Reynaud-Gaubert, M. Salaun, B. Wallaert, J. F. Cordier, M. Faouzi, R. Lazor, and the OrphaLung network

Subjects
Birt-Hogg-Dube syndrome, FLCN protein, human, Respiratory function tests, Pleurodesis, Medicine
Abstract

Abstract Background Birt-Hogg-Dubé syndrome (BHD) is a rare autosomal dominant disorder caused by mutations in the FLCN gene coding for folliculin. Its clinical expression includes cutaneous fibrofolliculomas, renal tumors, multiple pulmonary cysts, and recurrent spontaneous pneumothoraces. Data on lung function in BHD are scarce and it is not known whether lung function declines over time. We retrospectively assessed lung function at baseline and during follow-up in 96 patients with BHD. Results Ninety-five percent of BHD patients had multiple pulmonary cysts on computed tomography and 59% had experienced at least one pneumothorax. Mean values of forced expiratory volume in 1 second (FEV1), forced vital capacity (FVC), FEV1/FVC ratio, and total lung capacity were normal at baseline. Mean (standard deviation) residual volume (RV) was moderately increased to 116 (36) %pred at baseline, and RV was elevated > 120%pred in 41% of cases. Mean (standard deviation) carbon monoxide transfer factor (DLco) was moderately decreased to 85 (18) %pred at baseline, and DLco was decreased

Published
2020
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21. Case Report: Co-infection with SARS-CoV-2 and influenza H1N1 in a patient with acute respiratory distress syndrome and a pulmonary sarcoidosis [version 2; peer review: 2 approved]

Author

Laura Courtellemont, Abdelkrim El Khalil, Laurent Bret, Clémence Guillaume, Olivier Perche, Khalid Khadre, Thomas Guery, Sophie Iquel, Thomas Francia, Julie Bois, Thomas Brungs, Julien Decker, Laurence Got, Sylvain Briault, Toufik Kamel, Benoit Delamare, Jérôme Guinard, Thierry Boulain, Eric Legac, Lekbir Baala, and Dalila Benzekri-Lefevre

Subjects
Co-infection, SARS-CoV-2, Influenza H1N1, Pulmonary sarcoidosis, Comorbidity, eng, Medicine, Science
Abstract

Coronavirus disease 2019 (COVID-19) is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and has been a global public health concern. We report coinfection of SARS-CoV-2 and 2009 H1N1 Influenza strain in a French patient with pneumonia leading to acute respiratory distress syndrome. The patient also had a medical history of pulmonary sarcoidosis with a restrictive ventilatory syndrome and obesity, which would be a supplementary risk to develop a poor outcomes. This case highlights the possible coinfection of two severe SARS-CoV-2 and influenza H1N1 viruses in comorbid patient, which presents a higher risk to extend the care duration. The overlapping clinical features of the two respiratory syndromes is a challenge, and awareness is required to recommend an early differential diagnosis and it’s necessary to adopt the vigilant preventive measures and therapeutic strategies to prevent a deleterious impacts in patients with comorbid factors.

Published
2022
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24. Therapeutic bronchoscopy for malignant central airway obstructions caused by non‐bronchogenic cancers: Results from the EpiGETIF registry.

Author

Daigmorte, Clément, Usturoi, Daniela, Fournier, Clément, Wallyn, Frederic, Lorut, Christine, Héluain, Valentin, Mazières, Julien, Legodec, Julien, Escarguel, Bruno, Egenod, Thomas, Cellerin, Laurent, Favrolt, Nicolas, Lachkar, Samy, Crutu, Adrian, Briault, Amandine, Gut‐Gobert, Christophe, Bourinet, Valerian, Camuset, Juliette, Loïc, Perrot, and Schlossmacher, Pascal

Subjects
RESPIRATORY obstructions, BRONCHOSCOPY, ETIOLOGY of cancer, PROGNOSIS, SURVIVAL rate, CANCER treatment, HEAD & neck cancer, THYROID cancer
Abstract

Background and Objective: Little is known about malignant central airway obstruction (MCAO) complicating the metastatic spread of non‐bronchogenic solid cancers (NBC) and their bronchoscopic management. This study aimed to describe the epidemiology of this population and determine prognostic factors before therapeutic bronchoscopy (TB). Methods: In this multicenter study using the EpiGETIF registry, we analysed patients treated with TB for MCAO caused by NBC between January 2019 and December 2022. Results: From a database of 2389 patients, 436 patients (18%) with MCAO and NBC were identified. After excluding patients with direct local invasion, 214 patients (8.9%) were analysed. The main primaries involved were kidney (17.8%), colon (16.4%), sarcoma (15.4%), thyroid (8.9%) and head and neck (7.9%) cancers. Most patients (63.8%) had already received one or more lines of systemic treatment. Obstructions were purely intrinsic in 58.2%, extrinsic in 11.1% and mixed in 30.8%. Mechanical debulking was used in 73.4% of cases, combined with thermal techniques in 25.6% of cases. Airway stenting was required in 38.4% of patients. Median survival after TB was 11.2 months, influenced by histology (p = 0.002), performance status (p = 0.019), initial hypoxia (HR 1.45 [1.01–2.18]), prior oncologic treatment received (HR 1.82 [1.28–2.56], p < 0.001) and assessment of success at the end of the procedure (HR 0.66 [0.44–0.99], p < 0.001). Complications rate was 8.8%, mostly mild, with no procedure‐related mortality. Conclusion: TB for MCAO caused by a NBC metastasis provides rapid improvement of symptoms and prolonged survival. Patients should be promptly referred by medical oncologists for bronchoscopic management based on the prognostic factors identified. Therapeutic bronchoscopy for central airway obstructions caused by non‐bronchogenic cancers provides rapid improvement of symptoms. Median survival after TB (11.2 months) is influenced by histology, performance status, initial hypoxia, prior oncologic treatment received and immediate success of the procedure. [ABSTRACT FROM AUTHOR]

Published
2024
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25. Therapeutic bronchoscopy for malignant central airway obstruction: Introduction to the EpiGETIF registry.

