32 results on '"Ingangi, Vincenzo"'
Search Results
2. A Macroscopic Mathematical Model For Cell Migration Assays Using A Real-Time Cell Analysis
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Di Costanzo, Ezio, Ingangi, Vincenzo, Angelini, Claudia, Carfora, Maria Francesca, Carriero, Maria Vincenza, and Natalini, Roberto
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Quantitative Biology - Cell Behavior ,92B05, 92C17, 35K99 - Abstract
Experiments of cell migration and chemotaxis assays have been classically performed in the so-called Boyden Chambers. A recent technology, xCELLigence Real Time Cell Analysis, is now allowing to monitor the cell migration in real time. This technology measures impedance changes caused by the gradual increase of electrode surface occupation by cells during the course of time and provide a Cell Index which is proportional to cellular morphology, spreading, ruffling and adhesion quality as well as cell number. In this paper we propose a macroscopic mathematical model, based on \emph{advection-reaction-diffusion} partial differential equations, describing the cell migration assay using the real-time technology. We carried out numerical simulations to compare simulated model dynamics with data of observed biological experiments on three different cell lines and in two experimental settings: absence of chemotactic signals (basal migration) and presence of a chemoattractant. Overall we conclude that our minimal mathematical model is able to describe the phenomenon in the real time scale and numerical results show a good agreement with the experimental evidences.
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- 2016
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3. Poly(L-glutamic acid)-co-poly(ethylene glycol) block copolymers for protein conjugation
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Maso, Katia, Grigoletto, Antonella, Raccagni, Lucia, Bellini, Marino, Marigo, Ilaria, Ingangi, Vincenzo, Suzuki, Akira, Hirai, Midori, Kamiya, Masaki, Yoshioka, Hiroki, and Pasut, Gianfranco
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- 2020
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4. Urokinase receptor derived peptides as potent inhibitors of the formyl peptide receptor type 1-triggered cell migration
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Yousif, Ali Munaim, Ingangi, Vincenzo, Merlino, Francesco, Brancaccio, Diego, Minopoli, Michele, Bellavita, Rosa, Novellino, Ettore, Carriero, Maria Vincenza, Carotenuto, Alfonso, and Grieco, Paolo
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- 2018
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5. Improving the Therapeutic Potential of G-CSF through Compact Circular PEGylation Based on Orthogonal Conjugations
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Grigoletto, Antonella, primary, Marotti, Valentina, additional, Tedeschini, Tommaso, additional, Campara, Benedetta, additional, Marigo, Ilaria, additional, Ingangi, Vincenzo, additional, and Pasut, Gianfranco, additional
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- 2023
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6. Targeting of immunosuppressive myeloid cells from glioblastoma patients by modulation of size and surface charge of lipid nanocapsules
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Pinton, Laura, Magri, Sara, Masetto, Elena, Vettore, Marina, Schibuola, Ilaria, Ingangi, Vincenzo, Marigo, Ilaria, Matha, Kevin, Benoit, Jean-Pierre, Della Puppa, Alessandro, Bronte, Vincenzo, Lollo, Giovanna, and Mandruzzato, Susanna
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- 2020
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7. Supplementary Data S3 from Disabled Homolog 2 Controls Prometastatic Activity of Tumor-Associated Macrophages
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Marigo, Ilaria, primary, Trovato, Rosalinda, primary, Hofer, Francesca, primary, Ingangi, Vincenzo, primary, De Sanctis, Francesco, primary, Ugel, Stefano, primary, Canè, Stefania, primary, Simonelli, Anna, primary, Lamolinara, Alessia, primary, Iezzi, Manuela, primary, Fassan, Matteo, primary, Rugge, Massimo, primary, Boschi, Federico, primary, Borile, Giulia, primary, Eisenhaure, Thomas, primary, Sarkizova, Siranush, primary, Lieb, David, primary, Hacohen, Nir, primary, Azzolin, Luca, primary, Piccolo, Stefano, primary, Lawlor, Rita, primary, Scarpa, Aldo, primary, Carbognin, Luisa, primary, Bria, Emilio, primary, Bicciato, Silvio, primary, Murray, Peter J., primary, and Bronte, Vincenzo, primary
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- 2023
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8. Data from Disabled Homolog 2 Controls Prometastatic Activity of Tumor-Associated Macrophages
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Marigo, Ilaria, primary, Trovato, Rosalinda, primary, Hofer, Francesca, primary, Ingangi, Vincenzo, primary, De Sanctis, Francesco, primary, Ugel, Stefano, primary, Canè, Stefania, primary, Simonelli, Anna, primary, Lamolinara, Alessia, primary, Iezzi, Manuela, primary, Fassan, Matteo, primary, Rugge, Massimo, primary, Boschi, Federico, primary, Borile, Giulia, primary, Eisenhaure, Thomas, primary, Sarkizova, Siranush, primary, Lieb, David, primary, Hacohen, Nir, primary, Azzolin, Luca, primary, Piccolo, Stefano, primary, Lawlor, Rita, primary, Scarpa, Aldo, primary, Carbognin, Luisa, primary, Bria, Emilio, primary, Bicciato, Silvio, primary, Murray, Peter J., primary, and Bronte, Vincenzo, primary
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- 2023
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9. Supplementary Data from Disabled Homolog 2 Controls Prometastatic Activity of Tumor-Associated Macrophages
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Marigo, Ilaria, primary, Trovato, Rosalinda, primary, Hofer, Francesca, primary, Ingangi, Vincenzo, primary, De Sanctis, Francesco, primary, Ugel, Stefano, primary, Canè, Stefania, primary, Simonelli, Anna, primary, Lamolinara, Alessia, primary, Iezzi, Manuela, primary, Fassan, Matteo, primary, Rugge, Massimo, primary, Boschi, Federico, primary, Borile, Giulia, primary, Eisenhaure, Thomas, primary, Sarkizova, Siranush, primary, Lieb, David, primary, Hacohen, Nir, primary, Azzolin, Luca, primary, Piccolo, Stefano, primary, Lawlor, Rita, primary, Scarpa, Aldo, primary, Carbognin, Luisa, primary, Bria, Emilio, primary, Bicciato, Silvio, primary, Murray, Peter J., primary, and Bronte, Vincenzo, primary
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- 2023
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10. Structure-function relationship of an Urokinase Receptor-derived peptide which inhibits the Formyl Peptide Receptor type 1 activity
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Minopoli, Michele, Polo, Andrea, Ragone, Concetta, Ingangi, Vincenzo, Ciliberto, Gennaro, Pessi, Antonello, Sarno, Sabrina, Budillon, Alfredo, Costantini, Susan, and Carriero, Maria Vincenza
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- 2019
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11. Myeloid Cells as Clinical Biomarkers for Immune Checkpoint Blockade
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Peranzoni, Elisa, Ingangi, Vincenzo, Masetto, Elena, Pinton, Laura, and Marigo, Ilaria
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lcsh:Immunologic diseases. Allergy ,circulating biomarkers ,immune checkpoint inhibitors ,MDSC (myeloid-derived suppressor cell) ,myeloid cells ,predictive biomarkers ,resistance to immunotherapy ,TAM (tumor-associated macrophage) ,tumor biomarkers ,Animals ,Clinical Studies as Topic ,Drug Evaluation, Preclinical ,Humans ,Immune Checkpoint Inhibitors ,Immune Checkpoint Proteins ,Molecular Targeted Therapy ,Myeloid Cells ,Myeloid-Derived Suppressor Cells ,Organ Specificity ,Treatment Outcome ,Biomarkers ,Immunology ,Review ,Immunology and Allergy ,Preclinical ,Drug Evaluation ,lcsh:RC581-607 - Abstract
Immune checkpoint inhibitors are becoming standard treatments in several cancer types, profoundly changing the prognosis of a fraction of patients. Currently, many efforts are being made to predict responders and to understand how to overcome resistance in non-responders. Given the crucial role of myeloid cells as modulators of T effector cell function in tumors, it is essential to understand their impact on the clinical outcome of immune checkpoint blockade and on the mechanisms of immune evasion. In this review we focus on the existing clinical evidence of the relation between the presence of myeloid cell subsets and the response to anti-PD(L)1 and anti-CTLA-4 treatment. We highlight how circulating and tumor-infiltrating myeloid populations can be used as predictive biomarkers for immune checkpoint inhibitors in different human cancers, both at baseline and on treatment. Moreover, we propose to follow the dynamics of myeloid cells during immunotherapy as pharmacodynamic biomarkers. Finally, we provide an overview of the current strategies tested in the clinic that use myeloid cell targeting together with immune checkpoint blockade with the aim of uncovering the most promising approaches for effective combinations.
