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3. Radical oxygen species production induced by advanced oxidation protein products predicts clinical evolution and response to treatment in systemic sclerosis

Author

Servettaz, A., Guilpain, P., Goulvestre, C., Chereau, C., Hercend, C., Nicco, C., Guillevin, L., Weill, B., Mouthon, L., and Batteux, F.

Subjects
Oxidative stress -- Physiological aspects, Oxidative stress -- Research, Nitric oxide -- Health aspects, Oxidation-reduction reaction -- Research, Scleroderma (Disease) -- Development and progression, Scleroderma (Disease) -- Care and treatment, Systemic scleroderma -- Development and progression, Systemic scleroderma -- Care and treatment, Antioxidants -- Research, Radicals (Chemistry) -- Health aspects, Radicals (Chemistry) -- Research, Health
Published
2007

4. OP0307 Treatment of baff transgenic mice with ANTI-TNF: monoclonal ANTI-TNF are associated with a higher risk of lymphoma than etanercept

Author

Nocturne, G, primary, Bineta, L, additional, Boudaoud, S, additional, Pascaud, J, additional, Seror, R, additional, Nicco, C, additional, Chereau, C, additional, Mackay, F, additional, Vincent, F, additional, Lazure, T, additional, Ferlicot, S, additional, Stimmer, L, additional, Roulland, S, additional, Krzysiek, R, additional, Hacein-Bey, S, additional, Batteux, F, additional, and Mariette, X, additional

Published
2017
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5. Les souris BAFF transgéniques traitées par anti-TNF ont une augmentation du risque de lymphome sous anticorps monoclonaux et pas sous récepteur soluble

Author

Nocturne, G., primary, Ly, B., additional, Boudaoud, S., additional, Seror, R., additional, Nicco, C., additional, Chereau, C., additional, Kavian, N., additional, Batteux, F., additional, Mackay, F., additional, Vincent, F., additional, Lazure, T., additional, Krzysiek, R., additional, Hacein-Bey, S., additional, Stimmer, L., additional, Ferlicot, S., additional, and Mariette, X., additional

Published
2016
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8. Topical hemostatic powder promotes reepithelialization and reduces scar formation after extensive esophageal mucosal resection.

Author

Beye, B., Barret, M., Alatawi, A., Beuvon, F., Nicco, C., Pratico, C. A., Chereau, C., Chaussade, S., Batteux, F., and Prat, F.

Subjects
BARRETT'S esophagus, MUCOUS membranes, ENDOSCOPY, WOUND healing, HEMOSTATICS, LABORATORY swine, ANATOMY, THERAPEUTICS
Abstract

The development of techniques for endoscopic resection has provided new strategies for radical conservative treatment of superficial esophageal neoplasms, even those that are circumferential, such as Barrett's neoplasia. However, it is necessary to prevent the formation of scar tissue that can be responsible for esophageal strictures following circumferential resection. Preliminary data have suggested the possible efficacy of a hemostatic powder in the promotion of wound healing. The study aims to assess the effectiveness of Hemospray ( Cook Medical) in a swine model of post-endoscopic esophageal stricture. Our prospective controlled study included 21 pigs. A 6-cm circumferential submucosal dissection of the esophagus ( CESD) was performed in each pig. Group 1 ( n = 11) only underwent CESD and Group 2 ( n = 10) had repeated Hemospray applications after CESD. Clinical, endoscopic, and radiological monitoring were performed, blood levels of four inflammatory or pro-fibrotic cytokines were assessed, and histological analysis was performed. Median esophageal diameter was greater in the group treated with Hemospray (2 mm [1-3] vs. 3 mm [2-4], P = 0.01), and the rate of symptomatic esophageal stricture was 100% and 60% in Groups 1 and 2, respectively ( P = 0.09). The thicknesses of esophageal fibrosis and inflammatory cell infiltrate were significantly lower in Group 2 than in Group 1 ( P = 0.002 and 0.0003, respectively). The length of the neoepithelium was greater in Group 2 than in Group 1 ( P = 0.0004). Transforming growth factor- β levels were significantly lower in Group 2 than in Group 1 ( P = 0.01). The application of Hemospray after esophageal CESD reduces scar tissue formation and promotes reepithelialization, and therefore is a promising therapeutic approach in the prevention of post-endoscopic esophageal stricture. [ABSTRACT FROM AUTHOR]

Published
2016
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9. Détection de lésions néoplasiques colorectales par sonde endoscopique scintillante miniaturisée: étude de faisabilité in vivo dans un modèle murin de cancérogénèse colique

Author

Leblanc, S, primary, Anfre, P, additional, Burato, G, additional, Batteux, F, additional, Nicco, C, additional, Rouquette, A, additional, Chereau, C, additional, Noirault, E, additional, Hautefeuille, B, additional, Tillement, O, additional, and Prat, F, additional

Published
2012
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10. ENDOMETRIOSIS, ENDOMETRIUM, IMPLANTATION AND FALLOPIAN TUBE