Author

Guibert, Nicolas, Roy, Pascalin, Amari, Lyria, Legodec, Julien, Escarguel, Bruno, Fournier, Clément, Wallyn, Frederic, Cellerin, Laurent, Lorut, Christine, Usturoi, Daniela, Egenod, Thomas, Favrolt, Nicolas, Schlossmacher, Pascal, Bourinet, Valerian, Loïc, Perrot, Lachkar, Samy, Camuset, Juliette, Briault, Amandine, Kessler, Romain, and Gut‐Gobert, Christophe

Subjects
RESPIRATORY obstructions, BRONCHOSCOPY, CANCER treatment, TUBERCULOSIS, ARTIFICIAL respiration
Abstract

Background and Objective: EpiGETIF is a web‐based, multicentre clinical database created in 2019 aiming for prospective collection of data regarding therapeutic rigid bronchoscopy (TB) for malignant central airway obstruction (MCAO). Methods: Patients were enrolled into the registry from January 2019 to November 2022. Data were prospectively entered through a web‐interface, using standardized definitions for each item. The objective of this first extraction of data was to describe the population and the techniques used among the included centres to target, facilitate and encourage further studies in TB. Results: Overall, 2118 patients from 36 centres were included. Patients were on average 63.7 years old, mostly male and smokers. Most patients had a WHO score ≤2 (70.2%) and 39.6% required preoperative oxygen support, including mechanical ventilation in 6.7%. 62.4% had an already known histologic diagnosis but only 46.3% had received any oncologic treatment. Most tumours were bronchogenic (60.6%), causing mainly intrinsic or mixed obstruction (43.3% and 41.5%, respectively). Mechanical debulking was the most frequent technique (67.3%), while laser (9.8%) and cryo‐recanalization (2.7%) use depended on local expertise. Stenting was required in 54.7%, silicone being the main type of stent used (55.3%). 96.3% of procedure results were considered at least partially successful, resulting in a mean 4.1 points decrease on the Borg scale of dyspnoea. Complications were noted in 10.9%. Conclusion: This study exposes a high volume of TB that could represent a good source of future studies given the dismal amount of data about the effects of TB in certain populations and situations. The EpiGETIF registry has so far prospectively collected data from 2118 patients treated with therapeutic rigid bronchoscopy (TB) for malignant central airway obstruction (MCAO). This first report gives a picture of this population's epidemiological characteristics', anatomical presentations of MCAOs, techniques used during TB and main outcomes. See relatededitorial [ABSTRACT FROM AUTHOR]

Published
2024
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27. Plasma amyloid levels within the Alzheimer's process and correlations with central biomarkers

Author

Hanon, Olivier, Blanc, Frédéric, Boudali, Yasmina, Gabelle, Audrey, Seux, Marie–Laure, Lenoir, Hermine, Bayle, Catherine, Bombois, Stéphanie, Delbeuck, Xavier, Moulin, Florence, Duron, Emmanuelle, Latour, Florence, Plichart, Matthieu, Pichierri, Sophie, Orvoën, Galdric, Galbrun, Evelyne, Castelnovo, Giovanni, Volpe–Gillot, Lisette, Labourée, Florien, Cassagnaud, Pascaline, Paquet, Claire, Lala, Françoise, Dumurgier, Julien, Rigaud, Anne–Sophie, Perret–Guillaume, Christine, Alonso, Eliana, du Boisgueheneuc, Foucaud, Hugonot–Diener, Laurence, Rollin–Sillaire, Adeline, Martinaud, Olivier, Boully, Clémence, Spivac, Yann, Devendeville, Agnès, Belmin, Joël, Robert, Philippe–Henri, Dantoine, Thierry, Caillard, Laure, Wallon, David, Hannequin, Didier, Sastre, Nathalie, Haffen, Sophie, Kearney–Schwartz, Anna, Novella, Jean–Luc, Deramecourt, Vincent, Chauvire, Valérie, Abitbol, Gabiel, Schwald, Nathalie, Hommet, Caroline, Sellal, François, Cariot, Marie–Ange, Abdellaoui, Mohamed, Benisty, Sarah, Gherabli, Salim, Anthony, Pierre, Bloch, Frédéric, Charasz, Nathalie, Chauvelier, Sophie, Gaubert, Jean–Yves, Sacco, Guillaume, Guerin, Olivier, Boddaert, Jacques, Paccalin, Marc, Mackowiak, Marie–Anne, Rabus, Marie–Thérèse, Gissot, Valérie, Benetos, Athanase, Picard, Candice, Guillemaud, Céline, Gervais, Claire, Hugon, Jaques, Michel, Jean–Marc, David, Jean–Philippe, Paulin, Marion, Ousset, Pierre–Jean, Vandel, Pierre, Pariel, Sylvie, Camus, Vincent, Chawakilian, Anne, Joffredo, Léna, Troussiere, Anne–Cécile, Adam, Cécile, Dupuy, Diane, Paillaud, Elèna, Briault, Hélène, Saulnier, Isabelle, Mondon, Karl, Picat, Marie–Agnès, Laurent, Marie, Godefroy, Olivier, Daheb, Rezki, Libercier, Stéphanie, Krabchi, Djamila, Chupin, Marie, Vidal, Jean–Sébastien, Chaussade, Edouard, Lehmann, Sylvain, Schraen-Maschke, Suzanna, Vidal, Jean-Sébastien, Allinquant, Bernadette, Tréluyer, Jean-Marc, Gelé, Patrick, Delmaire, Christine, Blanc, Fredéric, Mangin, Jean-François, Buée, Luc, Touchon, Jacques, Hugon, Jacques, Vellas, Bruno, Berrut, Gilles, Volpe-Gillot, Lisette, Robert, Philippe-Henri, Novella, Jean-Luc, and Rigaud, Anne-Sophie

Published
2018
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29. Case Report: Co-infection with SARS-CoV-2 and influenza H1N1 in a patient with acute respiratory distress syndrome [version 1; peer review: 1 approved, 1 approved with reservations]

Author

Lekbir Baala, Dalila Benzekri-Lefevre, Laurent Bret, Clémence Guillaume, Laura Courtellemont, Abdelkrim El Khalil, Thomas Guery, Sophie Iquel, Olivier Perche, Khalid Khadre, Thomas Brungs, Julien Decker, Thomas Francia, Julie Bois, Benoit Delamare, Jérôme Guinard, Laurence Got, Sylvain Briault, Thierry Boulain, and Eric Legac

Subjects
Case Report, Articles, Co-infection, SARS-CoV-2, Influenza H1N1
Abstract

Coronavirus disease 2019 (COVID-19) is caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and has been a global public health concern. Co-infection of SARS-CoV-2 and other respiratory syndrome has been rarely reported. We report coinfection of SARS-CoV-2 and 2009 H1N1 Influenza strain in a French patient with pneumonia leading to acute respiratory distress syndrome. The patient also had a medical history of pulmonary sarcoidosis with a restrictive ventilatory syndrome, which would be a supplementary risk to develop a poor outcomes. This case highlights the possible coinfection of two severe SARS-CoV-2 and influenza H1N1 viruses, which presents a higher risk to extend the care duration. The overlapping clinical features of the two respiratory syndromes is a challenge, and awareness is required to recommend an early differential diagnosis.