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- 2020
12. Additional file 1 of Targeting of immunosuppressive myeloid cells from glioblastoma patients by modulation of size and surface charge of lipid nanocapsules
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Pinton, Laura, Magri, Sara, Masetto, Elena, Vettore, Marina, Schibuola, Ilaria, Ingangi, Vincenzo, Marigo, Ilaria, Matha, Kevin, Benoit, Jean-Pierre, Puppa, Alessandro Della, Bronte, Vincenzo, Lollo, Giovanna, and Mandruzzato, Susanna
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Additional file 1. Supplementary materials and methods. Isolation of cell populations from peripheral blood and tissue of GBM patients, preparation of lipid nanocapsules, LNC incorporation studies, multiparametric flow cytometry, confocal microscopy, statistical analysis.
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- 2020
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13. Disabled Homolog 2 Controls Prometastatic Activity of Tumor-Associated Macrophages
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Marigo, Ilaria, primary, Trovato, Rosalinda, additional, Hofer, Francesca, additional, Ingangi, Vincenzo, additional, Desantis, Giacomo, additional, Leone, Kevin, additional, De Sanctis, Francesco, additional, Ugel, Stefano, additional, Canè, Stefania, additional, Simonelli, Anna, additional, Lamolinara, Alessia, additional, Iezzi, Manuela, additional, Fassan, Matteo, additional, Rugge, Massimo, additional, Boschi, Federico, additional, Borile, Giulia, additional, Eisenhaure, Thomas, additional, Sarkizova, Siranush, additional, Lieb, David, additional, Hacohen, Nir, additional, Azzolin, Luca, additional, Piccolo, Stefano, additional, Lawlor, Rita, additional, Scarpa, Aldo, additional, Carbognin, Luisa, additional, Bria, Emilio, additional, Bicciato, Silvio, additional, Murray, Peter J., additional, and Bronte, Vincenzo, additional
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- 2020
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14. Myeloid Cells as Clinical Biomarkers for Immune Checkpoint Blockade
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Peranzoni, Elisa, primary, Ingangi, Vincenzo, additional, Masetto, Elena, additional, Pinton, Laura, additional, and Marigo, Ilaria, additional
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- 2020
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15. Targeting of immunosuppressive myeloid cells from glioblastoma patients by modulation of size and surface charge of lipid nanocapsules
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Pinton, Laura, primary, Magri, Sara, additional, Masetto, Elena, additional, Vettore, Marina, additional, Schibuola, Ilaria, additional, Ingangi, Vincenzo, additional, Marigo, Ilaria, additional, Matha, Kevin, additional, Benoit, Jean-Pierre, additional, Puppa, Alessandro Della, additional, Bronte, Vincenzo, additional, Lollo, Giovanna, additional, and Mandruzzato, Susanna, additional
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- 2020
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16. Targeting of immunosuppressive myeloid cells from glioblastoma patients by modulation of size and surface charge of lipid nanocapsules
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Pinton, Laura, primary, Magri, Sara, additional, Masetto, Elena, additional, Vettore, Marina, additional, Schibuola, Ilaria, additional, Ingangi, Vincenzo, additional, Marigo, Ilaria, additional, Matha, Kevin, additional, Benoit, Jean-Pierre, additional, Puppa, Alessandro Della, additional, Bronte, Vincenzo, additional, Lollo, Giovanna, additional, and Mandruzzato, Susanna, additional
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- 2019
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17. Role of Microenvironment on the Fate of Disseminating Cancer Stem Cells
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Ingangi, Vincenzo, primary, Minopoli, Michele, additional, Ragone, Concetta, additional, Motti, Maria Letizia, additional, and Carriero, Maria Vincenza, additional
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- 2019
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18. Additional file 4: Figure S2. of Targeting the cross-talk between Urokinase receptor and Formyl peptide receptor type 1 to prevent invasion and trans-endothelial migration of melanoma cells
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Ragone, Concetta, Minopoli, Michele, Ingangi, Vincenzo, Botti, Giovanni, Fratangelo, Federica, Pessi, Antonello, Stoppelli, Maria, Ascierto, Paolo, Ciliberto, Gennaro, Motti, Maria, and Carriero, Maria
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Proliferation rate of melanoma cells. Cell proliferation of the indicated melanoma cell lines assessed by monitoring impedance by RTCA xCELLigence system. The reported doubling times were calculated from the cell growth curves, during exponential growth. Data represent mean ± SD from a quadruplicate experiment representative of 3 replicates. (PDF 120 kb)
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- 2017
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19. Additional file 1: Figure S1. of Targeting the cross-talk between Urokinase receptor and Formyl peptide receptor type 1 to prevent invasion and trans-endothelial migration of melanoma cells
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Ragone, Concetta, Minopoli, Michele, Ingangi, Vincenzo, Botti, Giovanni, Fratangelo, Federica, Pessi, Antonello, Stoppelli, Maria, Ascierto, Paolo, Ciliberto, Gennaro, Motti, Maria, and Carriero, Maria
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Uncropped images of immunoblots. Full blots from Fig. 1b, Inset of the Fig. 2a, c, Fig. 4b, and Fig. 7a. (PDF 164Â kb)
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- 2017
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20. Targeting the cross-talk between Urokinase receptor and Formyl peptide receptor type 1 to prevent invasion and trans-endothelial migration of melanoma cells
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Ragone, Concetta, primary, Minopoli, Michele, additional, Ingangi, Vincenzo, additional, Botti, Giovanni, additional, Fratangelo, Federica, additional, Pessi, Antonello, additional, Stoppelli, Maria Patrizia, additional, Ascierto, Paolo Antonio, additional, Ciliberto, Gennaro, additional, Motti, Maria Letizia, additional, and Carriero, Maria Vincenza, additional
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- 2017