Author

Nesbitt-Hawes, E., primary, Campbell, N., additional, Won, H., additional, Maley, P., additional, Henry, A., additional, Abbott, J., additional, Potdar, N., additional, Mason-Birks, S., additional, Elson, C. J., additional, Gelbaya, T. A., additional, Nardo, L. G., additional, Stavroulis, A., additional, Nnoaham, K., additional, Hummelshoj, L., additional, Zondervan, K., additional, Saridogan, E., additional, GSWH Consortium, W. E. R. F., additional, Chamie, L. P., additional, Soares, A. C. P., additional, Kimati, C. T., additional, Gomes, C., additional, Fettback, P., additional, Riboldi, M., additional, Serafini, P., additional, Lalitkumar, S., additional, Menezes, J., additional, Evdokia, D., additional, Gemzell-Danielsson, K., additional, Lalitkumar, P. G. L., additional, Bailey, J., additional, Newman, T. A., additional, Johnston, A., additional, Zisimopoulou, K., additional, White, M., additional, Sadek, K., additional, Shreeve, N., additional, Macklon, N., additional, Cheong, Y., additional, Al-Akoum, M., additional, Akoum, A., additional, Giles, J., additional, Garrido, N., additional, Vidal, C., additional, Mondion, M., additional, Gallo, C., additional, Ramirez, J., additional, Pellicer, A., additional, Remohi, J., additional, Ghosh, S., additional, Chattopadhyay, R., additional, Jana, S., additional, Goswami, S. K., additional, Bose, G., additional, Chakravarty, M., additional, Chowdhuri, K., additional, Chakravarty, B. N., additional, Kendirci Ceviren, A., additional, Ozcelik Tanriverdi, N., additional, Urfan, A., additional, Donmez, L., additional, Isikoglu, M., additional, Romano, A., additional, Schreinemacher, M. H., additional, Backes, W. H., additional, Slenter, J. M., additional, Xanthoulea, S. A., additional, Delvoux, B., additional, van Winden, L., additional, Beets-Tan, R. G., additional, Evers, J. L. H., additional, Dunselman, G. A. J., additional, Jana, S. K., additional, Chaudhury, K., additional, Maruyama, T., additional, Yamasaki, A., additional, Miyazaki, K., additional, Arase, T., additional, Uchida, H., additional, Yoshimura, Y., additional, Kaser, D., additional, Ginsburg, E., additional, Missmer, S., additional, Correia, K., additional, Racowsky, C., additional, Streuli, I., additional, Chouzenoux, S., additional, de Ziegler, D., additional, Chereau, C., additional, Weill, B., additional, Chapron, C., additional, Batteux, F., additional, Arianmanesh, M., additional, Fowler, P. A., additional, Al-Gubory, K. H., additional, Urata, Y., additional, Osuga, Y., additional, Izumi, G., additional, Nagai, M., additional, Takamura, M., additional, Yamamoto, N., additional, Saito, A., additional, Hasegawa, A., additional, Takemura, Y., additional, Harada, M., additional, Hirata, T., additional, Hirota, Y., additional, Yoshino, O., additional, Koga, K., additional, Taketani, Y., additional, Mohebbi, A., additional, Janan, A., additional, Nasri, S., additional, Lakpour, M. R., additional, Ramazanali, F., additional, Moini, A., additional, Aflatoonian, R., additional, Germeyer, A., additional, Novak, O., additional, Renke, T., additional, Jung, M., additional, Jackus, J., additional, Toth, B., additional, Strowitzki, T., additional, Bhattacharya, J., additional, Mitra, A., additional, Kundu, S., additional, Pal, M., additional, Kundu, A., additional, Gumusel, A., additional, Basar, M., additional, Yaprak, E., additional, Aslan, E., additional, Arda, O., additional, Ilvan, S., additional, Kayisli, U., additional, Guzel, E., additional, Haouzi, D., additional, Monzo, C., additional, Lehmann, S., additional, Hirtz, C., additional, Tiers, L., additional, Hamamah, S., additional, Choi, D., additional, Choi, J., additional, Jo, M., additional, Lee, E., additional, Shen, X., additional, Wang, B. I. N., additional, Li, X., additional, Tamura, I., additional, Maekawa, R., additional, Asada, H., additional, Tamura, H., additional, Sugino, N., additional, Liu, H., additional, Jiang, Y., additional, Chen, J., additional, Zhu, L., additional, Wang, B., additional, Yan, G., additional, Sun, H., additional, Coughlan, C., additional, Sinagra, M., additional, Ledger, W., additional, Li, T. C., additional, Laird, S. M., additional, Dafopoulos, K., additional, Vrekoussis, T., additional, Chalvatzas, N., additional, Messini, C. I., additional, Kalantaridou, S., additional, Georgoulias, P., additional, Messinis, I. E., additional, Makrigiannakis, A., additional, Xue, Q., additional, Xu, Y., additional, Zuo, W. L., additional, Zhang, L., additional, Shang, J., additional, Zhu, S. N., additional, Bulun, S. E., additional, Tomassetti, C., additional, Geysenbergh, B., additional, Meuleman, C., additional, Fieuws, S., additional, D'Hooghe, T., additional, Suginami, K., additional, Sato, Y., additional, Horie, A., additional, Matsumoto, H., additional, Fujiwara, H., additional, Konishi, I., additional, Jung, Y., additional, Cho, S., additional, Choi, Y., additional, Lee, B., additional, Seo, S., additional, Urman, B., additional, Yakin, K., additional, Oktem, O., additional, Alper, E., additional, Taskiran, C., additional, Aksoy, S., additional, Takeuchi, K., additional, Kurematsu, T., additional, Yu-ki, Y., additional, Fukumoto, Y., additional, Homan, Y., additional, Sata, Y., additional, Kuroki, Y., additional, Takeuchi, M., additional, Awata, S., additional, Muneyyirci-Delale, O., additional, Charles, C., additional, Anopa, J., additional, Osei-Tutu, N., additional, Dalloul, M., additional, Weedon, J., additional, Muney, A., additional, Stratton, P., additional, Yilmaz, B., additional, Kilic, S., additional, Aksakal, O., additional, Kelekci, S., additional, Aksoy, Y., additional, Lordlar, N., additional, Sut, N., additional, Gungor, T., additional, Chan, J., additional, Tan, C. W., additional, Lee, Y. H., additional, Tan, H. H., additional, Choolani, M., additional, Griffith, L., additional, Oldeweme, J., additional, Barcena de Arellano, M. L., additional, Reichelt, U., additional, Schneider, A., additional, Mechsner, S., additional, Munch, S., additional, Vercellino, G. F., additional, Chiantera, V., additional, Santoro, L., additional, D'Onofrio, F., additional, Campo, S., additional, Ferraro, P. M., additional, Tondi, P., additional, Gasbarrini, A., additional, Santoliquido, A., additional, Jung, M. H., additional, Kim, H. Y., additional, Arnold, J., additional, Buttner, A., additional, Karaer, A., additional, Celik, O., additional, Bay Karabulut, A., additional, Celik, E., additional, Kiran, T. R., additional, Simsek, O. Y., additional, Yilmaz, E., additional, Turkcuoglu, I., additional, Tanrikut, E., additional, Alieva, K., additional, Kulakova, E., additional, Ipatova, M., additional, Smolnikova, V., additional, and Kalinina, E., additional

