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3. Computational Fluid Dynamics

Author

Thrane, L., Bras, A., Bakker, P., Brameshuber, W., Cazacliu, B., Ferrara, Liberato, Feys, D., Geiker, M., Gram, A., Grunewald, S., Mokeddem, S., Roussel, N. Rouquet N., Shah, S., Tregger, N., Uebachs, S., van Waarde, F., and Wallevik, J. E.

Published
2014

5. Fas-dependent apoptosis is impaired by SV40 T-antigen in transgenic liver

Author

Rouquet, N., Allemand, I., Molina, T., Bennoun, M., Briand, P., and Virginie JOULIN

Subjects
Male, Antigens, Polyomavirus Transforming, Antibodies, Monoclonal, Apoptosis, Mice, Transgenic, Simian virus 40, Receptors, Tumor Necrosis Factor, Mice, Liver Neoplasms, Experimental, Liver, Animals, Female, fas Receptor, Protein Kinase C
Abstract

A transgenic mouse model for hepatocarcinoma has been previously produced by targeting SV40 T-antigen expression to the liver. To evaluate the perturbation of cell death occurring during hepatocarcinogenesis, we examined the Fas-induced apoptosis on hepatocytes expressing T-antigen. Whereas anti-Fas antibody induced apoptosis in primary cultured normal hepatocytes, they imparted a weak cytotoxicity on primary cultured hepatocytes expressing T-antigen. This resistance of hepatic Fas-mediated apoptosis appears to result in an enhancement of a protective mechanism involving the protein kinase C signaling pathway rather than in a down-regulation of Fas-antigen expression. We further demonstrated that anti-Fas antibody does not have as efficient a lethal effect in T-antigen transgenic mice as in wild-type mice. The livers of transgenic mice injected with anti-Fas mAbs showed large intact regions with a few scattered apoptotic bodies: these regions strictly corresponded with carcinoma nodules, expressing high level of T-antigen. Our results describe a novel function for SV40 T-antigen which could contribute to viral pathogenesis by protecting infected cells against the host apoptotic defense mechanism.

6. Protection of hepatocytes from Fas-mediated apoptosis by a non-transforming SV40 T-antigen mutant

Author

Rouquet, N., Allemand, I., Grimber, G., thierry Molina, Briand, P., and Joulin, V.

Abstract

Apoptosis is crucial for the normal development of multicellular organisms and is also important for clearing injured cells, such as virus-infected cells or cancer cells. Defective regulation of apoptosis may contribute to viral pathogenesis and aetiology of cancer. Apoptosis of injured cells is principally triggered by the immune system through cytokines such as Fas-ligand and TNF-alpha. Thus, one of the functions of a viral oncogene, such as SV40T-antigen, may be to inhibit cytokine-mediated apoptosis. We previously demonstrated that Fas-mediated apoptosis of hepatocytes is blocked by the wild-type SV40T-antigen during hepatocarcinogenesis. We determined whether this inhibition was directly related to the T-antigen or whether it is a secondary event of cell transformation, by generating transgenic mice expressing a non-transforming T-antigen mutant able to bind endogenous p53 in the liver. This T-antigen mutant cannot induce hepatocarcinoma, unlike the wild-type T-antigen. However, like the wild-type T-antigen, the mutant was a potent inhibitor of apoptosis induced by the Fas-receptor, but not by the TNF-receptor. Therefore, SV40T-antigen has a new property; the inhibition of Fas-mediated apoptosis, which could facilitate the emergence of transformed hepatocytes, but is not sufficient to induce it.

7. Enhanced therapeutic effect of APAVAC immunotherapy in combination with dose-intense chemotherapy in dogs with advanced indolent B-cell lymphoma

Author

Fulvio Riondato, Nicole Rouquet, Damiano Stefanello, Silvia Sabattini, Luca Aresu, Laura Marconato, Stefano Comazzi, S. Pizzoni, Patrick Frayssinet, P Laganga, Marconato L, Stefanello, D, Sabattini, S, Comazzi, S, Riondato, F, Laganga, P, Frayssinet, P, Pizzoni, S, Rouquet, N, and Aresu, L.