Published
2020
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30. A machine learning approach to predict extreme inactivity in COPD patients using non-activity-related clinical data.

Author

Bernard Aguilaniu, David Hess, Eric Kelkel, Amandine Briault, Marie Destors, Jacques Boutros, Pei Zhi Li, and Anestis Antoniadis

Subjects
Medicine, Science
Abstract

Facilitating the identification of extreme inactivity (EI) has the potential to improve morbidity and mortality in COPD patients. Apart from patients with obvious EI, the identification of a such behavior during a real-life consultation is unreliable. We therefore describe a machine learning algorithm to screen for EI, as actimetry measurements are difficult to implement. Complete datasets for 1409 COPD patients were obtained from COLIBRI-COPD, a database of clinicopathological data submitted by French pulmonologists. Patient- and pulmonologist-reported estimates of PA quantity (daily walking time) and intensity (domestic, recreational, or fitness-directed) were first used to assign patients to one of four PA groups (extremely inactive [EI], overtly active [OA], intermediate [INT], inconclusive [INC]). The algorithm was developed by (i) using data from 80% of patients in the EI and OA groups to identify 'phenotype signatures' of non-PA-related clinical variables most closely associated with EI or OA; (ii) testing its predictive validity using data from the remaining 20% of EI and OA patients; and (iii) applying the algorithm to identify EI patients in the INT and INC groups. The algorithm's overall error for predicting EI status among EI and OA patients was 13.7%, with an area under the receiver operating characteristic curve of 0.84 (95% confidence intervals: 0.75-0.92). Of the 577 patients in the INT/INC groups, 306 (53%) were reclassified as EI by the algorithm. Patient- and physician- reported estimation may underestimate EI in a large proportion of COPD patients. This algorithm may assist physicians in identifying patients in urgent need of interventions to promote PA.

Published
2021
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31. Airway microbiota signals anabolic and catabolic remodeling in the transplanted lung

Author

Jougon, J., Velly, J.-F., Rozé, H., Blanchard, E., Dromer, C., Antoine, M., Cappello, M., Ruiz, M., Sokolow, Y., Vanden Eynden, F., Van Nooten, G., Barvais, L., Berré, J., Brimioulle, S., De Backer, D., Créteur, J., Engelman, E., Huybrechts, I., Ickx, B., Preiser, T.J.C., Tuna, T., Van Obberghe, L., Vancutsem, N., Vincent, J.-L., De Vuyst, P., Etienne, I., Féry, F., Jacobs, F., Knoop, C., Vachiéry, J.L., Van den Borne, P., Wellemans, I., Amand, G., Collignon, L., Giroux, M., Angelescu, D., Chavanon, O., Hacini, R., Pirvu, A., Porcu, P., Albaladejo, P., Allègre, C., Bataillard, A., Bedague, D., Briot, E., Casez-Brasseur, M., Colas, D., Dessertaine, G., Durand, M., Francony, G., Hebrard, A., Marino, M.R., Oummahan, B., Protar, D., Rehm, D., Robin, S., Rossi-Blancher, M., Augier, C., Bedouch, P., Boignard, A., Bouvaist, H., Briault, A., Camara, B., Claustre, J., Chanoine, S., Dubuc, M., Quétant, S., Maurizi, J., Pavèse, P., Pison, C., Saint-Raymond, C., Wion, N., Chérion, C., Grima, R., Jegaden, O., Maury, J.-M., Tronc, F., Flamens, C., Paulus, S., Mornex, J.-F., Philit, F., Senechal, A., Glérant, J.-C., Turquier, S., Gamondes, D., Chalabresse, L., Thivolet-Bejui, F., Barnel, C., Dubois, C., Tiberghien, A., Le Pimpec-Barthes, F., Bel, A., Mordant, P., Achouh, P., Boussaud, V., Guillemain, R., Méléard, D., Bricourt, M.O., Cholley, B., Pezella, V., Brioude, G., D'Journo, X.B., Doddoli, C., Thomas, P., Trousse, D., Dizier, S., Leone, M., Papazian, L., Bregeon, F., Basire, A., Coltey, B., Dufeu, N., Dutau, H., Garcia, S., Gaubert, J.Y., Gomez, C., Laroumagne, S., Nieves, A., Picard, L.C., Reynaud-Gaubert, M., Secq, V., Mouton, G., Baron, O., Lacoste, P., Perigaud, C., Roussel, J.C., Danner, I., Haloun, A., Magnan, A., Tissot, A., Lepoivre, T., Treilhaud, M., Botturi-Cavaillès, K., Brouard, S., Danger, R., Loy, J., Morisset, M., Pain, M., Pares, S., Reboulleau, D., Royer, P.-J., Fabre, D., Fadel, E., Mercier, O., Mussot, S., Stephan, F., Viard, P., Cerrina, J., Dorfmuller, P., Ghigna, S.M., Hervén, Ph., Le Roy Ladurie, F., Le Pavec, J., Thomas de Montpreville, V., Lamrani, L., Castier, Y., Cerceau, P., Augustin, P., Jean-Baptiste, S., Boudinet, S., Montravers, P., Brugière, O., Dauriat, G., Jébrak, G., Mal, H., Marceau, A., Métivier, A.-C., Thabut, G., Lhuillier, E., Dupin, C., Bunel, V., Falcoz, P., Massard, G., Santelmo, N., Ajob, G., Collange, O., Helms, O., Hentz, J., Roche, A., Bakouboula, B., Degot, T., Dory, A., Hirschi, S., Ohlmann-Caillard, S., Kessler, L., Kessler, R., Schuller, A., Bennedif, K., Vargas, S., Stauder, J., Ali-Azouaou, S., Bonnette, P., Chapelier, A., Puyo, P., Sage, E., Bresson, J., Caille, V., Cerf, C., Devaquet, J., Dumans-Nizard, V., Felten, M.-L., Fischler, M., Si Larbi, A.-G., Leguen, M., Ley, L., Liu, N., Trebbia, G., De Miranda, S., Douvry, B., Gonin, F., Grenet, D., Hamid, A.M., Neveu, H., Parquin, F., Picard, C., Roux, A., Stern, M., Bouillioud, F., Cahen, P., Colombat, M., Dautricourt, C., Delahousse, M., D'Urso, B., Gravisse, J., Guth, A., Hillaire, S., Honderlick, P., Lequintrec, M., Longchampt, E., Mellot, F., Scherrer, A., Temagoult, L., Tricot, L., Vasse, M., Veyrie, C., Zemoura, L., Berjaud, J., Brouchet, L., Dahan, M., Mathe, F.O., Benahoua, H., DaCosta, M., Serres, I., Merlet-Dupuy, V., Grigoli, M., Didier, A., Murris, M., Crognier, L., Fourcade, O., Krueger, T., Ris, H.B., Gonzalez, M., Jolliet, Ph., Marcucci, C., Chollet, M., Gronchi, F., Courbon, C., Berutto, C., Manuel, O., Koutsokera, A., Aubert, J.-D., Nicod, L.P., Mouraux, S., Bernasconi, E., Pattaroni, C., Marsland, B.J., Soccal, P.M., Rochat, T., Lücker, L.M., Hillinger, S., Inci, I., Weder, W., Schuepbach, R., Zalunardo, M., Benden, C., Schuurmans, M.M., Gaspert, A., Holzmann, D., Müller, N., Schmid, C., Vrugt, B., Fritz, A., Maier, D., Deplanche, K., Koubi, D., Ernst, F., Paprotka, T., Schmitt, M., Wahl, B., Boissel, J.-P., Olivera-Botello, G., Trocmé, C., Toussaint, B., Bourgoin-Voillard, S., Sève, M., Benmerad, M., Siroux, V., Slama, R., Auffray, C., Charron, D., Lefaudeux, D., Pellet, J., Mouraux, Stéphane, Bernasconi, Eric, Pattaroni, Céline, Koutsokera, Angela, Aubert, John-David, Claustre, Johanna, Pison, Christophe, Royer, Pierre-Joseph, Magnan, Antoine, Kessler, Romain, Benden, Christian, Soccal, Paola M., Marsland, Benjamin J., and Nicod, Laurent P.