Published
2012
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12. Effects of bile salts and aliphatic ionic surfactant on human lymphocyte proliferation.

Author

Podevin, P., Correia, L., Montet, J.C., Conti, F., Chereau, C., Calmus, Y., and Poupon, R.

Subjects
BILE salts, SURFACE active agents, LYMPHOCYTE transformation, PHYSIOLOGY
Abstract

Background The molecular mechanisms involved in the immunosuppressive properties of bile salts are partly unknown. Methods The aim of the study was to compare the effects of bile salts to those of various compounds with a steroid structure, or straight-chain hydrocarbons of different lengths and polar groups in the human mixed lymphocyte reaction. Results We showed a significant correlation between the effects of bile salts and a low critical micellar concentration, a high surface activity index, and the absence of conjugation. In addition to mixed lymphocyte reaction (MLR) inhibition, chenodeoxycholate (CDC) inhibit ConA-induced IL2 production without any effect on IL2 R expression. Fusidate, a negatively charged steroid, with physical properties comparable to those of deoxycholate, had similar effects. Cetyltrimethylammonium bromide (CTAB), which exhibited a very low critical micellar concentration, inhibited mixed lymphocyte reaction in an extent comparable to cyclosporin A. In contrast, aliphatic compounds with critical micellar concentrations in the same range as bile salts but with a lower molecular area had no effect. Conclusion Amphiphilic negatively charged molecules inhibit T-cell proliferation to an extent that is dependent upon their hydrophobicity. These results may be explained, at least in part, by a modification in the cell membrane lipid bilayer structure. [ABSTRACT FROM AUTHOR]

Published
2001
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15. Cavitation-induced release of liposomal chemotherapy in orthotopic murine pancreatic cancer models: A feasibility study.

Author

Camus M, Vienne A, Mestas JL, Pratico C, Nicco C, Chereau C, Marie JM, Moussatov A, Renault G, Batteux F, Lafon C, and Prat F

Subjects
Animals, Disease Models, Animal, Doxorubicin administration & dosage, Drug Delivery Systems methods, Feasibility Studies, Female, Liposomes, Male, Mice, Mice, Nude, Polyethylene Glycols administration & dosage, Rats, Rats, Inbred Lew, Ultrasonography, Antibiotics, Antineoplastic administration & dosage, Doxorubicin analogs & derivatives, Pancreatic Neoplasms drug therapy
Abstract