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21. Melanoma and immunotherapy bridge 2015
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Nanda, Vashisht G. Y., Peng, Weiyi, Hwu, Patrick, Davies, Michael A., Ciliberto, Gennaro, Fattore, Luigi, Malpicci, Debora, Aurisicchio, Luigi, Ascierto, Paolo Antonio, Croce, Carlo M., Mancini, Rita, Spranger, Stefani, Gajewski, Thomas F., Wang, Yangyang, Ferrone, Soldano, Vanpouille-Box, Claire, Wennerberg, Erik, Pilones, Karsten A., Formenti, Silvia C., Demaria, Sandra, Tang, Haidong, Wang, Yang, Fu, Yang-Xin, Dummer, Reinhard, Puzanov, Igor, Tarhini, Ahmad, Chauvin, Joe-Marc, Pagliano, Ornella, Fourcade, Julien, Sun, Zhaojun, Wang, Hong, Sanders, Cindy, Kirkwood, John M., Chen, Tseng-hui Timothy, Maurer, Mark, Korman, Alan J., Zarour, Hassane M., Stroncek, David F., Huber, Veronica, Rivoltini, Licia, Thurin, Magdalena, Rau, Tilman, Lugli, Alessandro, Pagès, Franck, Camarero, Jorge, Sancho, Arantxa, Jommi, Claudio, de Coaña, Yago Pico, Wolodarski, Maria, Yoshimoto, Yuya, Gentilcore, Giusy, Poschke, Isabel, Masucci, Giuseppe V., Hansson, Johan, Kiessling, Rolf, Scognamiglio, Giosuè, Sabbatino, Francesco, Marino, Federica Zito, Anniciello, Anna Maria, Cantile, Monica, Cerrone, Margherita, Scala, Stefania, D’alterio, Crescenzo, Ianaro, Angela, Cirin, Giuseppe, Liguori, Giuseppina, Bott, Gerardo, Chapman, Paul B., Robert, Caroline, Larkin, James, Haanen, John B., Ribas, Antoni, Hogg, David, Hamid, Omid, Testori, Alessandro, Lorigan, Paul, Sosman, Jeffrey A., Flaherty, Keith T., Yue, Huibin, Coleman, Shelley, Caro, Ivor, Hauschild, Axel, McArthur, Grant A., Sznol, Mario, Callahan, Margaret K., Kluger, Harriet, Postow, Michael A., Gordan, RuthAnn, Segal, Neil H., Rizvi, Naiyer A., Lesokhin, Alexander, Atkins, Michael B., Burke, Matthew M., Ralabate, Amanda, Rivera, Angel, Kronenberg, Stephanie A., Agunwamba, Blessing, Ruisi, Mary, Horak, Christine, Jiang, Joel, Wolchok, Jedd, Ascierto, Paolo A., Liszkay, Gabriella, Maio, Michele, Mandalà, Mario, Demidov, Lev, Stoyakovskiy, Daniil, Thomas, Luc, de la Cruz-Merino, Luis, Atkinson, Victoria, Dutriaux, Caroline, Garbe, Claus, Wongchenko, Matthew, Chang, Ilsung, Koralek, Daniel O., Rooney, Isabelle, Yan, Yibing, Dréno, Brigitte, Sullivan, Ryan, Patel, Manish, Hodi, Stephen, Amaria, Rodabe, Boasberg, Peter, Wallin, Jeffrey, He, Xian, Cha, Edward, Richie, Nicole, Ballinger, Marcus, Smith, David C., Bauer, Todd M., Wasser, Jeffrey S., Luke, Jason J., Balmanoukian, Ani S., Kaufman, David R., Zhao, Yufan, Maleski, Janet, Leopold, Lance, Gangadhar, Tara C., Long, Georgina V., Michielin, Olivier, VanderWalde, Ari, Andtbacka, Robert H. I., Cebon, Jonathan, Fernandez, Eugenio, Malvehy, Josep, Olszanski, Anthony J., Gause, Christine, Chen, Lisa, Chou, Jeffrey, Stephen Hodi, F., Brady, Benjamin, Mortier, Laurent, Hassel, Jessica C., Rutkowski, Piotr, McNeil, Catriona, Kalinka-Warzocha, Ewa, Lebbé, Celeste, Ny, Lars, Chacon, Matias, Queirolo, Paola, Loquai, Carmen, Cheema, Parneet, Berrocal, Alfonso, Eizmendi, Karmele Mujika, Bar-Sela, Gil, Hardy, Helene, Weber, Jeffrey S., Grob, Jean-Jacques, Marquez-Rodas, Ivan, Schmidt, Henrik, Briscoe, Karen, Baurain, Jean-François, Wolchok, Jedd D., Pinto, Rosamaria, De Summa, Simona, Garrisi, Vito Michele, Strippoli, Sabino, Azzariti, Amalia, Guida, Gabriella, Guida, Michele, Tommasi, Stefania, Jacquelot, Nicolas, Enot, David, Flament, Caroline, Pitt, Jonathan M., Vimond, Nadège, Blattner, Carolin, Yamazaki, Takahiro, Roberti, Maria-Paula, Vetizou, Marie, Daillere, Romain, Poirier-Colame, Vichnou, la Semeraro, Michaë, Caignard, Anne, Slingluff, Craig L, Sallusto, Federica, Rusakiewicz, Sylvie, Weide, Benjamin, Marabelle, Aurélien, Kohrt, Holbrook, Dalle, Stéphane, Cavalcanti, Andréa, Kroemer, Guido, Di Giacomo, Anna Maria, Maio, Michaele, Wong, Phillip, Yuan, Jianda, Umansky, Viktor, Eggermont, Alexander, Zitvogel, Laurence, Anna, Passarelli, Marco, Tucci, Stefania, Stucci, Francesco, Mannavola, Mariaelena, Capone, Gabriele, Madonna, Antonio, Ascierto Paolo, Franco, Silvestris, Roberti, María Paula, Enot, David P., Semeraro, Michaela, Jégou, Sarah, Flores, Camila, Kwon, Byoung S., Anderson, Ana Carrizossa, Borg, Christophe, Aubin, François, Ayyoub, Maha, De Presbiteris, Anna Lisa, Cordaro, Fabiola Gilda, Camerlingo, Rosa, Fratangelo, Federica, Mozzillo, Nicola, Pirozzi, Giuseppe, Patriarca, Eduardo J., Caputo, Emilia, Motti, Maria Letizia, Falcon, Rosaria, Miceli, Roberta, Capone, Mariaelena, Madonna, Gabriele, Mallardo, Domenico, Carrier, Maria Vincenza, Panza, Elisabetta, De Cicco, Paola, Armogida, Chiara, Ercolano, Giuseppe, Botti, Gerardo, Cirino, Giuseppe, Sandru, Angela, Blank, Miri, Balatoni, Timea, Olasz, Judit, Farkas, Emil, Szollar, Andras, Savolt, Akos, Godeny, Maria, Csuka, Orsolya, Horvath, Szabolcs, Eles, Klara, Shoenfeld, Yehuda, Kasler, Miklos, Costantini, Susan, Capone, Francesca, Moradi, Farnaz, Berglund, Pontus, Leandersson, Karin, Linnskog, Rickard, Andersson, Tommy, Prasad, Chandra Prakash, Nigro, Cristiana Lo, Lattanzio, Laura, Wang, Hexiao, Proby, Charlotte, Syed, Nelofer, Occelli, Marcella, Cauchi, Carolina, Merlano, Marco, Harwood, Catherine, Thompson, Alastair, Crook, Tim, Bifulco, Katia, Ingangi, Vincenzo, Minopoli, Michele, Ragone, Concetta, Pessi, Antonello, Mannavola, Francesco, D’Oronzo, Stella, Felici, Claudia, Tucci, Marco, Doronzo, Antonio, Silvestris, Franco, Ferretta, Anna, Guida, Stefania, Maida, Imma, Cocco, Tiziana, Passarelli, Anna, Quaresmini, Davide, Franzese, Ornella, Palermo, Belinda, Di Donna, Cosmo, Sperduti, Isabella, Foddai, MariaLaura, Stabile, Helena, Gismondi, Angela, Santoni, Angela, Nisticò, Paola, Sponghini, Andrea P., Platini, Francesca, Marra, Elena, Rondonotti, David, Alabiso, Oscar, Fierro, Maria T., Savoia, Paola, Stratica, Florian, Quaglino, Pietro, Di Monta, Gianluca, Corrado, Caracò, Di Marzo, Massimiliano, Ugo, Marone, Di Cecilia, Maria Luisa, Nicola, Mozzillo, Fusciello, Celeste, Marra, Antonio, Guarrasi, Rosario, Baldi, Carlo, Russo, Rosa, Di Giulio, Giovanni, Faiola, Vincenzo, Zeppa, Pio, Pepe, Stefano, Gambale, Elisabetta, Carella, Consiglia, Di Paolo, Alessandra, De Tursi, Michele, Marra, Laura, De Murtas, Fara, Sorrentino, Valeria, Voinea, Silviu, Panaitescu, Eugenia, Bolovan, Madalina, Stanciu, Adina, Cinca, Sabin, Botti, Chiara, Aquino, Gabriella, Anniciello, Annamaria, Fortes, Cristina, Mastroeni, Simona, Caggiati, Alessio, Passarelli, Francesca, Zappalà, Alba, Capuano, Maria, Bono, Riccardo, Nudo, Maurizio, Marino, Claudia, Michelozzi, Paola, De Biasio, Valeria, Battarra, Vincenzo C., Formenti, Silvia, Ascierto, Maria Libera, McMiller, Tracee L., Berger, Alan E., Danilova, Ludmila, Anders, Robert A., Netto, George J., Xu, Haiying, Pritchard, Theresa S., Fan, Jinshui, Cheadle, Chris, Cope, Leslie, Drake, Charles G., Pardoll, Drew M., Taube, Janis M., Topalian, Suzanne L., Gnjatic, Sacha, Nataraj, Sarah, Imai, Naoko, Rahman, Adeeb, Jungbluth, Achim A., Pan, Linda, Venhaus, Ralph, Park, Andrew, Lehmann, Frédéric F., Lendvai, Nikoletta, Cohen, Adam D., Cho, Hearn J., Daniel, Speiser, and Hirsh, Vera