Published
2018
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32. Clinical evaluation of pharmacists’ interventions on multidisciplinary lung transplant outpatients’ management: results of a 7-year observational study

Author

Boubou Camara, Marion Duwez, Sébastien Chanoine, Marion Lepelley, Thi Ha Vo, Hélène Pluchart, Roseline Mazet, Benoit Allenet, Christophe Pison, Amandine Briault, Christelle Saint-Raymond, Johanna Claustre, and Pierrick Bedouch

Subjects
Medicine
Abstract

Objectives Lung transplant (LT) recipients require multidisciplinary care because of the complexity of therapeutic management. Pharmacists are able to detect drug-related problems and provide recommendations to physicians through pharmacists’ interventions (PIs). We aimed at assessing the clinical impact of PIs on therapeutic management in LT outpatients.Design Data were collected prospectively from an LT recipients cohort during 7 years. A multidisciplinary committee assessed retrospectively the clinical impact of accepted PIs.Setting French University Hospital.Participants LT outpatients followed from 2009 to 2015.Primary outcome measures Clinical impact of PIs performed by pharmacists using the CLEO tool and the Pareto chart.Results 1449 PIs led to a change in patient therapeutic management and were mainly related to wrong dosage (39.6%) and untreated indication (19.6%). The clinical impact of PIs was ‘avoids fatality’, ‘major’ and ‘moderate’, in 0.1%, 7.0% and 57.9%, respectively. Immunosuppressants, antimycotics for systemic use and antithrombotic agents had the greatest clinical impact according to the Pareto chart. PIs related to drug–drug interactions (10%) mainly had a moderate and major clinical impact (82.3%, p

Published
2020
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33. GPATCH11 variants cause mis-splicing and early-onset retinal dystrophy with neurological impairment

Author

Perrault, Isabelle, primary, Zanetti, Andrea, additional, Fares-Taie, Lucas, additional, Amiel, Jeanne, additional, Roger, Jerome, additional, Audo, Isabelle, additional, Robert, Matthieu, additional, David, Pierre, additional, Jung, Vincent, additional, GOUDIN, Nicolas, additional, Guerrera, Ida, additional, Moriceau, Stéphanie, additional, Amana, Danielle, additional, Boddaert, Nathalie, additional, Briault, Sylvain, additional, Bruel, Ange-Line, additional, Gitiaux, Cyril, additional, Kaminska, Karolina, additional, Philip-Sarles, Nicole, additional, Quinodoz, Mathieu, additional, Santos, Christina, additional, Santos, Luisa Coutinho, additional, Sigaudy, Sabine, additional, Sá, Mariana Soeiro e, additional, Sousa, Ana Berta, additional, Thauvin, Christel, additional, Kaplan, Josseline, additional, Rivolta, Carlo, additional, and Rozet, Jean-Michel, additional

Published
2023
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35. Symbols, spaces and materiality : a transmission-based approach to Aegean Bronze Age ritual