Targeted and triggered release of liposomal drug using ultrasound (US) induced cavitation represents a promising treatment modality to increase the therapeutic-toxicity ratio of encapsulated chemotherapy., Objectives: To study the feasibility and efficacy of a combination of focused US and liposomal doxorubicin (US-L-DOX) release in orthotopic murine models of pancreatic cancer., Material and Methods: A confocal US setup was developed to generate US inertial cavitation delivery in a controlled and reproducible manner and designed for two distinct murine orthotopic pancreatic cancer models. Controlled cavitation at 1 MHz was applied within the tumors after L-DOX injection according to a preliminary pharmacokinetic study., Results: In vitro studies confirmed that L-DOX was cytostatic. In vivo pharmacokinetic study showed L-DOX peak tumor accumulation at 48h. Feasibility of L-DOX injection and US delivery was demonstrated in both murine models. In a nude mouse model, at W9 after implantation (W5 after treatment), US-L-DOX group (median [IQR] 51.43 mm 3 [35.1-871.95]) exhibited significantly lower tumor volumes than the sham group (216.28 [96.12-1202.92]), the US group (359.44 [131.48-1649.25]), and the L-DOX group (255.94 [84.09-943.72]), and a trend, although not statistically significant, to a lower volume than Gemcitabine group (90.48 [42.14-367.78])., Conclusion: This study demonstrates that inertial cavitation can be generated to increase the therapeutic effect of drug-carrying liposomes accumulated in the tumor. This approach is potentially an important step towards a therapeutic application of cavitation-induced drug delivery in pancreatic cancer., (Copyright © 2019 Elsevier Masson SAS. All rights reserved.)

Published
2019
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16. Role of the protein kinase BRAF in the pathogenesis of endometriosis.

Author

Santulli P, Marcellin L, Chouzenoux S, Boulard V, Just PA, Nicco C, Chereau C, Tosti C, Chapron C, and Batteux F

Subjects
Adult, Animals, Apoptosis drug effects, Case-Control Studies, Cell Proliferation drug effects, Disease Models, Animal, Endometriosis pathology, Epithelial Cells metabolism, Female, Humans, Mice, Mice, Nude, Mitogen-Activated Protein Kinases metabolism, Protein Kinase Inhibitors pharmacology, Stromal Cells metabolism, Vemurafenib, Young Adult, Antineoplastic Agents pharmacology, Endometriosis drug therapy, Indoles pharmacology, Proto-Oncogene Proteins B-raf metabolism, Sulfonamides pharmacology
Abstract

Objective: Mitogen-activated protein kinases (MAPKs) are involved in the proliferation and survival of endometriotic lesions. Vemurafenib (PLX4032) is a novel protein kinase inhibitor that targets BRAF, a member of the MAPK pathway. The present study tested the in vitro and in vivo effects of PLX4032 on endometriotic cells., Research Design and Methods: We conducted a laboratory study in a tertiary-care university hospital from January 2013 to September 2013. We enrolled a cohort of 40 patients: 20 with histologically proven endometriosis and 20 unaffected women. A thorough surgical examination of the abdominopelvic cavity was performed on all of the study participants. Ex vivo stromal and epithelial cells were extracted from endometrial and endometriotic biopsies from both sets of patients. Proliferation, apoptosis, pERK/ERK ratio, cell cycle regulation (Cyclin D1 and CDK4) and inflammation (PTGS2) were explored with and without PLX4032 treatment. Human endometriotic lesions were implanted into 40 nude mice that were separated into two groups according to PLX4032 or vehicle treatment, which they received for four weeks, before sacrifice and histological examination., Results: Treating endometriotic cells with PLX4032 abrogated the phosphorylation of ERK, significantly reducing the pERK/ERK ratio in both epithelial and stromal cells from endometriotic women compared to the controls (p < 0.05). In addition, treatment with PLX4032 significantly decreased proliferation in both stromal and epithelial cells with a concomitant decrease in Cyclin D1/CDK4 complex and PTGS2 levels. Using a murine model of endometriosis, we observed that PLX4032-treated mice displayed a significant decrease in implant volume compared to the initial size; a slight, but non-significant, increase in size was observed in the vehicle-treated mice., Conclusion: Our data suggest that MAPKs and BRAF are involved in the pathogenesis of endometriosis. PLX4032-induced inhibition of BRAF controlled endometriotic growth, both in vitro and in vivo, and could constitute a promising target for the treatment of endometriosis.

Published
2016
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17. Chalcone-Coumarin derivatives as potential anti-cancer drugs: an in vitro and in vivo investigation.

Author

Jamier V, Marut W, Valente S, Chereau C, Chouzenoux S, Nicco C, Lemarechal H, Weill B, Kirsch G, Jacob C, and Batteux F

Subjects
Animals, Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Chalcones chemistry, Coumarins chemistry, Female, Heterografts, Humans, Inhibitory Concentration 50, Kidney pathology, Liver pathology, Mice, Inbred BALB C, Necrosis, Neoplasm Transplantation, Reactive Oxygen Species metabolism, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Chalcones pharmacology, Coumarins pharmacology
Abstract