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Medicine(all) ,Biochemistry, Genetics and Molecular Biology(all) ,Meeting Abstracts - Abstract
Table of contents MELANOMA BRIDGE 2015 KEYNOTE SPEAKER PRESENTATIONS Molecular and immuno-advances K1 Immunologic and metabolic consequences of PI3K/AKT/mTOR activation in melanoma Vashisht G. Y. Nanda, Weiyi Peng, Patrick Hwu, Michael A. Davies K2 Non-mutational adaptive changes in melanoma cells exposed to BRAF and MEK inhibitors help the establishment of drug resistance Gennaro Ciliberto, Luigi Fattore, Debora Malpicci, Luigi Aurisicchio, Paolo Antonio Ascierto, Carlo M. Croce, Rita Mancini K3 Tumor-intrinsic beta-catenin signaling mediates tumor-immune avoidance Stefani Spranger, Thomas F. Gajewski K4 Intracellular tumor antigens as a source of targets of antibody-based immunotherapy of melanoma Yangyang Wang, Soldano Ferrone Combination therapies K5 Harnessing radiotherapy to improve responses to immunotherapy in cancer Claire Vanpouille-Box, Erik Wennerberg, Karsten A. Pilones, Silvia C. Formenti, Sandra Demaria K6 Creating a T cell-inflamed tumor microenvironment overcomes resistance to checkpoint blockade Haidong Tang, Yang Wang, Yang-Xin Fu K7 Biomarkers for treatment decisions? Reinhard Dummer K8 Combining oncolytic therapies in the era of checkpoint inhibitors Igor Puzanov K9 Immune checkpoint blockade for melanoma: should we combine or sequence ipilimumab and PD-1 antibody therapy? Michael A. Postow News in immunotherapy K10 An update on adjuvant and neoadjuvant therapy for melanom Ahmad Tarhini K11 Targeting multiple inhibitory receptors in melanoma Joe-Marc Chauvin, Ornella Pagliano, Julien Fourcade, Zhaojun Sun, Hong Wang, Cindy Sanders, John M. Kirkwood, Tseng-hui Timothy Chen, Mark Maurer, Alan J. Korman, Hassane M. Zarour K12 Improving adoptive immune therapy using genetically engineered T cells David F. Stroncek Tumor microenvironment and biomarkers K13 Myeloid cells and tumor exosomes: a crosstalk for assessing immunosuppression? Veronica Huber, Licia Rivoltini K14 Update on the SITC biomarker taskforce: progress and challenges Magdalena Thurin World-wide immunoscore task force: an update K15 The immunoscore in colorectal cancer highlights the importance of digital scoring systems in surgical pathology Tilman Rau, Alessandro Lugli K16 The immunoscore: toward an integrated immunomonitoring from the diagnosis to the follow up of cancer’s patients Franck Pagès Economic sustainability of melanoma treatments: regulatory, health technology assessment and market access issues K17 Nivolumab, the regulatory experience in immunotherapy Jorge Camarero, Arantxa Sancho K18 Evidence to optimize access for immunotherapies Claudio Jommi ORAL PRESENTATIONS Molecular and immuno-advances O1 Ipilimumab treatment results in CD4 T cell activation that is concomitant with a reduction in Tregs and MDSCs Yago Pico de Coaña, Maria Wolodarski, Yuya Yoshimoto, Giusy Gentilcore, Isabel Poschke, Giuseppe V. Masucci, Johan Hansson, Rolf Kiessling O2 Evaluation of prognostic and therapeutic potential of COX-2 and PD-L1 in primary and metastatic melanoma Giosuè Scognamiglio, Francesco Sabbatino, Federica Zito Marino, Anna Maria Anniciello, Monica Cantile, Margherita Cerrone, Stefania Scala, Crescenzo D’alterio, Angela Ianaro, Giuseppe Cirino, Paolo Antonio Ascierto, Giuseppina Liguori, Gerardo Botti O3 Vemurafenib in patients with BRAFV600 mutation–positive metastatic melanoma: final overall survival results of the BRIM-3 study Paul B. Chapman, Caroline Robert, James Larkin, John B. Haanen, Antoni Ribas, David Hogg, Omid Hamid, Paolo Antonio Ascierto, Alessandro Testori, Paul Lorigan, Reinhard Dummer, Jeffrey A. Sosman, Keith T. Flaherty, Huibin Yue, Shelley Coleman, Ivor Caro, Axel Hauschild, Grant A. McArthur O4 Updated survival, response and safety data in a phase 1 dose-finding study (CA209-004) of concurrent nivolumab (NIVO) and ipilimumab (IPI) in advanced melanoma Mario Sznol, Margaret K. Callahan, Harriet Kluger, Michael A. Postow, RuthAnn Gordan, Neil H. Segal, Naiyer A. Rizvi, Alexander Lesokhin, Michael B. Atkins, John M. Kirkwood, Matthew M. Burke, Amanda Ralabate, Angel Rivera, Stephanie A. Kronenberg, Blessing Agunwamba, Mary Ruisi, Christine Horak, Joel Jiang, Jedd Wolchok Combination therapies O5 Efficacy and correlative biomarker analysis of the coBRIM study comparing cobimetinib (COBI) + vemurafenib (VEM) vs placebo (PBO) + VEM in advanced BRAF-mutated melanoma patients (pts) Paolo A. Ascierto, Grant A. McArthur, James Larkin, Gabriella Liszkay, Michele Maio, Mario Mandalà, Lev Demidov, Daniil Stoyakovskiy, Luc Thomas, Luis de la Cruz-Merino, Victoria Atkinson, Caroline Dutriaux, Claus Garbe, Matthew Wongchenko, Ilsung Chang, Daniel O. Koralek, Isabelle Rooney, Yibing Yan, Antoni Ribas, Brigitte Dréno O6 Preliminary clinical safety, tolerability and activity results from a Phase Ib study of atezolizumab (anti-PDL1) combined with vemurafenib in BRAFV600-mutant metastatic melanoma Ryan Sullivan, Omid Hamid, Manish Patel, Stephen Hodi, Rodabe Amaria, Peter Boasberg, Jeffrey Wallin, Xian He, Edward Cha, Nicole Richie, Marcus Ballinger, Patrick Hwu O7 Preliminary safety and efficacy data from a phase 1/2 study of epacadostat (INCB024360) in combination with pembrolizumab in patients with advanced/metastatic melanoma Thomas F. Gajewski, Omid Hamid, David C. Smith, Todd M. Bauer, Jeffrey S. Wasser, Jason J. Luke, Ani S. Balmanoukian, David R. Kaufman, Yufan Zhao, Janet Maleski, Lance Leopold, Tara C. Gangadhar O8 Primary analysis of MASTERKEY-265 phase 1b study of talimogene laherparepvec (T-VEC) and pembrolizumab (pembro) for unresectable stage IIIB-IV melanoma Reinhard Dummer, Georgina V. Long, Antoni Ribas, Igor Puzanov, Olivier Michielin, Ari VanderWalde, Robert H.I. Andtbacka, Jonathan Cebon, Eugenio Fernandez, Josep Malvehy, Anthony J. Olszanski, Thomas F. Gajewski, John M. Kirkwood, Christine Gause, Lisa Chen, David R. Kaufman, Jeffrey Chou, F. Stephen Hodi News in immunotherapy O9 Two-year survival and safety update in patients (pts) with