Author

Briault, Camilla

Subjects
939.1
Abstract

This thesis explores the transmission of ritual practices in the second millennium BC Aegean. In contrast to previous approaches, which often overlook gaps in the diachronic record, emphasising continuity in cult practice over very long timescales, it is argued here that through charting the spatial and temporal distributions of three broad material types (cult symbols, spaces and objects), it is possible to document the spread of cult practice over time and space, and, crucially, to monitor changes in ritual between periods and between regions. Quantitative analyses of eight Cretan cult symbols, and examinations of each type of Aegean cult space and their associated ritual objects are employed in order to determine the extent to which ritual systems remained stable or underwent transformation over a thousand-year period. These analyses also expose the mechanisms by which ritual practice was transmitted. By relating the periods of stability and flux in ritual practice to the wider social and political changes seen in the Aegean during the Bronze Age, the role of ritual in the formation, maintenance and dissolution of political systems in different regions of the Aegean becomes more apparent. The wider aim of this thesis is to develop a new theoretical and methodological framework for examining the spread of ritual practices in prehistoric contexts, and the Aegean data thus serve as a case study on which to test that framework. The reproduction and transformation of ritual systems through time is an under-theorised area of prehistoric archaeology, and the second millennium BC Aegean provides an unusually attractive testing ground for theories of ritual transmission, due both to the quantity and range of the material available, and to the fine chronological control we now have over a large part of it. Focussing on ritual as a performance-based, materialised social practice, the framework combines models of cultural transmission drawn from archaeology, anthropology and cognitive psychology, and should be applicable not only to the Bronze Age Aegean, but to ritual stability and change in other prehistoric contexts.

Published
2005

37. Outcomes of Therapeutic Bronchoscopy in Malignant Airway Obstruction Causing Acute Respiratory Failure.

Author

Roy, Pascalin, Fournier, Clément, Barnestein, Robby, Wallyn, Frédéric, Bourinet, Valérian, Briault, Amandine, Camuset, Juliette, Cellerin, Laurent, Crutu, Adrian, Dewolf, Maxime, Egenod, Thomas, Favrolt, Nicolas, Héluain, Valentin, Lorut, Christine, Mangiapan, Gilles, Schlossmasscher, Pascal, Toublanc, Benedicte, Usturoi, Daniela, Legodec, Julien, and Vergnon, Jean-Michel

Subjects
ETIOLOGY of diseases, ADULT respiratory distress syndrome, BREAST, LUNGS, RESPIRATORY obstructions, BRONCHOSCOPY, SMALL cell lung cancer
Abstract

The article examines the effectiveness of therapeutic bronchoscopy in treating acute respiratory failure caused by malignant central airway obstruction (MCAO). It analyzes outcomes like survival, oxygen support weaning, and post-procedure oncologic treatment. It aims to guide clinical decisions and improve patient care for this challenging condition.

Published
2024
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38. Revisiting the systemic vasculitis in eosinophilic granulomatosis with polyangiitis (Churg-Strauss): A study of 157 patients by the Groupe d'Etudes et de Recherche sur les Maladies Orphelines Pulmonaires and the European Respiratory Society Taskforce on eosinophilic granulomatosis with polyangiitis (Churg-Strauss)

Author

Cottin, Vincent, Bel, Elisabeth, Bottero, Paolo, Dalhoff, Klaus, Humbert, Marc, Lazor, Romain, Sinico, Renato A., Sivasothy, Pasupathy, Wechsler, Michael E., Groh, Matthieu, Marchand-Adam, Sylvain, Khouatra, Chahéra, Wallaert, Benoit, Taillé, Camille, Delaval, Philippe, Cadranel, Jacques, Bonniaud, Philippe, Prévot, Grégoire, Hirschi, Sandrine, Gondouin, Anne, Dunogué, Bertrand, Chatté, Gérard, Briault, Christophe, Pagnoux, Christian, Jayne, David, Guillevin, Loïc, and Cordier, Jean-François

Published
2017
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39. GPATCH11variants cause mis-splicing and early-onset retinal dystrophy with neurological impairment

Author

Zanetti, Andrea, primary, Fares-Taie, Lucas, additional, Amiel, Jeanne, additional, Roger, Jérôme, additional, Audo, Isabelle, additional, Robert, Matthieu, additional, David, Pierre, additional, Jung, Vincent, additional, Goudin, Nicolas, additional, Guerrera, Ida Chiara, additional, Moriceau, Stéphanie, additional, Amana, Danielle, additional, Boddaert, Nathalie, additional, Briault, Sylvain, additional, Bruel, Ange-Line, additional, Gitiaux, Cyril, additional, Kaminska, Karolina, additional, Philip-Sarles, Nicole, additional, Quinodoz, Mathieu, additional, Santos, Cristina, additional, Coutinho Santos, Luisa, additional, Sigaudy, Sabine, additional, Soeiro e Sá, Mariana, additional, Sousa, Ana Berta, additional, Thauvin, Christel, additional, Rivolta, Carlo, additional, Kaplan, Josseline, additional, Rozet, Jean-Michel, additional, and Perrault, Isabelle, additional

Published
2023
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40. Visual Behavior Impairments as an Aberrant Sensory Processing in the Mouse Model of Fragile X Syndrome

Author

Chloé Felgerolle, Betty Hébert, Maryvonne Ardourel, Géraldine Meyer-Dilhet, Arnaud Menuet, Kimberley Pinto-Morais, Jean-Charles Bizot, Jacques Pichon, Sylvain Briault, and Olivier Perche

Subjects
Fragile X Syndrome, Fmr1−/y mice, FMRP, sensory sensitivity, visual abilities, depth perception, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Fragile X Syndrome (FXS), the most common inherited form of human intellectual disability (ID) associated with autistic-like behaviors, is characterized by dys-sensitivity to sensory stimuli, especially vision. In the absence of Fragile Mental Retardation Protein (FMRP), both retinal and cerebral structures of the visual pathway are impaired, suggesting that perception and integration of visual stimuli are altered. However, behavioral consequences of these defects remain unknown. In this study, we used male Fmr1−/y mice to further define visual disturbances from a behavioral perspective by focusing on three traits characterizing visual modality: perception of depth, contrasts and movements. We performed specific tests (Optomotor Drum, Visual Cliff) to evaluate these visual modalities, their evolution from youth to adulthood, and to assess their involvement in a cognitive task. We show that Fmr1−/y mice exhibit alteration in their visual skills, displaying impaired perspective perception, a drop in their ability to understand a moving contrasted pattern, and a defect in contrasts discrimination. Interestingly, Fmr1−/y phenotypes remain stable over time from adolescence to late adulthood. Besides, we report that color and shape are meaningful for the achievement of a cognitive test involving object recognition. Altogether, these results underline the significance of visual behavior alterations in FXS conditions and relevance of assessing visual skills in neuropsychiatric models before performing behavioral tasks, such as cognitive assessments, that involve visual discrimination.