Cancer cells display an overproduction of reactive oxygen species resulting from an exaggerated intrinsic oxidative stress. However, the concept of deleterious oxidants versus beneficial antioxidants has recently evolved. Indeed, molecules like natural coumarins have shown anti-oxidant or pro-oxidant properties depending on their intracellular concentration. Therefore, we have investigated the structure-activity relationship of a variety of coumarin derivatives in terms of cytotoxicity towards human and murine carcinoma cell lines (HT29, HepG2, A549, MCF7, OVCAR and CT26). Amongst those compounds, (E)-7-methoxy-4-(3-oxo-3- phenylprop-1-enyl)-2H-chromen-2-one and (E)-7-hydroxy-4-(3-(4-hydroxyphenyl)-3-oxoprop-1-enyl)-2H-chromen-2-one displayed the most potent cytotoxic effect on colon cancer cells, CT26, (IC50=4.9µM) linked to their pro-oxidant properties. Those compounds triggered the in vitro production of reactive oxygen species by tumor cells, leading to their death through a necrotic process. In vivo, molecules also slowed down tumor growth by 65.7% and 35.4%, respectively, without inducing significant side effects.

Published
2014
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18. Postresuscitation syndrome: potential role of hydroxyl radical-induced endothelial cell damage.

Author

Huet O, Dupic L, Batteux F, Matar C, Conti M, Chereau C, Lemiale V, Harrois A, Mira JP, Vicaut E, Cariou A, and Duranteau J

Subjects
Adult, Aged, Cardiopulmonary Resuscitation adverse effects, Cell Death, Cells, Cultured, Endothelial Cells physiology, Female, Glucosephosphate Dehydrogenase metabolism, Glutathione metabolism, Glutathione Peroxidase metabolism, Glutathione Reductase metabolism, Glycolysis physiology, Humans, Male, Middle Aged, Mitochondrial Diseases physiopathology, Out-of-Hospital Cardiac Arrest physiopathology, Reperfusion Injury blood, Reperfusion Injury physiopathology, Shock, Septic blood, Shock, Septic physiopathology, Superoxide Dismutase metabolism, Young Adult, Endothelial Cells metabolism, Hydroxyl Radical metabolism, Out-of-Hospital Cardiac Arrest blood
Abstract

Objective: After out of hospital cardiac arrest, it has been reported that endothelium dysfunction may occur during the postresuscitation syndrome. However, the consequences of the reperfusion phase on endothelial reactive oxygen species production and redox homeostasis have not been explored in out of hospital cardiac arrest patients., Design: Prospective, observational study., Setting: Medical intensive care unit in a university hospital., Patients: Twenty successfully resuscitated out of hospital cardiac arrest patients, seven septic shock patients, and ten healthy volunteers., Intervention: Plasma was collected from patients at admission and 12, 24, 36, 48, and 72 hrs after cardiac arrest. We studied the production of reactive oxygen species and cell survival during plasma perfusion using perfused endothelial cells (human umbilical vein endothelial cells) as a model. Cell antioxidant response was studied by measuring superoxide dismutase, glutathione peroxidase, and glutathione reductase activities and reduced and oxidized glutathione levels. Mitochondrial respiratory chain activity was assessed by measuring complex I, II, III, and IV activities and anaerobic glycolysis by measuring glucose-6-phosphate dehydrogenase activity., Measurements and Main Results: Using perfused endothelial cells as a model, we demonstrate that plasma from out of hospital cardiac arrest patients induced on naive human umbilical vein endothelial cells a significant and massive cell death compared to plasma from septic shock patients and healthy volunteers. An increase of reactive oxygen species production with a decrease in antioxidant defenses (superoxide dismutase, glutathione peroxidase, and glutathione reductase activities, reduced and oxidized glutathione levels) was observed. The metabolic consequence of plasma exposure showed that mitochondrial respiratory chain activity was significantly impaired and anaerobic glycolysis was significantly increased. Inhibiting hydroxyl radical production significantly decreased cell death, suggesting that plasma from out of hospital cardiac arrest induced significant cell death by triggering the Fenton reaction., Conclusion: Plasma from out of hospital cardiac arrest induces major endothelial toxicity with an acute pro-oxidant state in the cells and impairment of mitochondrial respiratory chain activity. This toxicity could be due to hydroxyl radical production by activation of the Fenton reaction.

Published
2011
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19. Mangafodipir protects against hepatic ischemia-reperfusion injury in mice.

Author

Coriat R, Leconte M, Kavian N, Bedda S, Nicco C, Chereau C, Goulvestre C, Weill B, Laurent A, and Batteux F

Subjects
Animals, Apoptosis, Aspartate Aminotransferases blood, Edetic Acid therapeutic use, Female, Glutathione metabolism, Ischemic Preconditioning, Lipid Peroxidation, Liver metabolism, Liver pathology, Mice, Mice, Inbred BALB C, Pyridoxal Phosphate therapeutic use, Reactive Oxygen Species metabolism, Reperfusion Injury metabolism, Survival Rate, Edetic Acid analogs & derivatives, Liver blood supply, Pyridoxal Phosphate analogs & derivatives, Reperfusion Injury prevention & control
Abstract