Subjects
Male, Time Factors, Lymphoma, Immunology and Microbiology (all), medicine.medical_treatment, Gastroenterology, Dog, Intradermal injection, Prospective Studies, B-cell lymphoma, Heat shock proteins, Hydroxyapatite, Immunotherapy, Indolent lymphoma, Animals, Antineoplastic Agents, Cancer Vaccines, Dogs, Drug Therapy, Drug Therapy, Combination, Female, Injections, Intradermal, Lymphoma, B-Cell, Survival Analysis, Therapeutic Uses, Treatment Outcome, Infectious Diseases, Public Health, Environmental and Occupational Health, Veterinary (all), Molecular Medicine, Medicine (all), Heat shock protein, Toxicity, Combination, Public Health, medicine.medical_specialty, Injections, Internal medicine, Intradermal, medicine, Survival analysis, Chemotherapy, B-Cell, Environmental and Occupational Health, General Veterinary, General Immunology and Microbiology, business.industry, Therapeutic effect, medicine.disease, Surgery, business
Abstract

The aim of this non-randomized controlled trial was to compare time to progression (TTP), lymphoma-specific survival (LSS), and safety of an autologous vaccine (consisting of hydroxyapatite ceramic powder and Heat Shock Proteins purified from the dogs' tumors, HSPPCs-HA) plus chemotherapy versus chemotherapy alone in dogs with newly diagnosed, clinically advanced, histologically confirmed, multicentric indolent B-cell lymphoma. The vaccine was prepared from dogs' resected lymph nodes and administered as an intradermal injection. Forty-five client-owned dogs were enrolled: 20 dogs were treated with dose-intense chemotherapy, and 25 received concurrent immunotherapy. Both treatment arms were well tolerated, with no exacerbated toxicity in dogs also receiving the vaccine. TTP was significantly longer for dogs treated with chemo-immunotherapy versus those receiving chemotherapy only (median, 209 versus 85 days, respectively, P=0.015). LSS was not significantly different between groups: dogs treated with chemo-immunotherapy had a median survival of 349 days, and those treated with chemotherapy only had a median survival of 200 days (P=0.173). Among vaccinated dogs, those mounting an immune response had a significantly longer TTP and LSS than those with no detectable response (P=0.012 and P=0.003, respectively). Collectively these results demonstrate that vaccination with HSPPCs-HA may produce clinical benefits with no increased toxicity, thereby providing a strategy for enhancing chemotherapy in dogs with advanced indolent lymphoma.

Published
2015

8. Randomized, placebo-controlled, double-blinded chemoimmunotherapy clinical trial in a pet dog model of diffuse large B-cell lymphoma

Author

Laura Marconato, Stefano Comazzi, Luca Aresu, P Laganga, Massimo Vignoli, Federica Rossi, Nicole Rouquet, Lorenzo Pezzoli, Vito F. Leone, Patrick Frayssinet, Marconato L., Frayssinet P., Rouquet N., Comazzi S., Leone V.F., Laganga P., Rossi F., Vignoli M., Pezzoli L., and Aresu L.

Subjects
Oncology, medicine.medical_specialty, Cancer Research, Randomization, Lymphoma, medicine.medical_treatment, Antineoplastic Agents, Active immunotherapy, Cancer Vaccines, law.invention, Antineoplastic Agent, Dogs, Adjuvants, Immunologic, Randomized controlled trial, Double-Blind Method, Antigens, Neoplasm, law, Chemoimmunotherapy, Immunologic, hemic and lymphatic diseases, Internal medicine, Dog, medicine, Large B-Cell, Animals, Adjuvants, Dog Diseases, Antigens, Durapatite, Heat-Shock Proteins, Lymphoma, Large B-Cell, Diffuse, Chemotherapy, Animal, business.industry, Heat-Shock Protein, medicine.disease, Diffuse, Clinical trial, Immunology, Neoplasm, Dog Disease, business, Diffuse large B-cell lymphoma, Cancer Vaccine
Abstract