Published
2019
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41. Early Retinal Defects in Fmr1−/y Mice: Toward a Critical Role of Visual Dys-Sensitivity in the Fragile X Syndrome Phenotype?

Author

Olivier Perche, Chloé Felgerolle, Maryvonne Ardourel, Audrey Bazinet, Arnaud Pâris, Rafaëlle Rossignol, Géraldine Meyer-Dilhet, Anne-Laure Mausset-Bonnefont, Betty Hébert, David Laurenceau, Céline Montécot-Dubourg, Arnaud Menuet, Jean-Charles Bizot, Jacques Pichon, Isabelle Ranchon-Cole, and Sylvain Briault

Subjects
Fragile X syndrome, Fmrp, vision, sensorial dys-sensitivity, peripheral nervous system, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571
Abstract

Fragile X Syndrome (FXS) is caused by a deficiency in Fragile X Mental Retardation Protein (FMRP) leading to global sensorial abnormalities, among which visual defects represent a critical part. These visual defects are associated with cerebral neuron immaturity especially in the primary visual cortex. However, we recently demonstrated that retinas of adult Fmr1−/y mice, the FXS murine model, present molecular, cellular and functional alterations. However, no data are currently available on the evolution pattern of such defects. As retinal stimulation through Eye Opening (EO) is a crucial signal for the cerebral visual system maturation, we questioned the precocity of molecular and functional retinal phenotype. To answer this question, we studied the retinal molecular phenotype of Fmr1−/y mice before EO until adult age and the consequences of the retinal loss of Fmrp on retinal function in young and adult mice. We showed that retinal molecular defects are present before EO and remain stable at adult age, leading to electrophysiological impairments without any underlying structural changes. We underlined that loss of Fmrp leads to a wide range of defects in the retina, settled even before EO. Our work demonstrates a critical role of the sensorial dysfunction in the Fmr1−/y mice overall phenotype, and provides evidence that altered peripheral perception is a component of the sensory processing defect in FXS conditions.

Published
2018
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42. Computed tomographic airway morphology after targeted lung denervation treatment in COPD

Author

Jorine E. Hartman, Felix J.F. Herth, Pallav Shah, Christophe Pison, Arschang Valipour, Dirk-Jan Slebos, Christine Abele, Irene Firlinger, Kiran Kothakuzhakal, Marina Duller, Bernd Lamprecht, Roland Kropfmueller, Kornelia Holzmann, Sandra Rathmeier, Ralf Hubner, Leonore Erdmann, Bettina Temmesfeld-Wollbrück, Christoph Ruwwe Glösenkamp, Wolfgang Gesierich, Frank Reichenberger, Christa Niehaus, Felix Herth, Ralf Eberhardt, Daniela Gompelmann, Brigitte Rump, Kaid Darwiche, Stephan Eisenmann, Ulrike Kaiser, Birte Schwarz, Ulrike Sampel, Christian Schumann, Robert Kaiser, Kathryn Schumann-Stoiber, Dirk Skowasch, Sabine Ring, Amandine Briault, Francois Arbib, Marie Jondot, Thierry Perez, Clement Fournier, Regis Matran, Michele Catto, Nathalie Bautin, Virginie De Broucker, Marie Willemin, Anne Prevotat, Ludivine Wemeau, Alice Gicquello, Morgane Foulon, Hasna Camara, Gaetan Deslee, Herve Vallerand, Sandra Dury, Delphine Gras, Margaux Bonnaire-Verdier, Romain Kessler, Sandrine Hirschi, Michele Porzio, Tristan Degot, Mathieu Canuet, Armelle Schuller, Julien Stauder, Sahra Ali Azouaou, Armelle Marceau, Hervé Mal, Yolande Costa, Pallav L. Shah, Justin Garner, Karthi Srikanthan, Cielito Caneja, John Thornton, Nick Ten Hacken, Jorine Hartman, Karin Klooster, Sonja Augustijn, Peter Bonta, Jouke Annema, Marianne van de Pol, Annika Goorsenberg, VU University medical center, Groningen Research Institute for Asthma and COPD (GRIAC), Pulmonology, ACS - Pulmonary hypertension & thrombosis, AII - Infectious diseases, AII - Inflammatory diseases, AII - Cancer immunology, CCA - Cancer biology and immunology, and CCA - Imaging and biomarkers

Subjects
Pulmonary and Respiratory Medicine
Abstract

This post-hoc analysis of the AIRFLOW-2 trial investigated the changes in airway CT-parameters after targeted lung denervation (TLD) and whether these changes are associated with treatment response. In the treatment group (n = 32), an improvement in air trapping was significantly associated with an improvement in residual volume (RV). Furthermore, improvements in Pi10 and airway lumen were significantly associated with an improvement in both RV and FEV1. Our results could suggest that when improving airway characteristics like decreasing airway wall thickness and increasing the airway lumen, this leads to less air trapping and an improvement in clinical outcomes.

Published
2023
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43. Computed tomographic airway morphology after targeted lung denervation treatment in COPD