Introduction and Aim: Mangafodipir is a contrast agent used in magnetic resonance imaging that concentrates in the liver and displays pleiotropic antioxidant properties. Since reactive oxygen species are involved in ischemia-reperfusion damages, we hypothesized that the use of mangafodipir could prevent liver lesions in a mouse model of hepatic ischemia reperfusion injury. Mangafodipir (MnDPDP) was compared to ischemic preconditioning and intermittent inflow occlusion for the prevention of hepatic ischemia-reperfusion injury in the mouse., Methods: Mice were subjected to 70% hepatic ischemia (continuous ischemia) for 90 min. Thirty minutes before the ischemic period, either mangafodipir (10 mg/kg) or saline was injected intraperitoneally. Those experimental groups were compared with one group of mice preconditioned by 10 minutes' ischemia followed by 15 minutes' reperfusion, and one group with intermittent inflow occlusion. Hepatic ischemia-reperfusion injury was evaluated by measurement of serum levels of aspartate aminotransferase (ASAT) activity, histologic analysis of the livers, and determination of hepatocyte apoptosis (cytochrome c release, caspase 3 activity). The effect of mangafodipir on the survival rate of mice was studied in a model of total hepatic ischemia., Results: Mangafodipir prevented experimental hepatic ischemia-reperfusion injuries in the mouse as indicated by a reduction in serum ASAT activity (P<0.01), in liver tissue damages, in markers of apoptosis (P<0.01), and by higher rates of survival in treated than in untreated animals (P<0.001). The level of protection by mangafodipir was similar to that observed following intermittent inflow occlusion and higher than after ischemic preconditioning., Conclusions: Mangafodipir is a potential new preventive treatment for hepatic ischemia-reperfusion injury.

Published
2011
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21. Interleukin-15 production during liver allograft rejection in humans.

Author

Conti F, Frappier J, Dharancy S, Chereau C, Houssin D, Weill B, and Calmus Y

Subjects
Acute Disease, Adult, Biomarkers blood, Chronic Disease, Female, Graft Rejection diagnosis, Graft Rejection pathology, Humans, Immunity, Cellular, Interleukin-15 blood, Liver Transplantation pathology, Male, Middle Aged, Transplantation, Homologous immunology, Graft Rejection immunology, Interleukin-15 genetics, Liver Transplantation immunology
Abstract

Background: The activity of interleukin (IL)-15, a cytokine produced by macrophages, is similar to that of IL-2. We investigated whether IL-15 plays a role in liver allograft rejection., Methods: We evaluated plasma levels and intrahepatic expression of IL-15 in 35 patients after liver transplantation, and then analyzed in vitro the influence of anticalcineurin drugs or steroids on IL-15 production and secretion. Finally, we examined the effects of IL-15 on lymphocyte proliferation in mixed lymphocyte culture in the presence or absence of anticalcineurin drugs or steroids., Results: Plasma levels and in situ expression of IL-15 were enhanced during liver allograft rejection, particularly during steroid-resistant acute rejection and during chronic rejection. In vitro, IL-15 production and secretion were inhibited by neither anticalcineurin drugs nor steroids. Exogenous IL-15 enhanced cell-mediated immune response, and this effect was not inhibited by immunosuppressive drugs., Conclusions: IL-15 can play a role in the initiation and outcome of acute and chronic rejection. Anti-IL-15 therapy in combination with classic immunosuppression therapy might thus be beneficial in the prevention of acute, and especially chronic, allograft rejection.

Published
2003
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22. Low level of interleukin 10 synthesis during liver allograft rejection.

Author

Conti F, Boulland ML, Leroy-Viard K, Chereau C, Dousset B, Soubrane O, Weill B, and Calmus Y

Subjects
Acute Disease, Azathioprine therapeutic use, Cells, Cultured, Chronic Disease, Cyclosporine pharmacology, Graft Rejection pathology, Humans, Immunosuppressive Agents pharmacology, Immunosuppressive Agents therapeutic use, Interleukin-10 blood, Interleukin-10 genetics, Liver Transplantation pathology, Lymphocyte Culture Test, Mixed, Lymphocytes drug effects, Methylprednisolone therapeutic use, Tacrolimus pharmacology, Transplantation, Homologous, Graft Rejection immunology, Interleukin-10 biosynthesis, Liver Transplantation immunology, Lymphocytes immunology
Abstract

Interleukin 10 (IL-10) is a macrophage and T-cell-derived cytokine with potent immunosuppressive properties. To assess its role in liver allograft rejection, we evaluated the plasma level and in situ production of IL-10 after liver transplantation and designed in vitro studies to asses the effects of IL-10 on the allogeneic response. Normal controls and liver transplant recipients with acute rejection, chronic rejection, other complications (recurrent hepatitis C, biliary complications), or no complications were evaluated. The plasma IL-10 level was measured by an immunoenzymatic technique. IL-10 expression in the liver was detected on frozen liver biopsies by in situ hybridization and immunohistochemistry. Plasma IL-10 levels were not elevated during acute or chronic rejection, when compared with liver recipients with uncomplicated transplants. IL-10 mRNA and protein expressions in the liver graft were restricted to rare scattered sinusoidal cells of transplant recipients with acute or chronic rejection, as well as in those with no complications. In mixed lymphocyte cultures performed with peripheral blood mononuclear cells (PBMC) from normal subjects, IL-10 decreased the cell proliferation in a dose-dependent manner, and this immunosuppression was synergistic with that of cyclosporine or FK506. These findings indicate that IL-10 production is low during allograft rejection. Thus, IL-10 therapy in association with cyclosporine or FK506 might be proposed after liver transplantation.