treatment-naïve advanced melanoma (MEL) receiving nivolumab (NIVO) or dacarbazine (DTIC) in CheckMate 066 Victoria Atkinson, Paolo A. Ascierto, Georgina V. Long, Benjamin Brady, Caroline Dutriaux, Michele Maio, Laurent Mortier, Jessica C. Hassel, Piotr Rutkowski, Catriona McNeil, Ewa Kalinka-Warzocha, Celeste Lebbé, Lars Ny, Matias Chacon, Paola Queirolo, Carmen Loquai, Parneet Cheema, Alfonso Berrocal, Karmele Mujika Eizmendi, Luis De La Cruz-Merino, Gil Bar-Sela, Christine Horak, Joel Jiang, Helene Hardy, Caroline Robert O10 Efficacy and safety of nivolumab (NIVO) in patients (pts) with advanced melanoma (MEL) who were treated beyond progression in CheckMate 066/067 Georgina V. Long, Jeffrey S. Weber, James Larkin, Victoria Atkinson, Jean-Jacques Grob, Reinhard Dummer, Caroline Robert, Ivan Marquez-Rodas, Catriona McNeil, Henrik Schmidt, Karen Briscoe, Jean-François Baurain, F. Stephen Hodi, Jedd D. Wolchok Tumor microenvironment and biomarkers O11 New biomarkers for response/resistance to BRAF inhibitor therapy in metastatic melanoma Rosamaria Pinto, Simona De Summa, Vito Michele Garrisi, Sabino Strippoli, Amalia Azzariti, Gabriella Guida, Michele Guida, Stefania Tommasi O12 Chemokine receptor patterns in lymphocytes mirror metastatic spreading in melanoma and response to ipilimumab Nicolas Jacquelot, David Enot, Caroline Flament, Jonathan M. Pitt, Nadège Vimond, Carolin Blattner, Takahiro Yamazaki, Maria-Paula Roberti, Marie Vetizou, Romain Daillere, Vichnou Poirier-Colame, Michaëla Semeraro, Anne Caignard, Craig L Slingluff Jr, Federica Sallusto, Sylvie Rusakiewicz, Benjamin Weide, Aurélien Marabelle, Holbrook Kohrt, Stéphane Dalle, Andréa Cavalcanti, Guido Kroemer, Anna Maria Di Giacomo, Michaele Maio, Phillip Wong, Jianda Yuan, Jedd Wolchok, Viktor Umansky, Alexander Eggermont, Laurence Zitvogel O13 Serum levels of PD1- and CD28-positive exosomes before Ipilimumab correlate with therapeutic response in metastatic melanoma patients Passarelli Anna, Tucci Marco, Stucci Stefania, Mannavola Francesco, Capone Mariaelena, Madonna Gabriele, Ascierto Paolo Antonio, Silvestris Franco O14 Immunological prognostic factors in stage III melanomas María Paula Roberti, Nicolas Jacquelot, David P Enot, Sylvie Rusakiewicz, Michaela Semeraro, Sarah Jégou, Camila Flores, Lieping Chen, Byoung S. Kwon, Ana Carrizossa Anderson, Caroline Robert, Christophe Borg, Benjamin Weide, François Aubin, Stéphane Dalle, Michele Maio, Jedd D. Wolchok, Holbrook Kohrt, Maha Ayyoub, Guido Kroemer, Aurélien Marabelle, Andréa Cavalcanti, Alexander Eggermont, Laurence Zitvogel POSTER PRESENTATIONS Molecular and immuno-advances P1 Human melanoma cells resistant to B-RAF and MEK inhibition exhibit mesenchymal-like features Anna Lisa De Presbiteris, Fabiola Gilda Cordaro, Rosa Camerlingo, Federica Fratangelo, Nicola Mozzillo, Giuseppe Pirozzi, Eduardo J. Patriarca, Paolo A. Ascierto, Emilia Caputo P2 Anti-proliferative and pro-apoptotic effect of ABT888 on melanoma cell lines and its potential role in the treatment of melanoma resistant to B-RAF inhibitors Federica Fratangelo, Rosa Camerlingo, Emilia Caputo, Maria Letizia Motti, Rosaria Falcone, Roberta Miceli, Mariaelena Capone, Gabriele Madonna, Domenico Mallardo, Maria Vincenza Carriero, Giuseppe Pirozzi and Paolo Antonio Ascierto P3 Involvement of the L-cysteine/CSE/H2S pathway in human melanoma progression Elisabetta Panza, Paola De Cicco, Chiara Armogida, Giuseppe Ercolano, Rosa Camerlingo, Giuseppe Pirozzi, Giosuè Scognamiglio, Gerardo Botti, Giuseppe Cirino, Angela Ianaro P4 Cancer stem cell antigen revealing pattern of antibody variable region genes were defined by immunoglobulin repertoire analysis in patients with malignant melanoma Beatrix Kotlan, Gabriella Liszkay, Miri Blank, Timea Balatoni, Judit Olasz, Emil Farkas, Andras Szollar, Akos Savolt, Maria Godeny, Orsolya Csuka, Szabolcs Horvath, Klara Eles, Yehuda Shoenfeld and Miklos Kasler P5 Upregulation of Neuregulin-1 expression is a hallmark of adaptive response to BRAF/MEK inhibitors in melanoma Debora Malpicci, Luigi Fattore, Susan Costantini, Francesca Capone, Paolo Antonio Ascierto, Rita Mancini, Gennaro Ciliberto P6 HuR positively regulates migration of HTB63 melanoma cells Farnaz Moradi, Pontus Berglund, Karin Leandersson, Rickard Linnskog, Tommy Andersson, Chandra Prakash Prasad P7 Prolyl 4- (C-P4H) hydroxylases have opposing effects in malignant melanoma: implication in prognosis and therapy Cristiana Lo Nigro, Laura Lattanzio, Hexiao Wang, Charlotte Proby, Nelofer Syed, Marcella Occelli, Carolina Cauchi, Marco Merlano, Catherine Harwood, Alastair Thompson, Tim Crook P8 Urokinase receptor antagonists: novel agents for the treatment of melanoma Maria Letizia Motti, Katia Bifulco, Vincenzo Ingangi, Michele Minopoli, Concetta Ragone, Federica Fratangelo, Antonello Pessi, Gennaro Ciliberto, Paolo Antonio Ascierto, Maria Vincenza Carriero P9 Exosomes released by melanoma cell lines enhance chemotaxis of primary tumor cells Francesco Mannavola, Stella D’Oronzo, Claudia Felici, Marco Tucci, Antonio Doronzo, Franco Silvestris P10 New insights in mitochondrial metabolic reprogramming in melanoma Anna Ferretta, Gabriella Guida, Stefania Guida, Imma Maida, Tiziana Cocco, Sabino Strippoli, Stefania Tommasi, Amalia Azzariti, Michele Guida P11 Lenalidomide restrains the proliferation in melanoma cells through a negative regulation of their cell cycle Stella D’Oronzo, Anna Passarelli, Claudia Felici, Marco Tucci, Davide Quaresmini, Franco Silvestris Combination therapies P12 Chemoimmunotherapy elicits polyfunctional anti-tumor CD8 + T cells depending on the activation of an AKT pathway sustained by ICOS Ornella Franzese, Belinda Palermo, Cosmo Di Donna, Isabella Sperduti, MariaLaura Foddai, Helena Stabile, Angela Gismondi, Angela Santoni, Paola Nisticò P13 Favourable toxicity profile of combined BRAF and MEK inhibitors in metastatic melanoma patients Andrea P. Sponghini, Francesca Platini, Elena Marra, David Rondonotti, Oscar Alabiso, Maria T. Fierro, Paola Savoia, Florian Stratica, Pietro Quaglino P14 Electrothermal bipolar vessel sealing system dissection reduces seroma output or time to drain removal following axillary and ilio-inguinal node dissection in melanoma patients: a pilot study Di Monta Gianluca, Caracò Corrado, Di Marzo Massimiliano, Marone Ugo, Di Cecilia Maria Luisa, Mozzillo Nicola News in immunotherapy P15 Clinical and immunological response to ipilimumab in a metastatic melanoma patient with HIV infection Francesco Sabbatino, Celeste Fusciello1, Antonio Marra, Rosario Guarrasi, Carlo