Author

Hartman, Jorine E., primary, Herth, Felix J.F., additional, Shah, Pallav, additional, Pison, Christophe, additional, Valipour, Arschang, additional, Slebos, Dirk-Jan, additional, Abele, Christine, additional, Firlinger, Irene, additional, Kothakuzhakal, Kiran, additional, Duller, Marina, additional, Lamprecht, Bernd, additional, Kropfmueller, Roland, additional, Holzmann, Kornelia, additional, Rathmeier, Sandra, additional, Hubner, Ralf, additional, Erdmann, Leonore, additional, Temmesfeld-Wollbrück, Bettina, additional, Ruwwe Glösenkamp, Christoph, additional, Gesierich, Wolfgang, additional, Reichenberger, Frank, additional, Niehaus, Christa, additional, Herth, Felix, additional, Eberhardt, Ralf, additional, Gompelmann, Daniela, additional, Rump, Brigitte, additional, Darwiche, Kaid, additional, Eisenmann, Stephan, additional, Kaiser, Ulrike, additional, Schwarz, Birte, additional, Sampel, Ulrike, additional, Schumann, Christian, additional, Kaiser, Robert, additional, Schumann-Stoiber, Kathryn, additional, Skowasch, Dirk, additional, Ring, Sabine, additional, Briault, Amandine, additional, Arbib, Francois, additional, Jondot, Marie, additional, Perez, Thierry, additional, Fournier, Clement, additional, Matran, Regis, additional, Catto, Michele, additional, Bautin, Nathalie, additional, De Broucker, Virginie, additional, Willemin, Marie, additional, Prevotat, Anne, additional, Wemeau, Ludivine, additional, Gicquello, Alice, additional, Foulon, Morgane, additional, Camara, Hasna, additional, Deslee, Gaetan, additional, Vallerand, Herve, additional, Dury, Sandra, additional, Gras, Delphine, additional, Bonnaire-Verdier, Margaux, additional, Kessler, Romain, additional, Hirschi, Sandrine, additional, Porzio, Michele, additional, Degot, Tristan, additional, Canuet, Mathieu, additional, Schuller, Armelle, additional, Stauder, Julien, additional, Azouaou, Sahra Ali, additional, Marceau, Armelle, additional, Mal, Hervé, additional, Costa, Yolande, additional, Shah, Pallav L., additional, Garner, Justin, additional, Srikanthan, Karthi, additional, Caneja, Cielito, additional, Thornton, John, additional, Hacken, Nick Ten, additional, Hartman, Jorine, additional, Klooster, Karin, additional, Augustijn, Sonja, additional, Bonta, Peter, additional, Annema, Jouke, additional, van de Pol, Marianne, additional, and Goorsenberg, Annika, additional

Published
2023
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44. FMR protein: Evidence of an emerging role in retinal aging?

Author

M. Ardourel, I. Ranchon-Cole, A. Pâris, C. Felgerolle, N. Acar, F. Lesne, S. Briault, O. Perche, Université d'Orléans (UO), Immunologie et Neurogénétique Expérimentales et Moléculaires (INEM), Université d'Orléans (UO)-Centre National de la Recherche Scientifique (CNRS), CHU Clermont-Ferrand, Neuro-Dol (Neuro-Dol), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Clermont Auvergne (UCA), Université Clermont Auvergne (UCA), Centre des Sciences du Goût et de l'Alimentation [Dijon] (CSGA), Université de Bourgogne (UB)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)-Institut Agro Dijon, Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro), Université Bourgogne Franche-Comté [COMUE] (UBFC), Hôpital La Source [Orléans] (HLSO), The research was supported by CHR of Orleans, CNRS of Orleans, University of Orleans and regional Centre-Val de Loire grant (FRAX-SENS, 2017-2020).Corresponding author: Genetic Department, Regional Hospital, 14 avenue de l’hôpital, F-45071, Orléans. E-mail address: olivier.perche@chr-orleans.fr (O. Perche)., and Julien, Sabine

Subjects
Adult, Aging, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Vision, Infant, Retina, Sensory Systems, Contrast Sensitivity, Mice, Fragile X Mental Retardation Protein, Cellular and Molecular Neuroscience, Ophthalmology, [SDV.MHEP.OS] Life Sciences [q-bio]/Human health and pathology/Sensory Organs, Fmrp Vision Electroretinography Age-related Aging, Retinal Cone Photoreceptor Cells, Electroretinography, Humans, Animals, [SDV.MHEP.OS]Life Sciences [q-bio]/Human health and pathology/Sensory Organs, Age-related, Fmrp, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology
Abstract

Short communication 7 p.; International audience; Aging is a multifactorial process that affects the entire organism by cumulative alterations. Visual function impairments that go along with aging are commonly observed, causing lower visual acuity, lower contrast sensitivity, and impaired dark adaptation. Electroretinogram analysis revealed that the amplitudes of rod- and cone-mediated responses are reduced in aged mice and humans. Reports suggested that age-related changes observed in both rod and cone photoreceptor functionality were linked to oxidative stress regulation or free radical production homeostasis. Interestingly, several recent reports linked the fragile X mental retardation protein (FMRP) cellular activity with oxidative stress regulation in several tissue including brain tissue where FMRP participates to the response to stress via protein translation in neurite or is involved in free radical production and abnormal glutathione homeostasis. Based on these recent literatures, we raised the question about the effect of FMRP absence in the aging retina of Fmr1(-/y) compared to their WT littermates. Indeed, up to now, only young or adult mice (

Published
2022
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50. Blood Gene Expression Predicts Bronchiolitis Obliterans Syndrome

