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2. Mission Design of DESTINY+: Toward Active Asteroid (3200) Phaethon and Multiple Small Bodies

Author

Ozaki, Naoya, Yamamoto, Takayuki, Gonzalez-Franquesa, Ferran, Gutierrez-Ramon, Roger, Pushparaj, Nishanth, Chikazawa, Takuya, Tos, Diogene Alessandro Dei, Çelik, Onur, Marmo, Nicola, Kawakatsu, Yasuhiro, Arai, Tomoko, Nishiyama, Kazutaka, and Takashima, Takeshi

Subjects
Astrophysics - Earth and Planetary Astrophysics, Astrophysics - Instrumentation and Methods for Astrophysics, Computer Science - Computational Engineering, Finance, and Science
Abstract

DESTINY+ is an upcoming JAXA Epsilon medium-class mission to fly by the Geminids meteor shower parent body (3200) Phaethon. It will be the world's first spacecraft to escape from a near-geostationary transfer orbit into deep space using a low-thrust propulsion system. In doing so, DESTINY+ will demonstrate a number of technologies that include a highly efficient ion engine system, lightweight solar array panels, and advanced asteroid flyby observation instruments. These demonstrations will pave the way for JAXA's envisioned low-cost, high-frequency space exploration plans. Following the Phaethon flyby observation, DESTINY+ will visit additional asteroids as its extended mission. The mission design is divided into three phases: a spiral-shaped apogee-raising phase, a multi-lunar-flyby phase to escape Earth, and an interplanetary and asteroids flyby phase. The main challenges include the optimization of the many-revolution low-thrust spiral phase under operational constraints; the design of a multi-lunar-flyby sequence in a multi-body environment; and the design of multiple asteroid flybys connected via Earth gravity assists. This paper shows a novel, practical approach to tackle these complex problems, and presents feasible solutions found within the mass budget and mission constraints. Among them, the baseline solution is shown and discussed in depth; DESTINY+ will spend two years raising its apogee with ion engines, followed by four lunar gravity assists, and a flyby of asteroids (3200) Phaethon and (155140) 2005 UD. Finally, the flight operations plan for the spiral phase and the asteroid flyby phase are presented in detail.

Published
2022
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3. Systemic treatment in advanced phyllodes tumor of the breast: a multi-institutional European retrospective case-series analyses

Author

Palassini, E., Mir, O., Grignani, G., Vincenzi, B., Gelderblom, H., Sebio, A., Valverde, C., Baldi, G. G., Brunello, A., Cardellino, G. G., Marrari, A., Badalamenti, G., Martin-Broto, J., Ferraresi, V., Libertini, M., Turano, S., Gataa, I., Collini, P., Tos, A. P. Dei, Gennaro, M., Bini, F., Provenzano, S., Vullo, S. Lo, Mariani, L., Le Cesne, A., and Casali, P. G.

Published
2022
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4. Pharmacological modulation of Kv1.3 potassium channel selectively triggers pathological B lymphocyte apoptosis in vivo in a genetic CLL model

Author

Severin, Filippo, Urbani, Andrea, Varanita, Tatiana, Bachmann, Magdalena, Azzolini, Michele, Martini, Veronica, Pizzi, Marco, Tos, Angelo Paolo Dei, Frezzato, Federica, Mattarei, Andrea, Ghia, Paolo, Bertilaccio, Maria Teresa Sabrina, Gulbins, Erich, Paradisi, Cristina, Zoratti, Mario, Semenzato, Gianpietro Carlo, Leanza, Luigi, Trentin, Livio, and Szabò, Ildiko

Published
2022
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5. Per- and polyfluoroalkyl substances (PFAS) exposure in melanoma patients: a retrospective study on prognosis and histological features

Author

Del Fiore, Paolo, Cavallin, Francesco, Mazza, Marcodomenico, Benna, Clara, Monico, Alessandro Dal, Tadiotto, Giulia, Russo, Irene, Ferrazzi, Beatrice, Tropea, Saveria, Buja, Alessandra, Cozzolino, Claudia, Cappellesso, Rocco, Nicolè, Lorenzo, Piccin, Luisa, Pigozzo, Jacopo, Chiarion-Sileni, Vanna, Vecchiato, Antonella, Menin, Chiara, Bassetto, Franco, Tos, Angelo Paolo Dei, Alaibac, Mauro, and Mocellin, Simone

Published
2022
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7. International consensus statement on allergy and rhinology: Sinonasal tumors