Published
1998

23. Comparison between aortic and sinusoidal liver endothelial cells as targets of hyperacute xenogeneic rejection in the pig to human combination.

Author

Cattan P, Zhang B, Braet F, Atia N, Conti F, Conjeaud H, Weill B, Chereau C, Houssin D, and Calmus Y

Subjects
Acute Disease, Animals, Cells, Cultured, Complement System Proteins immunology, Humans, Liver immunology, Male, Organ Specificity, Antibodies, Heterophile immunology, Antigens, Heterophile immunology, Aorta immunology, Endothelium, Vascular immunology, Graft Rejection immunology, Immunoglobulin G immunology, Immunoglobulin M immunology, Liver blood supply, Swine immunology, Transplantation, Heterologous immunology
Abstract

Endothelial cells of aortic origin are usually used in vitro as targets of hyperacute xenogeneic rejection, although endothelial cells from organs may have different properties. The sensitivities of aortic and liver endothelial cells to hyperacute xenogeneic rejection were compared in the pig to human combination. Sinusoidal liver endothelial cells were isolated and purified by collagenase perfusion of pig livers, sedimentation on a percoll gradient and selective adherence. Purity and viability of isolated liver endothelial cells after adherence were 85+/-6% and >95%, respectively. Endothelial cells from pig aortae (purity and viability >95%) were isolated by scraping. Immunoblotting analysis of xenoantigens on liver and aortic endothelial cell membranes preparations showed identical patterns. The strongest bands revealed by human IgM were located between 110 and 135 kD, while human IgG detected two major bands at 115 and 75kD. The membrane expression of xenoantigens recognized by human sera, analyzed by flow cytometry, was significantly lower on liver than on aortic endothelial cells (IgM: P=0.0006; IgG: P=0.0009). However, the complement-dependent cytotoxic activity of human sera was the same whether liver (54.5+/-1.4%) or aortic endothelial cells (50.0+/-4.2%) were used as targets. Taken together, those results allow the use of aortic instead of sinusoidal liver endothelial cells in the characterization of pig antigens recognized by human natural antibodies.

Published
1996
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24. Study of the toxicity of various concentrations of 2-3-butanediol with University of Wisconsin solution or L15 culture medium in cultured porcine endothelial cells.

Author

Eschwege P, Chereau C, Randrianjohany A, Cardoso J, and Houssin D

Subjects
Adenosine, Allopurinol, Animals, Aorta, Cells, Cultured, Endothelium, Vascular cytology, Glutathione, Insulin, Organic Chemicals, Raffinose, Swine, Butylene Glycols toxicity, Cell Survival drug effects, Culture Media, Serum-Free, Endothelium, Vascular drug effects, Organ Preservation Solutions
Published
1995

25. Effect of cholestasis and bile acids on interferon-induced 2',5'-adenylate synthetase and NK cell activities.

Author

Podevin P, Calmus Y, Bonnefis MT, Veyrunes C, Chereau C, and Poupon R

Subjects
Animals, Chenodeoxycholic Acid pharmacology, Cholestasis immunology, Enzyme Induction drug effects, Humans, Killer Cells, Natural drug effects, Lymphocytes drug effects, Lymphocytes enzymology, Male, Rats, Rats, Wistar, Ursodeoxycholic Acid pharmacology, 2',5'-Oligoadenylate Synthetase biosynthesis, Bile Acids and Salts pharmacology, Cholestasis enzymology, Interferon-alpha pharmacology, Killer Cells, Natural immunology
Abstract

Background/aims: The mechanisms involved in resistance to interferon alfa in patients with chronic hepatitis C are unclear. Both cirrhosis and cholestasis have been shown to be predictive of resistance. The aim of this study was to evaluate the influence of cholestasis and bile acids on 2',5'-oligoadenylate synthetase and natural killer activities, which are both involved in the antiviral activity of interferon., Methods: 2',5'-Oligoadenylate synthetase activity was evaluated in spleen, liver, and isolated hepatocytes from bile duct-ligated rats, and the effect of bile acids in vitro on interferon-induced 2',5'-oligoadenylate synthetase and natural killer activities was examined in fresh mononuclear cells from healthy subjects., Results: Cholestasis had a time-dependent inhibitory effect on 2',5'-oligoadenylate synthetase activity in liver, spleen, and isolated hepatocytes from cholestatic rats (-70%, 86%, and 70% relative to baseline, respectively). In vitro, endogenous bile acids had a concentration-dependent inhibitory effect on interferon-induced 2',5'-oligoadenylate synthetase and natural killer activities, which was related to their structure. This inhibitory effect correlated with the surface activity index., Conclusions: Cholestasis and bile acids diminish the biological activity of interferon and natural killer activity. The results suggest a decrease in the antiviral defenses in cholestatic conditions.