Purpose: Active immunotherapy is a promising antitumoral strategy; however its use in combination with chemotherapy in dogs with large B-cell lymphoma (DLBCL) remains largely untested. Heat shock proteins (HSP) bind the small peptides they chaperone (HSPPC), allowing for immunization of the host against a large repertoire of tumor-associated antigens. Hydroxylapatite vehicles HSPPCs and acts as an immunologic adjuvant. The aim of this study was to show that an autologous vaccine with hydroxylapatite and tumor-derived HSPPCs is safe and therapeutically effective in dogs with DLBCL. Experimental Design: Nineteen dogs with naturally occurring DLBCL were entered into a prospective randomized placebo-controlled double-blinded trial of HSPPCs–hydroxylapatite plus chemotherapy versus chemotherapy alone. Endpoints included time to progression (TTP), lymphoma-specific survival (LSS), and incidence of toxicoses. Results: Median first TTP after randomization to the vaccine arm was 304 days versus 41 days for the control arm (P = 0.0004). There was also a statistically significant difference in duration of second remission between the two groups (P = 0.02). Median LSS was 505 days for the vaccinated dogs versus 159 days for the unvaccinated dogs (P = 0.0018). Six vaccinated dogs achieved molecular remission, as shown by clonal immunoglobulin H (IgH) rearrangement. Toxicoses were comparable between the two treatment arms. Conclusions: The results of this trial demonstrate that the autologous vaccine tested here is safe and efficacious in prolonging TTP and LSS in dogs with DLBCL when used in combination with dose-intense chemotherapy. On the basis of these results, additional evaluation of this novel therapeutic strategy is warranted in human DLBCL. Clin Cancer Res; 20(3); 668–77. ©2013 AACR.

Published
2014

9. Minimal residual disease detection by flow cytometry and PARR in lymph node, peripheral blood and bone marrow, following treatment of dogs with diffuse large B-cell lymphoma

Author

Laura Marconato, Valeria Martini, Serena Ferraresso, Luca Aresu, Mauro Dacasto, Patrick Frayssinet, Nicole Rouquet, Fulvio Riondato, Eleonora Guadagnin, Stefano Comazzi, Arianna Aricò, Mery Giantin, Michele Drigo, Aresu L., Arico A., Ferraresso S., Martini V., Comazzi S., Riondato F., Giantin M., Dacasto M., Guadagnin E., Frayssinet P., Rouquet N., Drigo M., and Marconato L.

Subjects
Pathology, medicine.medical_specialty, Neoplasm, Residual, Lymphoma, Genes, Immunoglobulin Heavy Chain, Gene Rearrangement, T-Lymphocyte, PARR, Polymerase Chain Reaction, Flow cytometry, Dogs, Bone Marrow, hemic and lymphatic diseases, medicine, Dog, Animals, Dog Diseases, Lymph node, Canine Lymphoma, General Veterinary, biology, medicine.diagnostic_test, business.industry, Animal, Minimal residual disease, flow cytometry, lymphoma, minimal residual disease, Blood Chemical Analysi, Lymph Node, medicine.disease, Flow Cytometry, Prognosis, Transthyretin, medicine.anatomical_structure, biology.protein, Animal Science and Zoology, Bone marrow, Lymph Nodes, Lymphoma, Large B-Cell, Diffuse, Dog Disease, Neoplasm Recurrence, Local, business, Diffuse large B-cell lymphoma, Blood Chemical Analysis
Abstract

The most promising techniques for detecting minimal residual disease (MRD) in canine lymphoma are flow cytometry (FC) and polymerase chain reaction amplification of antigen receptor genes (PARR). However, the agreement between these methods has not been established. MRD was monitored by FC and PARR following treatment of dogs affected with diffuse large B-cell lymphoma (DLBCL), comparing results in lymph node (LN), peripheral blood (PB) and bone marrow (BM) samples. The prognostic impact of MRD on time to relapse (TTR) and lymphoma-specific survival (LSS) was also assessed.Fourteen dogs with previously untreated DLBCL were enrolled into the study; 10 dogs eventually relapsed, while four dogs with undetectable MRD were still in remission at the end of the study. At diagnosis, the concordance rate between FC and PARR was 100%, 78.6%, and 643% for LN, PB and BM, respectively. At the end of treatment, the agreement rates were 35.7%, 50%, and 57.1% for LN, PB and BM, respectively. At least one of the follow-up samples from dogs experiencing relapse was PARR.; conversely, FC was not able to detect MRD in seven of the dogs that relapsed. PARR was more sensitive than FC in predicting TTR, whereas the combination of PARR and FC was more sensitive than either technique alone in predicting LSS using PB samples. The results suggest that immunological and molecular techniques should be used in combination when monitoring for MRD in canine DLBCL. (C) 2014 Elsevier Ltd. All rights reserved.

Published
2014

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