Author

Kuan, Edward C., primary, Wang, Eric W., additional, Adappa, Nithin D., additional, Beswick, Daniel M., additional, London, Nyall R., additional, Su, Shirley Y., additional, Wang, Marilene B., additional, Abuzeid, Waleed M., additional, Alexiev, Borislav, additional, Alt, Jeremiah A., additional, Antognoni, Paolo, additional, Alonso‐Basanta, Michelle, additional, Batra, Pete S., additional, Bhayani, Mihir, additional, Bell, Diana, additional, Bernal‐Sprekelsen, Manuel, additional, Betz, Christian S., additional, Blay, Jean‐Yves, additional, Bleier, Benjamin S., additional, Bonilla‐Velez, Juliana, additional, Callejas, Claudio, additional, Carrau, Ricardo L., additional, Casiano, Roy R., additional, Castelnuovo, Paolo, additional, Chandra, Rakesh K., additional, Chatzinakis, Vasileios, additional, Chen, Simon B., additional, Chiu, Alexander G., additional, Choby, Garret, additional, Chowdhury, Naweed I., additional, Citardi, Martin J., additional, Cohen, Marc A., additional, Dagan, Roi, additional, Dalfino, Gianluca, additional, Dallan, Iacopo, additional, Dassi, Camila Soares, additional, de Almeida, John, additional, Tos, Angelo P. Dei, additional, DelGaudio, John M., additional, Ebert, Charles S., additional, El‐Sayed, Ivan H., additional, Eloy, Jean Anderson, additional, Evans, James J., additional, Fang, Christina H., additional, Farrell, Nyssa F., additional, Ferrari, Marco, additional, Fischbein, Nancy, additional, Folbe, Adam, additional, Fokkens, Wytske J., additional, Fox, Meha G., additional, Lund, Valerie J., additional, Gallia, Gary L., additional, Gardner, Paul A., additional, Geltzeiler, Mathew, additional, Georgalas, Christos, additional, Getz, Anne E., additional, Govindaraj, Satish, additional, Gray, Stacey T., additional, Grayson, Jessica W., additional, Gross, Bradley A., additional, Grube, Jordon G., additional, Guo, Ruifeng, additional, Ha, Patrick K., additional, Halderman, Ashleigh A., additional, Hanna, Ehab Y., additional, Harvey, Richard J., additional, Hernandez, Stephen C., additional, Holtzman, Adam L., additional, Hopkins, Claire, additional, Huang, Zhigang, additional, Huang, Zhenxiao, additional, Humphreys, Ian M., additional, Hwang, Peter H., additional, Iloreta, Alfred M., additional, Ishii, Masaru, additional, Ivan, Michael E., additional, Jafari, Aria, additional, Kennedy, David W., additional, Khan, Mohemmed, additional, Kimple, Adam J., additional, Kingdom, Todd T., additional, Knisely, Anna, additional, Kuo, Ying‐Ju, additional, Lal, Devyani, additional, Lamarre, Eric D., additional, Lan, Ming‐Ying, additional, Le, Hien, additional, Lechner, Matt, additional, Lee, Nancy Y., additional, Lee, Jivianne K., additional, Lee, Victor H., additional, Levine, Corinna G., additional, Lin, Jin‐Ching, additional, Lin, Derrick T., additional, Lobo, Brian C., additional, Locke, Tran, additional, Luong, Amber U., additional, Magliocca, Kelly R., additional, Markovic, Svetomir N., additional, Matnjani, Gesa, additional, McKean, Erin L., additional, Meço, Cem, additional, Mendenhall, William M., additional, Michel, Loren, additional, Na'ara, Shorook, additional, Nicolai, Piero, additional, Nuss, Daniel W., additional, Nyquist, Gurston G., additional, Oakley, Gretchen M., additional, Omura, Kazuhiro, additional, Orlandi, Richard R., additional, Otori, Nobuyoshi, additional, Papagiannopoulos, Peter, additional, Patel, Zara M., additional, Pfister, David G., additional, Phan, Jack, additional, Psaltis, Alkis J., additional, Rabinowitz, Mindy R., additional, Ramanathan, Murugappan, additional, Rimmer, Ryan, additional, Rosen, Marc R., additional, Sanusi, Olabisi, additional, Sargi, Zoukaa B., additional, Schafhausen, Philippe, additional, Schlosser, Rodney J., additional, Sedaghat, Ahmad R., additional, Senior, Brent A., additional, Shrivastava, Raj, additional, Sindwani, Raj, additional, Smith, Timothy L., additional, Smith, Kristine A., additional, Snyderman, Carl H., additional, Solares, C. Arturo, additional, Sreenath, Satyan B., additional, Stamm, Aldo, additional, Stölzel, Katharina, additional, Sumer, Baran, additional, Surda, Pavol, additional, Tajudeen, Bobby A., additional, Thompson, Lester D. R., additional, Thorp, Brian D., additional, Tong, Charles C. L., additional, Tsang, Raymond K., additional, Turner, Justin H., additional, Turri‐Zanoni, Mario, additional, Udager, Aaron M., additional, van Zele, Thibaut, additional, VanKoevering, Kyle, additional, Welch, Kevin C., additional, Wise, Sarah K., additional, Witterick, Ian J., additional, Won, Tae‐Bin, additional, Wong, Stephanie N., additional, Woodworth, Bradford A., additional, Wormald, Peter‐John, additional, Yao, William C., additional, Yeh, Chien‐Fu, additional, Zhou, Bing, additional, Palmer, James N., additional, Abiri, Arash, additional, Adams, Carrie D., additional, Ayoub, Noel F., additional, Bitner, Benjamin F., additional, Boyd, Jacob T., additional, Chang, Michael T., additional, Chapurin, Nikita, additional, Chaskes, Mark B., additional, Chua, Andy, additional, Chung, Sei Y., additional, Contrera, Kevin J., additional, Dilley, Katelyn K., additional, Dutra, André Zanette, additional, Eide, Jacob G., additional, Fenberg, Rachel, additional, Godse, Neal R., additional, Jawad, Basit, additional, Johnson, Jared, additional, Johnson, B. Jake, additional, Judd, Ryan, additional, Khalife, Sarah, additional, Khosravi, Pooya, additional, Kolarski, Mirko Manojlovic, additional, Kong, Keonho A., additional, Kshirsagar, Rijul S., additional, Lee, Joseph S., additional, Lin, Tian‐Yun, additional, McCormick, Justin P., additional, Melder, Katie, additional, Morse, Elliot, additional, Nguyen, Theodore V., additional, Norwood, Timothy G., additional, Pang, Jonathan C., additional, Parsel, Sean M., additional, Patel, Prayag S., additional, Ringel, Barak, additional, Schneider, Alexander L., additional, Spielman, Daniel B., additional, Spock, Todd, additional, and Vasudev, Milind, additional

Published
2023
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8. Publisher Correction: Reprogramming normal cells into tumour precursors requires ECM stiffness and oncogene-mediated changes of cell mechanical properties

Author

Panciera, Tito, Citron, Anna, Di Biagio, Daniele, Battilana, Giusy, Gandin, Alessandro, Giulitti, Stefano, Forcato, Mattia, Bicciato, Silvio, Panzetta, Valeria, Fusco, Sabato, Azzolin, Luca, Totaro, Antonio, Tos, Angelo Paolo Dei, Fassan, Matteo, Vindigni, Vincenzo, Bassetto, Franco, Rosato, Antonio, Brusatin, Giovanna, Cordenonsi, Michelangelo, and Piccolo, Stefano

Published
2020
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9. Gastrointestinal stromal tumours: ESMO-EURACAN-GENTURIS Clinical Practice Guidelines for diagnosis, treatment and follow-up