Baldi, Rosa Russo, Di Giulio Giovanni, Vincenzo Faiola, Pio Zeppa, Stefano Pepe P16 Immunotherapy and hypophysitis: a case report Elisabetta Gambale, Consiglia Carella, Alessandra Di Paolo, Michele De Tursi Tumor microenvironment and biomarkers P17 New immuno- histochemical markers for the differential diagnosis of atypical melanocytic lesions with uncertain malignant potential Laura Marra, Giosuè Scognamiglio, Monica Cantile, Margherita Cerrone, Fara De Murtas, Valeria Sorrentino, Anna Maria Anniciello, Gerardo Botti P18 Utility of simultaneous measurement of three serum tumor markers in melanoma patients Angela Sandru, Silviu Voinea, Eugenia Panaitescu, Madalina Bolovan, Adina Stanciu, Sabin Cinca P19 The significance of various cut-off levels of melanoma inhibitory activity in evaluation of cutaneous melanoma patients Angela Sandru, Silviu Voinea, Eugenia Panaitescu, Madalina Bolovan, Adina Stanciu, Sabin Cinca P20 The long noncoding RNA HOTAIR is associated to metastatic progression of melanoma and it can be identified in the blood of patients with advanced disease Chiara Botti, Giosuè Scognamiglio, Laura Marra, Gabriella Aquino, Rosaria Falcone, Annamaria Anniciello, Paolo Antonio Ascierto, Gerardo Botti, Monica Cantile Other P21 The effect of Sentinel Lymph Node Biopsy in melanoma mortality: timing of dissection Cristina Fortes, Simona Mastroeni, Alessio Caggiati, Francesca Passarelli, Alba Zappalà, Maria Capuano, Riccardo Bono, Maurizio Nudo, Claudia Marino, Paola Michelozzi P22 Epidemiological survey on related psychopathology in melanoma Valeria De Biasio, Vincenzo C. Battarra IMMUNOTHERAPY BRIDGE KEYNOTE SPEAKER PRESENTATIONS Immunotherapy beyond melanoma K19 Predictor of response to radiation and immunotherapy Silvia Formenti K20 Response and resistance to PD-1 pathway blockade: clues from the tumor microenvironment Maria Libera Ascierto, Tracee L. McMiller, Alan E. Berger, Ludmila Danilova, Robert A. Anders, George J. Netto, Haiying Xu, Theresa S. Pritchard, Jinshui Fan, Chris Cheadle, Leslie Cope, Charles G. Drake, Drew M. Pardoll, Janis M. Taube and Suzanne L. Topalian K21 Combination immunotherapy with autologous stem cell transplantation, protein immunization, and PBMC reinfusion in myeloma patients Sacha Gnjatic, Sarah Nataraj, Naoko Imai, Adeeb Rahman, Achim A. Jungbluth, Linda Pan, Ralph Venhaus, Andrew Park, Frédéric F. Lehmann, Nikoletta Lendvai, Adam D. Cohen, and Hearn J. Cho K22 Anti-cancer immunity despite T cell “exhaustion” Speiser Daniel Immunotherapy in oncology (I-O): data from clinical trial K23 The Checkpoint Inhibitors for the Treatment of Metastatic Non-small Cell Lung Cancer (NSCLC) Vera Hirsh
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22. Retro-inverso Urokinase Receptor Antagonists for the Treatment of Metastatic Sarcomas
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Carriero, Maria Vincenza, primary, Bifulco, Katia, additional, Ingangi, Vincenzo, additional, Costantini, Susan, additional, Botti, Giovanni, additional, Ragone, Concetta, additional, Minopoli, Michele, additional, Motti, Maria Letizia, additional, Rea, Domenica, additional, Scognamiglio, Giosuè, additional, Botti, Gerardo, additional, Arra, Claudio, additional, Ciliberto, Gennaro, additional, and Pessi, Antonello, additional
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- 2017
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23. Treatment with a Urokinase Receptor-derived Cyclized Peptide Improves Experimental Colitis by Preventing Monocyte Recruitment and Macrophage Polarization
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Genua, Marco, primary, Ingangi, Vincenzo, additional, Fonteyne, Philippe, additional, Piontini, Andrea, additional, Yousif, Ali M., additional, Merlino, Francesco, additional, Grieco, Paolo, additional, Malesci, Alberto, additional, Carriero, Maria V., additional, and Danese, Silvio, additional
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- 2016
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24. A Macroscopic Mathematical Model for Cell Migration Assays Using a Real-Time Cell Analysis
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Di Costanzo, Ezio, primary, Ingangi, Vincenzo, additional, Angelini, Claudia, additional, Carfora, Maria Francesca, additional, Carriero, Maria Vincenza, additional, and Natalini, Roberto, additional
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- 2016
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25. The urokinase receptor-derived cyclic peptide [SRSRY] suppresses neovascularization and intravasation of osteosarcoma and chondrosarcoma cells
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Ingangi, Vincenzo, primary, Bifulco, Katia, additional, Yousif, Ali Munaim, additional, Ragone, Concetta, additional, Motti, Maria Letizia, additional, Rea, Domenica, additional, Minopoli, Michele, additional, Botti, Giovanni, additional, Scognamiglio, Giuseppe, additional, Fazioli, Flavio, additional, Gallo, Michele, additional, De Chiara, Annarosaria, additional, Arra, Claudio, additional, Grieco, Paolo, additional, and Carriero, Maria Vincenza, additional
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- 2016
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26. Cyclization of the Urokinase Receptor-Derived Ser-Arg-Ser-Arg-Tyr Peptide Generates a Potent Inhibitor of Trans-Endothelial Migration of Monocytes
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Yousif, Ali Munaim, primary, Minopoli, Michele, additional, Bifulco, Katia, additional, Ingangi, Vincenzo, additional, Di Carluccio, Gioconda, additional, Merlino, Francesco, additional, Motti, Maria Letizia, additional, Grieco, Paolo, additional, and Carriero, Maria Vincenza, additional
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- 2015
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27. Urokinase receptor promotes ovarian cancer cell dissemination through its 84-95 sequence
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Bifulco, Katia, primary, Votta, Giuseppina, additional, Ingangi, Vincenzo, additional, Carluccio, Gioconda Di, additional, Rea, Domenica, additional, Losito, Simona, additional, Montuori, Nunzia, additional, Ragno, Pia, additional, Stoppelli, Maria Patrizia, additional, Arra, Claudio, additional, and Carriero, Maria Vincenza, additional
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- 2014
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28. Urokinase receptor derived peptides as potent inhibitors of the formyl peptide receptor type 1-triggered cell migration.