Author

Richard Danger, Pierre-Joseph Royer, Damien Reboulleau, Eugénie Durand, Jennifer Loy, Adrien Tissot, Philippe Lacoste, Antoine Roux, Martine Reynaud-Gaubert, Carine Gomez, Romain Kessler, Sacha Mussot, Claire Dromer, Olivier Brugière, Jean-François Mornex, Romain Guillemain, Marcel Dahan, Christiane Knoop, Karine Botturi, Aurore Foureau, Christophe Pison, Angela Koutsokera, Laurent P. Nicod, Sophie Brouard, Antoine Magnan, The COLT and SysCLAD Consortia, J. Jougon, J.-F. Velly, H. Rozé, E. Blanchard, C. Dromer, M. Antoine, M. Cappello, R. Souilamas, M. Ruiz, Y. Sokolow, F. Vanden Eynden, G. Van Nooten, L. Barvais, J. Berré, S. Brimioulle, D. De Backer, J. Créteur, E. Engelman, I. Huybrechts, B. Ickx, T. J. C. Preiser, T. Tuna, L. Van Obberghe, N. Vancutsem, J.-L. Vincent, P. De Vuyst, I. Etienne, F. Féry, F. Jacobs, C. Knoop, J. L. Vachiéry, P. Van den Borne, I. Wellemans, G. Amand, L. Collignon, M. Giroux, E. Arnaud-Crozat, V. Bach, P.-Y. Brichon, P. Chaffanjon, O. Chavanon, A. de Lambert, J. P. Fleury, S. Guigard, K. Hireche, A. Pirvu, P. Porcu, R. Hacini, P. Albaladejo, C. Allègre, A. Bataillard, D. Bedague, E. Briot, M. Casez-Brasseur, D. Colas, G. Dessertaine, M. Durand, G. Francony, A. Hebrard, M. R. Marino, B. Oummahan, D. Protar, D. Rehm, S. Robin, M. Rossi-Blancher, P. Bedouch, A. Boignard, H. Bouvaist, A. Briault, B. Camara, S. Chanoine, M. Dubuc, S. Lantuéjoul, S. Quétant, J. Maurizi, P. Pavèse, C. Pison, C. Saint-Raymond, N. Wion, C. Chérion, R. Grima, O. Jegaden, J.-M. Maury, F. Tronc, C. Flamens, S. Paulus, J. F. Mornex, F. Philit, A. Senechal, J.-C. Glérant, S. Turquier, D. Gamondes, L. Chalabresse, F. Thivolet-Bejui, C. Barnel, C. Dubois, A. Tiberghien, F. Le Pimpec-Barthes, A. Bel, P. Mordant, P. Achouh, V. Boussaud, R. Guillemain, D. Méléard, M. O. Bricourt, B. Cholley, V. Pezella, M. Adda, M. Badier, F. Bregeon, B. Coltey, X. B. D’Journo, S. Dizier, C. Doddoli, N. Dufeu, H. Dutau, J. M. Forel, J. Y. Gaubert, C. Gomez, M. Leone, A. Nieves, B. Orsini, L. Papazian, L. C. Picard, M. Reynaud-Gaubert, A. Roch, J. M. Rolain, E. Sampol, V. Secq, P. Thomas, D. Trousse, M. Yahyaoui, O. Baron, P. Lacoste, C. Perigaud, J. C. Roussel, I. Danner, A. Haloun, A. Magnan, A. Tissot, T. Lepoivre, M. Treilhaud, K. Botturi-Cavaillès, S. Brouard, R. Danger, J. Loy, M. Morisset, M. Pain, S. Pares, D. Reboulleau, P. J. Royer, E. Durand, A. Foureau, Ph. Dartevelle, D. Fabre, E. Fadel, O. Mercier, S. Mussot, F. Stephan, P. Viard, J. Cerrina, P. Dorfmuller, S. Feuillet, M. Ghigna, Ph. Hervén, F. Le Roy Ladurie, J. Le Pavec, V. Thomas de Montpreville, L. Lamrani, Y. Castier, P. Cerceau, F. Francis, G. Lesèche, N. Allou, P. Augustin, S. Boudinet, M. Desmard, G. Dufour, P. Montravers, O. Brugière, G. Dauriat, G. Jébrak, H. Mal, A. Marceau, A.-C. Métivier, G. Thabut, B. Ait Ilalne, P. Falcoz, G. Massard, N. Santelmo, G. Ajob, O. Collange, O. Helms, J. Hentz, A. Roche, B. Bakouboula, T. Degot, A. Dory, S. Hirschi, S. Ohlmann-Caillard, L. Kessler, R. Kessler, A. Schuller, K. Bennedif, S. Vargas, P. Bonnette, A. Chapelier, P. Puyo, E. Sage, J. Bresson, V. Caille, C. Cerf, J. Devaquet, V. Dumans-Nizard, M. L. Felten, M. Fischler, A. G. Si Larbi, M. Leguen, L. Ley, N. Liu, G. Trebbia, S. De Miranda, B. Douvry, F. Gonin, D. Grenet, A. M. Hamid, H. Neveu, F. Parquin, C. Picard, A. Roux, M. Stern, F. Bouillioud, P. Cahen, M. Colombat, C. Dautricourt, M. Delahousse, B. D’Urso, J. Gravisse, A. Guth, S. Hillaire, P. Honderlick, M. Lequintrec, E. Longchampt, F. Mellot, A. Scherrer, L. Temagoult, L. Tricot, M. Vasse, C. Veyrie, L. Zemoura, J. Berjaud, L. Brouchet, M. Dahan, F. Le Balle, O. Mathe, H. Benahoua, A. Didier, A. L. Goin, M. Murris, L. Crognier, O. Fourcade, T. Krueger, H. B. Ris, M. Gonzalez, J.-D. Aubert, L. P. Nicod, B. J. Marsland, T. C. Berutto, T. Rochat, P. Soccal, Ph. Jolliet, A. Koutsokera, C. Marcucci, O. Manuel, E. Bernasconi, M. Chollet, F. Gronchi, C. Courbon, Zurich S. Hillinger, I. Inci, P. Kestenholz, W. Weder, R. Schuepbach, M. Zalunardo, C. Benden, U. Buergi, L. C. Huber, B. Isenring, M. M. Schuurmans, A. Gaspert, D. Holzmann, N. Müller, C. Schmid, B. Vrugt, T. Rechsteiner, A. Fritz, D. Maier, K. Desplanche, D. Koubi, F. Ernst, T. Paprotka, M. Schmitt, B. Wahl, J.-P. Boissel, G. Olivera-Botello, C. Trocmé, B. Toussaint, S. Bourgoin-Voillard, M. Séve, M. Benmerad, V. Siroux, R. Slama, C. Auffray, D. Charron, and J. Pellet

Subjects
lung transplantation, bronchiolitis obliterans syndrome, gene expression, biomarkers, blood, Immunologic diseases. Allergy, RC581-607
Abstract

Bronchiolitis obliterans syndrome (BOS), the main manifestation of chronic lung allograft dysfunction, leads to poor long-term survival after lung transplantation. Identifying predictors of BOS is essential to prevent the progression of dysfunction before irreversible damage occurs. By using a large set of 107 samples from lung recipients, we performed microarray gene expression profiling of whole blood to identify early biomarkers of BOS, including samples from 49 patients with stable function for at least 3 years, 32 samples collected at least 6 months before BOS diagnosis (prediction group), and 26 samples at or after BOS diagnosis (diagnosis group). An independent set from 25 lung recipients was used for validation by quantitative PCR (13 stables, 11 in the prediction group, and 8 in the diagnosis group). We identified 50 transcripts differentially expressed between stable and BOS recipients. Three genes, namely POU class 2 associating factor 1 (POU2AF1), T-cell leukemia/lymphoma protein 1A (TCL1A), and B cell lymphocyte kinase, were validated as predictive biomarkers of BOS more than 6 months before diagnosis, with areas under the curve of 0.83, 0.77, and 0.78 respectively. These genes allow stratification based on BOS risk (log-rank test p

Published
2018
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