Author

Casali, Paolo G., Blay, Jean-Yves, Abecassis, N., Bajpai, J., Bauer, Sebastian, Biagini, R., Bielack, S., Bonvalot, Sylvie, Boukovinas, I., Bovee, J. V. M. G., Boye, K., Brodowicz, T., Buonadonna, A., Álava, Enrique de, Tos, A. P. dei, García del Muro, Xavier, Dufresne, Armelle, Eriksson, Mikael, Fedenko, Alexander, Ferraresi, Virginia, Ferrari, A., Frezza, Anna M., Gasperoni, Silvia, Gelderblom, Hans, Gouin, Francois, Grignani, Giovanni, Haas, R. L., Hassan, A. B., Hindi, Nadia, Hohenberger, Peter, Joensuu, Heikki, Jones, Robin L., Jungels, C., Jutte, P., Kasper, Bernd, Kawai, Akira, Kopeckova, K., Krákorová, D. A., Le Cesne, A, Le Grange, F, Legius, E., Leithner, Andreas, López-Pousa, Antonio, Martín-Broto, Javier, Merimsky, O., Messiou, C., Miah, A. B., Mir, Olivier, Montemurro, M., Morosi, Carlo, Palmerini, Emanuela, Pantaleo, M. A., Piana, R., Piperno-Neumann, S., Reichardt, Peter, Rutkowski, Piotr, Safwat, A. A., Sangalli, C., Sbaraglia, Marta, Scheipl, S., Schöffski, P., Sleijfer, S., Strauss, D., Strauss, S. J., Sundby-Hall, Kirsten, Trama, A., Unk, M., Sande, M. A. J. van de, Graaf, W.T.A. van der, Houdt, W. J. van, Frebourg, T., Gronchi, Alesandro, Stacchiotti, Silvia, ESMO Guidelines Committee, EURACAN, GENTURIS, Casali, Paolo G., Blay, Jean-Yves, Abecassis, N., Bajpai, J., Bauer, Sebastian, Biagini, R., Bielack, S., Bonvalot, Sylvie, Boukovinas, I., Bovee, J. V. M. G., Boye, K., Brodowicz, T., Buonadonna, A., Álava, Enrique de, Tos, A. P. dei, García del Muro, Xavier, Dufresne, Armelle, Eriksson, Mikael, Fedenko, Alexander, Ferraresi, Virginia, Ferrari, A., Frezza, Anna M., Gasperoni, Silvia, Gelderblom, Hans, Gouin, Francois, Grignani, Giovanni, Haas, R. L., Hassan, A. B., Hindi, Nadia, Hohenberger, Peter, Joensuu, Heikki, Jones, Robin L., Jungels, C., Jutte, P., Kasper, Bernd, Kawai, Akira, Kopeckova, K., Krákorová, D. A., Le Cesne, A, Le Grange, F, Legius, E., Leithner, Andreas, López-Pousa, Antonio, Martín-Broto, Javier, Merimsky, O., Messiou, C., Miah, A. B., Mir, Olivier, Montemurro, M., Morosi, Carlo, Palmerini, Emanuela, Pantaleo, M. A., Piana, R., Piperno-Neumann, S., Reichardt, Peter, Rutkowski, Piotr, Safwat, A. A., Sangalli, C., Sbaraglia, Marta, Scheipl, S., Schöffski, P., Sleijfer, S., Strauss, D., Strauss, S. J., Sundby-Hall, Kirsten, Trama, A., Unk, M., Sande, M. A. J. van de, Graaf, W.T.A. van der, Houdt, W. J. van, Frebourg, T., Gronchi, Alesandro, Stacchiotti, Silvia, ESMO Guidelines Committee, EURACAN, and GENTURIS

Abstract

Gastrointestinal stromal tumours (GISTs) are malignant mesenchymal tumours with a variable clinical behaviour, marked by differentiation towards the interstitial cells of Cajal.1 GISTs belong to the family of soft tissue sarcomas (STSs) but are treated separately due to their peculiar histogenesis, clinical behaviour and specific therapy. This European Society for Medical Oncology (ESMO)–European Reference Network for Rare Adult Solid Cancers (EURACAN)–European Reference Network for Genetic Tumour Risk Syndromes (GENTURIS) Clinical Practice Guideline (CPG) will cover GISTs while other STSs are covered in the ESMO–EURACAN–European Reference Network for Paediatric Oncology (ERN PaedCan)–GENTURIS STS CPG.

Published
2022

16. Soft tissue and visceral sarcomas: ESMO-EURACAN Clinical Practice Guidelines for diagnosis, treatment and follow-up (vol 29, pg 51, 2018)

Author

Casali, P. G., Abecassis, N., Aro, H. T., Bauer, S., Biagini, R., Bielack, S., Bonvalot, S., Boukovinas, I., Bovee, J. V. M. G., Brodovvicz, T., Broto, J. M., Buonadonna, A., De Alava, E., Tos, A. P. Dei, Del Muro, X. G., Dileo, P., Eriksson, M., Fedenko, A., Ferraresi, V., Ferrari, A., Ferrari, S., Frezza, A. M., Gasperoni, S., Gelderblom, H., Gil, T., Grignani, G., Gronchi, A., Haas, R. L., Hassan, B., Hohenberger, P., Lssels, R., Joensuu, H., Jones, R. L., Judson, I., Jutte, P., Kaal, S., Kasper, B., Kopeckova, K., Krakorova, D. A., Le Cesne, A., Lugowska, I., Merimsky, O., Montemurro, M., Pantaleo, M. A., Piana, R., Picci, P., Piperno-Neumann, S., Pousa, A. L., Sleijfer, S., van der Graaf, W. T. A., ​Basic and Translational Research and Imaging Methodology Development in Groningen (BRIDGE), Public Health Research (PHR), and Man, Biomaterials and Microbes (MBM)

Published
2018

18. Bone sarcomas: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up

Author

Hogendoorn, P. C. W., Athanasou, N., Bielack, S., De Alava, E., Tos, A. P. Dei, Ferrari, S., Gelderblom, H., Grimer, R., Hall, K. Sundby, Hassan, B., Jurgens, H., Paulussen, M., Rozeman, L., Taminiau, A.H.M., Whelan, J., Vanel, D., Hogendoorn, P. C. W., Athanasou, N., Bielack, S., De Alava, E., Tos, A. P. Dei, Ferrari, S., Gelderblom, H., Grimer, R., Hall, K. Sundby, Hassan, B., Jurgens, H., Paulussen, M., Rozeman, L., Taminiau, A.H.M., Whelan, J., and Vanel, D.

Published
2017

19. PML expression in soft tissue sarcoma: Prognostic and predictive value in alkylating agents/antracycline-based first line therapy

Author

Vincenzi, Bruno, primary, Santini, Daniele, additional, Schiavon, Gaia, additional, Frezza, Anna Maria, additional, Silletta, Marianna, additional, Crucitti, Pierfilippo, additional, Casali, Paolo, additional, Tos, Angelo P. Dei, additional, Rossi, Sabrina, additional, Rizzo, Sergio, additional, Badalamenti, Giuseppe, additional, Tomasino, Rosa Maria, additional, Russo, Antonio, additional, Butrynski, James E., additional, and Tonini, Giuseppe, additional

Published
2012
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20. Best clinical management of tenosynovial giant cell tumour (TGCT): A consensus paper from the community of experts.