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Merlino, Francesco, Brancaccio, Diego, Bellavita, Rosa, Novellino, Ettore, Carotenuto, Alfonso, Yousif, Ali Munaim, Grieco, Paolo, Carriero, Maria Vincenza, Ingangi, Vincenzo, and Minopoli, Michele
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FORMYL peptide receptors , *ENZYME inhibitors , *CELL migration , *UROKINASE , *PLASMINOGEN activators , *MONOCYTES , *STRUCTURE-activity relationships , *MOLECULAR docking - Abstract
The receptor for the urokinase-type plasminogen activator (uPAR) is a widely recognized master regulator of cell migration. We and others have previously documented that the uPAR(84–95) sequence, interacts with the formyl peptide receptors (FPR)s, henceforth inducing cell migration of several cell lines, including leukocytes, and the synthetic shorter peptide (Ser 88 -Arg-Ser-Arg-Tyr 92 , SRSRY) retains chemotactic activity in vitro and in vivo . Recently, we have developed the head-to-tail cyclic analog [SRSRY], a new potent and stable inhibitor of monocyte trafficking. This prompted us to develop novel cyclic and linear analogs of [SRSRY] with the aim to broaden the knowledge about structure-activity relationships of peptide [SRSRY]. Herein we report their synthesis, effects on cell migration, conformational and docking analyses which served to envisage a new pharmacophore model for inhibitors of FPR1-triggered cell migration. [ABSTRACT FROM AUTHOR]
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- 2018
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29. Treatment with a Urokinase Receptor-derived Cyclized Peptide Improves Experimental Colitis by Preventing Monocyte Recruitment and Macrophage Polarization
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Maria Vincenza Carriero, Ali Munaim Yousif, Silvio Danese, Philippe Fonteyne, Marco Genua, Alberto Malesci, Francesco Merlino, Vincenzo Ingangi, Andrea Piontini, Paolo Grieco, Genua, Marco, Ingangi, Vincenzo, Fonteyne, Philippe, Piontini, Andrea, Yousif, ALI MUNAIM, Merlino, Francesco, Grieco, Paolo, Malesci, Alberto, Carriero, Maria V, Danese, Silvio, Genua, M, Ingangi, V, Fonteyne, P, Piontini, A, Yousif, Am, Merlino, F, Grieco, P, Malesci, A, Carriero, Mv, and Danese, S
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0301 basic medicine ,Leukocyte migration ,experimental colitis ,Macrophage polarization ,Enzyme-Linked Immunosorbent Assay ,Severity of Illness Index ,inflammatory bowel diseases ,Monocytes ,Mice ,03 medical and health sciences ,Cell Movement ,Weight Loss ,urokinase receptor ,medicine ,Animals ,Immunology and Allergy ,Interleukin 6 ,biology ,Chemistry ,Macrophages ,Monocyte ,Dextran Sulfate ,Gastroenterology ,Cell Polarity ,Colitis ,macrophages ,Urokinase receptor ,Interleukin 10 ,030104 developmental biology ,medicine.anatomical_structure ,Immunology ,peptides ,Cancer research ,biology.protein ,Cytokines ,Tumor necrosis factor alpha ,monocytes ,Oligopeptides ,Plasminogen activator - Abstract
Background:Leukocyte migration across the blood barrier and into tissues represents a key process in the pathogenesis of inflammatory bowel diseases. The urokinase receptor (urokinase-type plasminogen activator receptor) is a master regulator of leukocyte recruitment. We recently found that cyclization of the urokinase-type plasminogen activator receptor-derived peptide Ser-Arg-Ser-Arg-Tyr [SRSRY] inhibits transendothelial migration of monocytes. Now, we have explored the effects of [SRSRY] administration during experimental colitis.Methods:The effects of [SRSRY] on cytokine profile, cytoskeletal organization, and cell migration were investigated using phorbol-12-myristate acetate-differentiated THP-1 cells exposed to polarizing stimuli. In vivo, [SRSRY] was intraperitoneally administered during dextran sodium sulfate- or 2,4,6-trinitrobenzene sulfonic acid-induced colitis in wild-type or urokinase-type plasminogen activator receptor knockout mice. Levels of pro-inflammatory cytokines and inflammatory monocytes in mucosal infiltrates were assessed by enzyme-linked immunosorbent assay and flow cytometry, respectively.Results:[SRSRY] prevents M0 to M1 transition and migration of M1 polarized macrophages. In vivo, [SRSRY] reduces intestinal inflammation diminishing body weight loss and disease activity index. These beneficial effects are accompanied by a reduction of interleukin 1, interleukin 6, and tumor necrosis factor , an increase of interleukin 10, and an abridged recruitment of inflammatory monocytes to the inflamed tissue.Conclusions:Altogether, these findings indicate that [SRSRY] may be considered as a new drug useful for the pharmacological treatment of chronic inflammatory diseases, such as inflammatory bowel diseases. BACKGROUND: Leukocyte migration across the blood barrier and into tissues represents a key process in the pathogenesis of inflammatory bowel diseases. The urokinase receptor (urokinase-type plasminogen activator receptor) is a master regulator of leukocyte recruitment. We recently found that cyclization of the urokinase-type plasminogen activator receptor-derived peptide Ser-Arg-Ser-Arg-Tyr [SRSRY] inhibits transendothelial migration of monocytes. Now, we have explored the effects of [SRSRY] administration during experimental colitis.METHODS: The effects of [SRSRY] on cytokine profile, cytoskeletal organization, and cell migration were investigated using phorbol-12-myristate acetate-differentiated THP-1 cells exposed to polarizing stimuli. In vivo, [SRSRY] was intraperitoneally administered during dextran sodium sulfate- or 2,4,6-trinitrobenzene sulfonic acid-induced colitis in wild-type or urokinase-type plasminogen activator receptor knockout mice. Levels of pro-inflammatory cytokines and inflammatory monocytes in mucosal infiltrates were assessed by enzyme-linked immunosorbent assay and flow cytometry, respectively.RESULTS: [SRSRY] prevents M0 to M1 transition and migration of M1 polarized macrophages. In vivo, [SRSRY] reduces intestinal inflammation diminishing body weight loss and disease activity index. These beneficial effects are accompanied by a reduction of interleukin 1β, interleukin 6, and tumor necrosis factor α, an increase of interleukin 10, and an abridged recruitment of inflammatory monocytes to the inflamed tissue.CONCLUSIONS: Altogether, these findings indicate that [SRSRY] may be considered as a new drug useful for the pharmacological treatment of chronic inflammatory diseases, such as inflammatory bowel diseases.
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- 2016
30. Urokinase receptor derived peptides as potent inhibitors of the formyl peptide receptor type 1-triggered cell migration
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Ali Munaim Yousif, Michele Minopoli, Ettore Novellino, Francesco Merlino, Alfonso Carotenuto, Diego Brancaccio, Paolo Grieco, Rosa Bellavita, Vincenzo Ingangi, Maria Vincenza Carriero, Yousif, Ali Munaim, Ingangi, Vincenzo, Merlino, Francesco, Brancaccio, Diego, Minopoli, Michele, Bellavita, Rosa, Novellino, Ettore, Carriero, Maria Vincenza, Carotenuto, Alfonso, and Grieco, Paolo
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0301 basic medicine ,Peptide ,Receptors, Urokinase Plasminogen Activator ,03 medical and health sciences ,Structure-Activity Relationship ,0302 clinical medicine ,Formyl peptide receptor ,Cell Movement ,Cell Line, Tumor ,Drug Discovery ,medicine ,Animals ,Humans ,Receptor ,Peptide conformational analysi ,chemistry.chemical_classification ,Pharmacology ,Dose-Response Relationship, Drug ,Molecular Structure ,Chemistry ,Animal ,Monocyte ,Peptide structure-activity relationship ,Drug Discovery3003 Pharmaceutical Science ,Organic Chemistry ,Chemotaxis ,Cell migration ,General Medicine ,Receptors, Formyl Peptide ,Rats ,Cell biology ,Urokinase receptor ,030104 developmental biology ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Rat ,Peptide inhibitors of cell migration ,Urokinase-type plasminogen activator receptor ,Pharmacophore ,Peptides ,Human - Abstract
The receptor for the urokinase-type plasminogen activator (uPAR) is a widely recognized master regulator of cell migration. We and others have previously documented that the uPAR(84–95) sequence, interacts with the formyl peptide receptors (FPR)s, henceforth inducing cell migration of several cell lines, including leukocytes, and the synthetic shorter peptide (Ser88-Arg-Ser-Arg-Tyr92, SRSRY) retains chemotactic activity in vitro and in vivo. Recently, we have developed the head-to-tail cyclic analog [SRSRY], a new potent and stable inhibitor of monocyte trafficking. This prompted us to develop novel cyclic and linear analogs of [SRSRY] with the aim to broaden the knowledge about structure-activity relationships of peptide [SRSRY]. Herein we report their synthesis, effects on cell migration, conformational and docking analyses which served to envisage a new pharmacophore model for inhibitors of FPR1-triggered cell migration.