Published
1995
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27. Prevention of hyperacute xenograft rejection by intravenous immunoglobulin in the pig-to-human combination.

Author

Gautreau C, Cardoso J, Woimant G, Zhao Z, Chereau C, Cherruau B, Vandeginste N, Devillier P, and Houssin D

Subjects
Acute Disease, Animals, Complement System Proteins immunology, Cytotoxicity, Immunologic, Endothelium, Vascular immunology, Erythrocytes immunology, Graft Rejection immunology, Humans, Immunosuppression Therapy methods, Lymphocytes immunology, Swine, Blood Transfusion, Graft Rejection prevention & control, Immunoglobulins, Intravenous therapeutic use, Transplantation, Heterologous immunology
Published
1994

29. Study of the target antigens of hyperacute xenogeneic rejection in discordant combinations.

Author

Calmus Y, Ayani E, Chereau C, Kahan A, Houssin D, and Weill B

Subjects
Acute Disease, Animals, Antibodies, Monoclonal, Antibody Specificity, Guinea Pigs, Histocompatibility Antigens analysis, Immunoblotting, Kidney immunology, Liver immunology, Lung immunology, Major Histocompatibility Complex, Male, Myocardium immunology, Rats, Rats, Inbred Lew, Antigens, Heterophile analysis, Graft Rejection immunology, Transplantation, Heterologous immunology
Published
1993

30. [Superacute xenogenic rejection: attempted treatment with anti-idiotypic antibodies].

Author

Salamé E, Chereau C, Calmus Y, Ayani E, Houssin D, and Weill B

Subjects
Acute Disease, Animals, Guinea Pigs, Heart Transplantation mortality, Rats, Transplantation, Heterologous, Antibodies, Anti-Idiotypic therapeutic use, Graft Rejection prevention & control, Heart Transplantation methods
Abstract

Heart xenotransplantation in the guinea-pig to rat model, a highly discordant combination, is invariably followed by a hyperacute rejection of the graft. Preformed IgMs were shown to be responsible for the destruction of the graft by stimulating the complement cascade. We tried to inhibit preformed antibodies, before transplantation, by inducing anti-idiotypic antibodies using autologous Fab' mu specific for guinea-pig endothelial cells. This treatment seems to exert a neutralizing effect on xenogeneic hyperimmunization, against guinea-pig endothelial cells but not against preformed anti-guinea-pig antibodies.

Published
1992

31. The role of natural IgM in the hyperacute rejection of discordant heart xenografts.

Author

Gambiez L, Salame E, Chereau C, Calmus Y, Cardoso J, Ayani E, Houssin D, and Weill B

Subjects
Animals, Endothelium, Vascular cytology, Endothelium, Vascular metabolism, Graft Rejection, Guinea Pigs, Immunoglobulin Fab Fragments metabolism, Immunoglobulin Fragments pharmacology, Male, Perfusion, Protein Binding drug effects, Rats, Rats, Inbred Lew, Time Factors, Transplantation, Heterologous, Heart Transplantation immunology, Immunoglobulin M physiology
Abstract

The mechanism of xenograft hyperacute rejection in discordant species combinations remains controversial. The purpose of this work was to study the role of natural antibodies in the hyperacute rejection of guinea pig hearts transplanted into rats, a highly discordant combination. This study was conducted in vitro, ex vivo, and in vivo. The endothelial cells of the graft being the first targets damaged in the process of hyperacute rejection, the binding of rat natural antibodies to guinea pig endothelial cells was studied by immunofluorescence. The study was carried out in vitro on guinea pig endothelial cells in culture, and ex vivo on isolated guinea pig hearts perfused with either rat serum or immunoglobulins or immunoglobulin fragments bearing the antigen-binding site. In vitro and ex vivo, rat natural IgM were found to bind specifically to guinea pig endothelial cells, since IgM fragments bearing the antigen-binding site (Fab mu and Fab' mu) could be detected on these cells. IgM fragments were able to inhibit the fixation of native IgM molecules. In contrast, rat IgG only bound to endothelial cells through Fc portions. Thus rat natural IgM might play a role in hyperacute rejection by binding to the graft endothelial cells and triggering the complement cascade activation. In order to test the role of natural IgM in vivo, isolated guinea pig hearts were first perfused with rat Fab' mu, which inhibit the binding of IgM and are unable to activate the complement cascade. These hearts were then transplanted into Lewis rats. The rejection time of Fab' mu-perfused guinea pig hearts was prolonged compared with hearts perfused with buffer or IgG F(ab')2. Therefore, in the guinea pig to rat combination, preventing the binding of the recipient's natural IgM to the graft endothelium delays the hyperacute rejection. In addition, natural IgM are likely to play a greater role than natural IgG.

Published
1992
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