Author

Silvia, Stacchiotti, Hans Roland, Dürr, Inga-Marie, Schaefer, Klaus, Woertler, Rick, Haas, Annalisa, Trama, Augusto, Caraceni, Jyoti, Bajpai, Giacomo Giulio, Baldi, Nicholas, Bernthal, Jean-Yves, Blay, Kjetil, Boye, Javier-Martin, Broto, Wei-Wu Tom, Chen, Tos Paolo Angelo, Dei, Jayesh, Desai, Stephan, Emhofer, Mikael, Eriksson, Alessandro, Gronchi, and Hans, Gelderblom

Abstract

• TGCT is a rare mesenchymal tumor, affecting joints and tendon sheaths. • Diffuse-type TGCT shows a high risk of local relapse following surgical resection. • At relapse, TGCT may cause chronic pain, and severely impact function and QoL. • A global consensus meeting was held in 2022 to define clinical management of TGCT. • Best evidence-based practice for the optimal approach to TGCT is presented herein. Tenosynovial giant cell tumour (TGCT) is a rare, locally aggressive, mesenchymal tumor arising from the joints, bursa and tendon sheaths. TGCT comprises a nodular- and a diffuse-type, with the former exhibiting mostly indolent course and the latter a locally aggressive behavior. Although usually not life-threatening, TGCT may cause chronic pain and adversely impact function and quality of life (QoL). CSFR1 inhibitors are effective with benefit on symptoms and QoL but are not available in most countries. The degree of uncertainty in selecting the most appropriate therapy and the lack of guidelines on the clinical management of TGCT make the adoption of new treatments inconsistent across the world, with suboptimal outcomes for patients. A global consensus meeting was organized in June 2022, involving experts from several disciplines and patient representatives from SPAGN to define the best evidence-based practice for the optimal approach to TGCT and generate the recommendations presented herein. [ABSTRACT FROM AUTHOR]

Published
2023
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21. Time to Definitive Failure to the First Tyrosine Kinase Inhibitor in Localized GI Stromal Tumors Treated With Imatinib As an Adjuvant: A European Organisation for Research and Treatment of Cancer Soft Tissue and Bone Sarcoma Group Intergroup...

Author

Casali, Paolo G., Le Cesne, Axel, Poveda Velasco, Andres, Kotasek, Dusan, Rutkowski, Piotr, Hohenberger, Peter, Fumagalli, Elena, Judson, Ian R., Italiano, Antoine, Gelderblom, Hans, Adenis, Antoine, Hartmann, Jörg T., Duffaud, Florence, Goldstein, David, Broto, Javier M., Gronchi, Alessandro, Tos, Angelo P. Dei, Marréaud, Sandrine, van der Graaf, Winette T. A., and Zalcberg, John R.

Published
2015
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23. Small Cell Osteosarcoma

Author

Righi, Alberto, Gambarotti, Marco, Longo, Serena, Benini, Stefania, Gamberi, Gabriella, Cocchi, Stefania, Vanel, Daniel, Picci, Piero, Bertoni, Franco, Simoni, Antonella, Franchi, Alessandro, and Tos, Angelo Paolo Dei

Abstract

Small round cell osteosarcoma is a very rare type of osteosarcoma, histologically mimicking other small round cell malignancies of bone, most notably Ewing sarcoma. To distinguish small cell osteosarcoma from other primary small cell malignancies of bone, we evaluated the immunohistochemical (IHC) expression of CD99 and SATB2, a marker of osteoblastic differentiation. Second, we analyzed EWSR1and FUSgene aberrations using fluorescence in situ hybridization andor reverse transcription–polymerase chain reaction (RT-PCR) techniques to assess whether small cell osteosarcoma and Ewing sarcoma share the same genetic alteration analysis. Thirty-six cases of primitive small cell osteosarcoma of bone were included in this study. All the cases of small cell osteosarcoma showed strong nuclear expression of SATB2 associated with negativity for CD99 antibody or weak, cytoplasmic staining in few neoplastic cells. Reverse transcription–polymerase chain reaction was negative for EWS-FLI1 type 1-2, EWS-ERG type 1, and CIC-DUX4 in the 10 available cases of small cell osteosarcoma analyzed. Fluorescence in situ hybridization analysis was feasible with a readable signal in 13 cases of small cell osteosarcoma, and none of these cases showed any EWSR1and FUSgene rearrangements. In conclusion, it appears extremely useful to combine IHC analysis of SATB2 and CD99 with molecular analysis of Ewing sarcoma–associated genetic aberrations, to differentiate small cell osteosarcoma from other small round cell malignancies of bone. The strong IHC expression of SATB2 associated with CD99 immunonegativity and the absence of EWSR1and FUSgene rearrangements in small cell osteosarcoma argues against the existence of a morphologicgenetic continuum with Ewing sarcoma.

Published
2015
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24. Myogenic Differentiation and Histologic Grading Are Major Prognostic Determinants in Retroperitoneal Liposarcoma

Author

Gronchi, Alessandro, Collini, Paola, Miceli, Rosalba, Valeri, Barbara, Renne, Salvatore L., Dagrada, Gianpaolo, Fiore, Marco, Sanfilippo, Roberta, Barisella, Marta, Colombo, Chiara, Morosi, Carlo, Stacchiotti, Silvia, Casali, Paolo G., Tos, Angelo P. Dei, and Pilotti, Silvana

Abstract

The aim of the present work was to improve the understanding of the impact of malignancy grade and myogenicrhabdomyoblastic differentiation on the natural course of retroperitoneal liposarcoma. All consecutive patients affected by primary well-differentiated (WD)dedifferentiated (DD) retroperitoneal liposarcoma, surgically treated at our institution between January 2002 and December 2011, were retrospectively evaluated. Tumors were stained for mdm2 and 5 myogenic markers (smooth muscle actin-, h-caldesmon, calponin, desmin, myogenin). The French National Federation of the Centers for the Fight Against Cancer (FNCLCC) grading system was applied. Overall survival, crude cumulative incidence of local recurrence, and distant metastases were calculated. Multivariable analyses were carried out. A total of 144 patients were identified. Median follow-up was 68 months (interquartile range: 46 to 104 mo). Fifty-two patients were affected by WDG1 and 92 by DD liposarcoma. Among the latter, 60 were grade G2 and 32 G3. Myogenic differentiation was present in 54 cases (852 WDG1, 2760 DDG2, 1832 DDG3). Seven cases had a rhabdomyoblastic DD component (160 DDG2 and 632 DDG3). Five-year overall survival rates were 93, 57, and 21 for WDG1 liposarcoma, G2 DD, and G3 DD liposarcoma, respectively, and 75, 42, and 29 for liposarcoma without myogenic differentiation, with myogenic differentiation, with rhabdomyoblastic differentiation, respectively (P<0.001). Of note, 56 patients affected by G3 DD liposarcoma with a rhabdomyoblastic component died within 8 months. FNCLCC grade and myogenic differentiation significantly predicted the outcome of retroperitoneal liposarcoma. These should be factored into treatment decision-making and possibly used to stratify patients in clinical trials.