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- 2018
31. The urokinase receptor-derived cyclic peptide [SRSRY] suppresses neovascularization and intravasation of osteosarcoma and chondrosarcoma cells
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Ali Munaim Yousif, G. Botti, Annarosaria De Chiara, Giuseppe Scognamiglio, Katia Bifulco, Paolo Grieco, Domenica Rea, Michele Minopoli, Maria Letizia Motti, Michele Gallo, Claudio Arra, Maria Vincenza Carriero, Concetta Ragone, Vincenzo Ingangi, Flavio Fazioli, Ingangi, Vincenzo, Bifulco, Katia, Yousif, ALI MUNAIM, Ragone, Concetta, Motti, MARIA LETIZIA, Rea, Domenica, Minopoli, Michele, Botti, Giovanni, Scognamiglio, Giuseppe, Fazioli, Flavio, Gallo, Michele, De Chiara, Annarosaria, Arra, Claudio, Grieco, Paolo, and Carriero, Maria Vincenza
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0301 basic medicine ,musculoskeletal diseases ,formyl peptide receptor type 1 ,Angiogenesis ,Mice, Nude ,Bone Neoplasms ,Peptides, Cyclic ,Receptors, Urokinase Plasminogen Activator ,03 medical and health sciences ,Mice ,0302 clinical medicine ,Cell Movement ,Cell Line, Tumor ,osteosarcoma ,urokinase receptor ,Medicine ,Animals ,Humans ,Neoplasm Invasiveness ,Receptor ,chondrosarcoma ,Formyl peptide receptor ,Neovascularization, Pathologic ,business.industry ,Intravasation ,Cell migration ,medicine.disease ,Receptors, Formyl Peptide ,peptide ,Urokinase receptor ,030104 developmental biology ,Oncology ,030220 oncology & carcinogenesis ,Immunology ,Cancer research ,peptides ,Osteosarcoma ,Female ,Chondrosarcoma ,business ,Research Paper - Abstract
// Vincenzo Ingangi 1, 2 , Katia Bifulco 1 , Ali Munaim Yousif 3 , Concetta Ragone 1, 2 , Maria Letizia Motti 4 , Domenica Rea 5 , Michele Minopoli 1 , Giovanni Botti 1 , Giuseppe Scognamiglio 6 , Flavio Fazioli 7 , Michele Gallo 7 , Annarosaria De Chiara 6 , Claudio Arra 5 , Paolo Grieco 3 , Maria Vincenza Carriero 1 1 Neoplastic Progression Unit, Department of Experimental Oncology, IRCCS Istituto Nazionale Tumori “Fondazione G. Pascale”, Naples, Italy 2 SUN Second University of Naples, Naples, Italy 3 Department of Pharmacy, University Federico II, Naples, Italy 4 University ‘Parthenope’, Naples, Italy 5 Animal Facility, IRCCS Istituto Nazionale Tumori “Fondazione G. Pascale”, Naples, Italy 6 Pathology Unit, IRCCS Istituto Nazionale Tumori “Fondazione G. Pascale”, Naples, Italy 7 Surgery Unit, IRCCS Istituto Nazionale Tumori “Fondazione G. Pascale”, Naples, Italy Correspondence to: Maria Vincenza Carriero, email: mariolinacarriero@yahoo.it , m.carriero@istitutotumori.na.it Keywords: urokinase receptor, formyl peptide receptor type 1, osteosarcoma, chondrosarcoma, peptides Received: April 18, 2016 Accepted: May 20, 2016 Published: June 13, 2016 ABSTRACT The receptor for the urokinase-type plasminogen activator (uPAR) is a widely recognized master regulator of cell migration and uPAR 88–92 is the minimal sequence required to induce cell motility and angiogenesis by interacting with the formyl peptide receptor type 1 (FPR1). In this study, we present evidence that the cyclization of the uPAR 88–92 sequence generates a new potent inhibitor of migration, and extracellular matrix invasion of human osteosarcoma and chondrosarcoma cells expressing comparable levels of FPR1 on cell surface. In vitro , the cyclized peptide [SRSRY] prevents formation of capillary-like tubes by endothelial cells co-cultured with chondrosarcoma cells and trans-endothelial migration of osteosarcoma and chondrosarcoma cells. When chondrosarcoma cells were subcutaneously injected in nude mice, tumor size, intra-tumoral microvessel density and circulating tumor cells in blood samples collected before the sacrifice, were significantly reduced in animals treated daily with i.p-administration of 6 mg/Kg [SRSRY] as compared to animals treated with vehicle only. Our findings indicate that [SRSRY] prevents three key events occurring during the metastatic process of osteosarcoma and chondrosarcoma cells: the extracellular matrix invasion, the formation of a capillary network and the entry into bloodstream.
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- 2016
32. Cyclization of the Urokinase Receptor-Derived Ser-Arg-Ser-Arg-Tyr Peptide Generates a Potent Inhibitor of Trans-Endothelial Migration of Monocytes
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Gioconda Di Carluccio, Katia Bifulco, Michele Minopoli, Francesco Merlino, Paolo Grieco, Ali Munaim Yousif, Vincenzo Ingangi, Maria Letizia Motti, Maria Vincenza Carriero, Yousif, ALI MUNAIM, Minopoli, Michele, Bifulco, Katia, Ingangi, Vincenzo, Di Carluccio, Gioconda, Merlino, Francesco, Motti, MARIA LETIZIA, Grieco, Paolo, and Carriero, Maria Vincenza
- Subjects
Macrophage ,media_common.quotation_subject ,lcsh:Medicine ,Biology ,Monocyte ,Monocytes ,Cell Line ,Receptors, Urokinase Plasminogen Activator ,Cell Line, Tumor ,medicine ,Animals ,Amino Acid Sequence ,lcsh:Science ,Receptor ,Internalization ,Peptide sequence ,Chromatography, High Pressure Liquid ,media_common ,Biochemistry, Genetics and Molecular Biology (all) ,Multidisciplinary ,Formyl peptide receptor ,Animal ,Medicine (all) ,Macrophages ,lcsh:R ,Transendothelial and Transepithelial Migration ,Chemotaxis ,Cell migration ,Molecular biology ,Rats ,Urokinase receptor ,medicine.anatomical_structure ,Agricultural and Biological Sciences (all) ,Cyclization ,Peptide ,Rat ,lcsh:Q ,Peptides ,Protein Binding ,Research Article - Abstract
The receptor for the urokinase-type plasminogen activator (uPAR) is a widely recognized master regulator of cell migration and uPAR88-92 is the minimal sequence required to induce cell motility. We and others have previously documented that the uPAR88-92 sequence, even in the form of synthetic linear peptide (SRSRY), interacts with the formyl peptide receptor type 1 (FPR1), henceforth inducing cell migration of several cell lines, including monocytes. FPR1 is mainly expressed by mammalian phagocytic leukocytes and plays a crucial role in chemotaxis. In this study, we present evidence that the cyclization of the SRSRY sequence generates a new potent and stable inhibitor of monocyte trafficking. In rat basophilic leukaemia RBL-2H3/ETFR cells expressing high levels of constitutively activated FPR1, the cyclic SRSRY peptide ([SRSRY]) blocks FPR1 mediated cell migration by interfering with both internalization and ligand-uptake of FPR1. Similarly to RBL-2H3/ETFR cells, [SRSRY] competes with fMLF for binding to FPR1 and prevents agonist-induced FPR1 internalization in human monocyte THP-1 cells. Unlike scramble [RSSYR], [SRSRY] inhibits fMLF-directed migration of monocytes in a dose-dependent manner, with IC50 value of 0.01 nM. PMA-differentiated THP-1 cell exposure to fMLF gradient causes a marked cytoskeletal re-organization with the formation of F-actin rich pseudopodia that are prevented by the addition of [SRSRY]. Furthermore, [SRSRY] prevents migration of human primary monocytes and trans-endothelial migration of monocytes. Our findings indicate that [SRSRY] is a new FPR1 inhibitor which may suggest the development of new drugs for treating pathological conditions sustained by increased motility of monocytes, such as chronic inflammatory diseases.
- Published
- 2015
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