Published
2015
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26. The Reticulin Algorithm for Adrenocortical Tumor Diagnosis

Author

Duregon, Eleonora, Fassina, Ambrogio, Volante, Marco, Nesi, Gabriella, Santi, Raffaella, Gatti, Gaia, Cappellesso, Rocco, Dalino Ciaramella, Paolo, Ventura, Laura, Gambacorta, Marcello, Tos, Angelo Paolo Dei, Loli, Paola, Mannelli, Massimo, Mantero, Franco, Berruti, Alfredo, Terzolo, Massimo, and Papotti, Mauro

Abstract

The pathologic diagnosis of adrenocortical carcinoma (ACC) still needs to be improved, because the renowned Weiss Score (WS) system has a poor reproducibility of some parameters and is difficult to apply in borderline cases and in ACC variants. The “reticulin algorithm” (RA) defines malignancy through an altered reticulin framework associated with 1 of the 3 following parameter: necrosis, high mitotic rate, and vascular invasion. This study aimed at validating the interobserver reproducibility of reticulin stain evaluation in an unpublished series of 245 adrenocortical tumors (61 adenomas and 184 carcinomas) from 5 Italian centers, classified according to the WS. Eight pathologists reviewed all reticulin-stained slides. After training, a second round of evaluation on discordant cases was performed 10 weeks later. The RA reclassified 67 cases (27) as adenomas, including 44 with no reticulin alterations and 23 with an altered reticulin framework but lacking the subsequent parameters of the triad. The other 178 cases (73) were carcinomas according to the above-mentioned criteria. A complete (88 pathologists) interobserver agreement was reached in 75 of cases (=0.702), irrespective of case derivation, pathologists’ experience, and histologic variants, and was further improved when only those cases with high WS and clinically malignant behavior were considered. After the training, the overall agreement increased to 86. We conclude that reticulin staining is a reliable technique and an easy-to-interpret system in adrenocortical tumors; moreover, it has a high interobserver reproducibility, which supports the notion of using such a method in the proposed 2-step RA approach for ACC diagnosis.

Published
2013
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27. Impact of Molecular Analysis on the Final Sarcoma Diagnosis

Author

Neuville, Agnes, Ranchère-Vince, Dominique, Tos, Angelo Paolo Dei, Cristina Montesco, Maria, Hostein, Isabelle, Toffolatti, Luisa, Chibon, Frédéric, Pissaloux, Daniel, Alberti, Laurent, Decouvelaere, Anne-Valérie, Albert, Sabrina, Riccardo Rossi, Carlo, Blay, Jean-Yves, and Coindre, Jean-Michel

Abstract

Sarcomas are rare, heterogenous, and often difficult to classify. A large proportion of sarcomas are associated with specific molecular genetic lesions such as translocations, mutations, and amplifications, which are helpful in the diagnosis of individual cases. However, the exact impact of molecular genetics on the final diagnosis of sarcomas is unknown. In this study, all soft tissue and visceral sarcomas arising in patients living in 3 European regions in 2 countries (representing 13 million inhabitants) were collected and reviewed during 2 consecutive years. A molecular analysis was performed for all suspicions of sarcomas with specific genetic lesions mutations of KITPDGFRAin gastrointestinal stromal tumors (GISTs), reciprocal translocation, or amplification of MDM2in atypical lipomatous tumors, well-differentiated liposarcoma-dedifferentiated liposarcoma (ALTWDLPS-DDLPS). To evaluate the impact of molecular tests, a premolecular analysis diagnosis was proposed with 3 categories of certainty: certain, probable, or possible. A molecular analysis was performed in 7631484 tumors corresponding to 295 cases in which GIST was suspected, 248 sarcomas with a suspicion of translocation, and 220 cases in which ALTWDLPS-DDLPS was suspected. Molecular analysis was found to be useful (confirms a probable diagnosis) in 11 (4) GISTs, 62 (26) suspicions of translocation, and 66 (31) suspicions of ALTWDLPS-DDLPS; and necessary (allows a possible diagnosis) in 2 (<1) GISTs, 31 (12) suspicions of translocation, and 19 (9) suspicions of ALTWDLPS-DDLPS. This study performed in an epidemiological setting demonstrates the significant impact of molecular analysis on the final sarcoma diagnosis and favors such an analysis on any tumor with a suspicion of a specific genomic abnormality and for which the diagnosis is uncertain.

Published
2013
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28. Myxoid liposarcoma and the mammalian target of rapamycin pathway

Author

Sanfilippo, Roberta, Tos, Angelo P. Dei, and Casali, Paolo G.

Abstract

Myxoidround cell liposarcoma (MRCL) represents about 10 of all soft-tissue sarcomas. Therapeutic options for this subgroup of tumours are limited, essentially doxorubicin-based regimens and trabectedin. Recently, the mammalian target of rapamycin (mTOR) pathway has been identified as a therapeutic target in several sarcomas. MRCLs should be included among these, as various molecular aberrations of the mTOR pathway have been recently reported.

Published
2013
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29. Dedifferentiation in Gastrointestinal Stromal Tumor to an Anaplastic KIT-negative Phenotype

Author

Antonescu, Cristina R., Romeo, Salvatore, Zhang, Lei, Nafa, Khedoudja, Hornick, Jason L., Nielsen, Gunnlaugur Petur, Mino-Kenudson, Mari, Huang, Hsuan-Ying, Mosquera, Juan-Miguel, Tos, Paolo A. Dei, and Fletcher, Christopher D.M.

Abstract

Most gastrointestinal stromal tumors (GISTs) can be recognized by their monotonous cytologic features and overexpression of KIT oncoprotein. Altered morphology and loss of CD117 reactivity has been described previously after chronic imatinib treatment; however, this phenomenon has not been reported in imatinib-naive tumors. Eight patients with abrupt transition from a classic CD117-positive spindle cell GIST to an anaplastic CD117-negative tumor were investigated for underlying molecular mechanisms of tumor progression. Pathologic and molecular analysis was performed on each of the 2 components. Genomic DNA polymerase chain reaction for KIT, PDGFRA, BRAF, and KRAShot spot mutations and fluorescence in situ hybridization for detecting KITgene copy number alterations were performed. TP53mutational analysis was performed in 5 cases. There were 7 men and 1 woman, with an age range of 23 to 65 years. Five of the primary tumors were located in the stomach, and 1 case each originated in the small bowel, colon, and rectum. In 3 patients, the dedifferentiated component occurred in the setting of imatinib resistance, whereas the remaining 5 occurred de novo. The dedifferentiated component had an anaplastic appearance, including 1 angiosarcomatous phenotype, with high mitotic activity and necrosis, and showed complete loss of CD117 (88) and CD34 (58) expression and de novo expression of either cytokeratin (48) or desmin (18). There was no difference in the KITgenotype between the 2 components. However, 2 imatinib-resistant tumors showed coexistence of KITexon 11 and exon 13 mutations. Fluorescence in situ hybridization showed loss of 1 KITgene in 3 cases and low-level amplification of KITin 2 other cases in the CD117-negative component, compared with the CD117-positive area. TP53mutation was identified in 15 cases tested, being present in both components. In summary, dedifferentiation in GIST may occur either de novo or after chronic imatinib exposure and can represent a diagnostic pitfall. This phenomenon is not related to additional KITmutations, but might be secondary to genetic instability, either represented by loss of heterozygosity or low level of KITamplification.

Published
2013
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30. Clinical application of molecular pathology in sarcomas

Author

Romeo, Salvatore and Tos, Angelo P Dei

Abstract

This review is intended to highlight the clinical application of molecular pathology as a tool for diagnostic accuracy and prognostic and predictive use and finally to discover novel molecular therapeutic targets.

Published
2011
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31. The reappraisal of gastrointestinal stromal tumors: from Stout to the KIT revolution

Author

Tos, Angelo P. Dei

Abstract

For five decades gastrointestinal stromal tumors (GISTs) truly have represented one of the most confusing as well as neglected areas of both surgical pathology and clinical oncology. The recognition of the central role played by KIT expression in the development of the interstitial cell of Cajal and of the activating KIT mutations in the pathogenesis of GIST have been the keys for a more precise categorization of this long elusive clinicopathological entity. A Consensus Conference held at the National Institutes of Health in 2001 provided both an evidence-based definition and a practical scheme for the assessment of the risk of aggressive clinical behavior. This scheme is based on evaluation of the size and mitotic rate of the tumors, and its use is strongly advocated. On the basis of current data GISTs can be defined as a distinctive group of KIT-expressing mesenchymal neoplasms of the gastrointestinal tract, showing differentiation towards the interstitial cell of Cajal, also known as the gastrointestinal pacemaker cells. Metastatic GISTs have been a virtually incurable disease until the elucidation of the role of KIT mutations. STI-571 (imatinib mesylate) is a molecule that inhibits the function of various receptors with tyrosine kinase activity, such as abl, the bcr-abl chimeric product, platelet-derived growth factor receptor, and KIT. Following its successful use in the treatment of chronic myeloid leukemia, STI-571 has also proved extremely effective in targeting metastatic GIST. Data regarding the duration of the response to this therapy are not yet available, and therefore any overenthusiasm should be avoided. Nonetheless, the GIST story remains paradigmatic of a totally innovative approach to cancer therapy which until now is the most elegant translation of cancer biology experimental knowledge into clinical practice.

Published
2003
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32. Coordinated expression and amplification of the <TOGGLE>MDM2</TOGGLE>, <TOGGLE>CDK4</TOGGLE>, and <TOGGLE>HMGI-C</TOGGLE> genes in atypical lipomatous tumours

Author

Tos, Angelo P. Dei, Doglioni, Claudio, Piccinin, Sara, Sciot, Raf, Furlanetto, Alberto, Boiocchi, Mauro, Cin, Paola Dal, Maestro, Roberta, Fletcher, Christopher D. M., and Tallini, Giovanni

Abstract

Atypical lipomatous tumours (ALTs) represent a distinctive subset of mesenchymal neoplasms featuring mature adipocytic differentiation. Most ALTs are characterized cytogenetically by the presence of supernumerary ring and/or long marker chromosomes derived from the chromosomal region 12q13–15. The 12q13–15 chromosome region contains several genes which may play an important role in human tumorigenesis. A series of ALTs was analysed by investigating the MDM2, CDK4, and HMGI-C genes and their proteins. The study was extended to a series of ordinary lipomas, to determine whether the immunohistochemical investigation of these gene products might play any diagnostic role. Cytogenetic analysis revealed the presence of various cytogenetic aberrations involving the 12q13–15 region in 11/18 (61%) lipomas and of ring chromosomes in all ALTs. Overexpression of mdm2 protein was observed in 6/12 (50%) atypical lipomatous tumours. All lipomas were mdm2-negative. cdk4 overexpression was present in 100% of ALTs. Weak cdk4 immunopositivity was detected in 2/18 (11%) ordinary lipomas in a minority of cells. HMGI-C immunopositivity was observed in 10/12 (83%) ALTs. Positive immunoreactivity was also observed in 8/18 (44%) lipomas. Southern blot analysis revealed amplification of the CDK4 and MDM2 genes in 3/5 ALTs analysed. HMGI-C was amplified in 3/5 cases and was deleted in one case. Mutation analysis of the CDK4 gene did not demonstrate any mutation. These data support the hypothesis that ordinary lipomas may form a molecular genetic and morphological continuum with ALT. At one end of the spectrum are lipomas characterized by 12q13–15 rearrangements and HMGI-C activation and at the other end are ALTs with ring chromosomes, 12q13–15 amplification with overrepresentation of the HMGI-C, CDK4 or MDM2 genes, and aberrant cdk4, mdm2, and HMGI-C protein expression. These findings not only provide insights into the molecular pathogenesis of lipomatous tumours, but also indicate that the immunohistochemical analysis of mdm2 and cdk4 may help to increase diagnostic accuracy. Copyright © 2000 John Wiley & Sons, Ltd.

Published
2000

33. A preliminary study of AQUAPORIN 1 immunolocalization in chronic subdural hematoma membranes.

Author

Basaldella, Luca, Perin, Alessandro, Orvieto, Enrico, Marton, Elisabetta, Itskevich, David, Tos, Angelo Paolo Dei, and Longatti, Pierluigi

Subjects
AQUAPORINS, SUBDURAL hematoma, CELL membranes, CRANIOTOMY, IMMUNOHISTOCHEMISTRY, DURA mater
Abstract

Abstract: Aquaporin 1 (AQP1) is a molecular water channel expressed in many anatomical locations, particularly in epithelial barriers specialized in water transport. The aim of this study was to investigate AQP1 expression in chronic subdural hematoma (CSDH) membranes. In this preliminary study, 11 patients with CSDH underwent burr hole craniectomy and drainage. Membrane specimens were stained with a monoclonal antibody targeting AQP1 for immunohistochemical analysis. The endothelial cells of the sinusoid capillaries of the outer membranes exhibited an elevated immunoreactivity to AQP1 antibody compared to the staining intensity of specimens from the inner membrane and normal dura. These findings suggest that the outer membrane might be the source of the increased fluid accumulation responsible for chronic hematoma enlargement. [Copyright &y& Elsevier]

Published
2010
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34. bcl-2 EXPRESSION IN PLEURAL AND EXTRAPLEURAL SOLITARY FIBROUS TUMOURS

Author

CHILOSI, MARCO, FACCHETTI, FABIO, TOS, ANGELO P. DEI, LESTANI, MAURIZIO, MORASSI, MARIA L., MARTIGNONI, GUIDO, SORIO, CLAUDIO, BENEDETTI, ALICE, MORELLI, LUCA, DOGLIONI, CLAUDIO, BARBERIS, MASSIMO, MENESTRINA, FABIO, and VIALE, GIUSEPPE

Abstract

This study evaluated the immunoreactivity for bcl-2, a molecule involved in the control of programmed cell death, in cases of pleural (14) and extrapleural (2) solitary fibrous tumour (SFT), malignant mesotheliomas of different histological types, and a variety of extrapleural CD34-positive and CD34-negative spindle-cell tumours. In all SFTs, strong and diffuse immunostaining was demonstrated with anti-bcl-2 antibody, sharply contrasting with the complete lack of staining observed in all mesotheliomas. The specificity of immunodetection of bcl-2 in SFT was confirmed by immunoblot analysis, showing a band consistent with the bcl-2 protein. At extrapleural locations, strong bcl-2 immunoreactivity was observed in Schwannoma (2/3 cases), synovial sarcoma (4/4 cases), and all cases of CD34-positive gastrointestinal stromal tumour (GIST; 10/10 cases). Most sarcomas were bcl-2-negative. Lack of bcl-2 expression was demonstrated in tumours which can pose problems in the differential diagnosis of SFT and can exhibit haemangiopericytoma-like features, including haemangiopericytoma (3 cases), dermatofibrosarcoma protuberans (16 cases), and deep-seated fibrous histiocytoma (3 cases). The constitutive expression of bcl-2 in SFT widens the spectrum of available markers for these tumours, providing a useful adjunct to their differential diagnosis in difficult cases at pleural and extrapleural sites, and contributing to the understanding of their histogenesis and molecular pathogenesis. © 1997 by John Wiley & Sons, Ltd.

Published
1997
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35. MOLECULAR ABNORMALITIES OF THE p53 PATHWAY IN DEDIFFERENTIATED LIPOSARCOMA

Author

TOS, ANGELO P. DEI, DOGLIONI, CLAUDIO, PICCININ, SARA, MAESTRO, ROBERTA, MENTZEL, THOMAS, BARBARESCHI, MATTIA, BOIOCCHI, MAURO, and FLETCHER, CHRISTOPHER D. M.

Abstract

Dedifferentiated liposarcoma represents a distinct subtype of liposarcoma and is characterized by the presence of abrupt transition from well-differentiated liposarcoma to high-grade pleomorphic sarcoma (mostly MFH-like). A key role for p53 in tumour progression of this subset of liposarcomas has been suggested on the basis of p53 immunopositivity. A series of 14 dedifferentiated liposarcomas has been investigated by analysing the p53 gene and protein together with the p53-related molecules p21Waf1 and mdm2, to verify whether the p53 pathway is involved in the development and progression of this tumour type. The results indicate that the p53 gene is rarely involved in dedifferentiated liposarcoma (7 per cent of cases analysed) and that low percentages of p53 immunopositivity are still compatible with integrity of the p53 gene. This concept is also supported by the observed preservation of p21Waf1 immunoreactivity in all but the p53-mutated cases. By contrast, mdm2 overexpression emerges as the most frequent abnormality in dedifferentiated liposarcoma (57 and 78 per cent of cases in well-differentiated and high-grade areas, respectively). © 1997 by John Wiley & Sons, Ltd.

Published
1997
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36. Cyclin D3 expression in normal, reactive and neoplastic tissues

Author

Doglioni, Claudio, Chiarelli, Concetta, Macrí, Ettore, Tos, Angelo P. Dei, Meggiolaro, Enzo, Palma, Paolo Dalla, and Barbareschi, Mattia

Abstract

Cyclin D3 immunohistochemical expression was investigated in normal, reactive, and neoplastic human embryonal and adult tissues. In the fetus, cyclin D3 was expressed in selected developmental phases of a limited number of cell systems. In normal adult tissues, cyclin D3 showed two patterns of distribution: in lymphoid tissues it was expressed in proliferative compartments, while in most other tissues it was expressed by terminally differentiated/quiescent cells. This dual role in proliferation and differentiation was partially conserved in neoplasms. In non-Hodgkin lymphomas, cyclin D3 immunolabelling was correlated with proliferative activity and progression; a significant exception was seen in cyclin D1-positive mantle cell lymphomas, which were cyclin D3-negative. Benign endocrine tumours were frequently strongly cyclin D3-positive, while high-grade (small cell) neuroendocrine carcinomas were always negative. In most other epithelial neoplasms, cyclin D3 immunostaining was heterogeneous. In breast carcinomas, no relationship was seen between ER status and MIB1 labelling; cyclins D3 and D1 were frequently expressed in the same tumour, while occasional tumours showed an inverse quantitative relationship between cyclins D1 and D3, and rare tumours were negative for both. In soft tissue neoplasms, cyclin D3 was consistently expressed in some tumours, such as stromal tumours of the gastrointestinal tract and embryonal rhabdomyosarcomas. Our data suggest that cyclin D3 has a dual role in proliferation and differentiation in normal tissues and in some neoplastic conditions; that the cyclin D3 expression pattern is different from cyclin D1, suggesting non-redundant functions; that cyclin D3 expression is strong in endocrine cells secreting steroid hormones, and in their neoplastic counterparts; and that cyclin D3 deregulation may be of pathogenetic relevance in lymphomagenesis and could be diagnostically useful. © 1998 John Wiley & Sons, Ltd.

Published
1998
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42. Bone sarcomas: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up

Author

Hogendoorn, P. C. W., Athanasou, N., Bielack, S., De Alava, E., Tos, A. P. Dei, Ferrari, S., Gelderblom, H., Grimer, R., Hall, K. Sundby, Hassan, B., Jurgens, H., Paulussen, M., Rozeman, L., Taminiau, A.H.M., Whelan, J., Vanel, D., Hogendoorn, P. C. W., Athanasou, N., Bielack, S., De Alava, E., Tos, A. P. Dei, Ferrari, S., Gelderblom, H., Grimer, R., Hall, K. Sundby, Hassan, B., Jurgens, H., Paulussen, M., Rozeman, L., Taminiau, A.H.M., Whelan, J., and Vanel, D.

44. Authors' reply

Author

Chilosi, Marco, Tos, Angelo P. Dei, Faccheti, Fabio, Lestani, Maurizio, Doglioni, Claudio, and Viale, Giuseppe

Abstract

No Abstract

Published
1998
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45. Short, full-dose adjuvant chemotherapy (CT) in high-risk adult soft tissue sarcomas (STS): long-term follow-up of a randomized clinical trial from the Italian Sarcoma Group and the Spanish Sarcoma Group.

Author

Gronchi, A., Stacchiotti, S., Verderio, P., Ferrari, S., Broto, J. Martin, Lopez-Pousa, A., Llombart-Bosch, A., Tos, A. P. Dei, Collini, P., Jurado, J. Cruz, De Paoli, A., Donati, D. M., Poveda, A., Quagliuolo, V., Comandone, A., Grignani, G., Morosi, C., Messina, A., De Sanctis, R., and Bottelli, S.

Subjects
*CANCER chemotherapy, *SOFT tissue tumors, *EPIRUBICIN, *DRUG dosage, *CANCER radiotherapy, *TUMOR treatment
Abstract

Background: To report on long-term results of a phase 3 trial comparing three versus five cycles of adjuvant chemotherapy (CT) with full-dose epirubicinþifosfamide in high-risk soft tissue sarcomas (STS). Methods: Patients (pts) were randomized to receive three preoperative cycles of epirubicin 120 mg/m² and ifosfamide 9 g/m² (Arm A) or to receive the same three preoperative cycles plus two postoperative cycles (Arm B). Radiotherapy could be either delivered in the preoperative or in the postoperative setting. Non-inferiority of the primary end point, OS, was assessed by the confidence interval of the hazard ratio (HR; Arm A/Arm B) derived from Cox model. Results: Between January 2002 and April 2007, 164 pts were assigned to arm A and 164 to arm B. At a median followup (FU) of 117 months (IQ range 103-135 months), 123 deaths were recorded: 58 in Arm A and 65 in Arm B. Ten-year OS was 61% for the entire group of patients: 64% in Arm A and 59% in Arm B. The intention-to-treat analysis confirmed that three cycles were not inferior to five cycles (one-sided 95% upper confidence limit was 1.24). A per protocol analysis was consistent with these results. Pts with leiomyosarcoma and undifferentiated pleomorphic sarcoma (UPS) had the lowest, and the highest response rates, respectively. Consistently, Leiomyosarcoma and UPS had the worse and the best prognosis, respectively. Conclusions: At a longer FU, the non-inferiority of three cycles of a full-dose conventional CT in comparison to five is confirmed. Response to therapy is also confirmed to be associated with better survival. This regimen is currently tested within an ongoing international trial against three cycles of a neoadjuvant histology-tailored CT (ClinicalTrials.gov Identifier: NCT01710176). [ABSTRACT FROM AUTHOR]

Published
2016
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46. Descriptive epidemiology of Kaposi sarcoma in Europe. Report from the RARECARE project.

Author

Stiller, C. A., Trama, A., Brewster, D. H., Verne, J., Bouchardy, C., Navarro, C., Chirlaque, M. D., Marcos-Gragera, R., Visser, O., Serraino, D., Weiderpass, E., Tos, A. P. Dei, and Ascoli, V.

Subjects
*KAPOSI'S sarcoma, *HERPESVIRUS diseases, *EPIDEMIOLOGY of cancer, *IMMUNOCOMPROMISED patients, *DISEASE incidence, *RARE diseases
Abstract

Kaposi sarcoma (KS) is a virus-related malignancy which most frequently arises in skin' though visceral sites can also be involved. Infection with Kaposi sarcoma herpes virus (KSHV or HHV-8) is required for development of KS. Nowadays' most cases worldwide occur in persons who are immunosuppressed' usually because of HIV infection or as a result of therapy to combat rejection of a transplanted organ' but classic Kaposi sarcoma is predominantly a disease of the elderly without apparent immunosuppression. We analyzed 2667 KS incident cases diagnosed during 1995-2002 and registered by 75 population-based European cancer registries contributing to the RARECARE project. Total crude and age-standardized incidence rate was 0.3 per 100'000 per year with an estimated 1642 new cases per year in the EU27 countries. Age-standardized incidence rate was 0.8 per 100'000 in Southern Europe but below 0.3 per 100'000 in all other regions. The elevated rate in southern Europe was attributable to a combination of classic Kaposi sarcoma in some Mediterranean countries and the relatively high incidence of AIDS in several countries. Five-year relative survival for 2000-2002 by the period method was 75%. More than 10'000 persons were estimated to be alive in Europe at the beginning of 2008 with a past diagnosis of KS. The aetiological link with suppressed immunity means that many people alive following diagnosis of KS suffer comorbidity from a pre-existing condition. While KS is a rare cancer' it has a relatively good prognosis and so the number of people affected by it is quite large. Thus it provides a notable example of the importance of networking in diagnosis' therapy and research for rare cancers. [ABSTRACT FROM AUTHOR]

Published
2014
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47. Anthracycline, Gemcitabine, and Pazopanib in Epithelioid Sarcoma A Multi-institutional Case Series

Author

Olivier Mir, Olga Anurova, Robert S. Benjamin, Naofumi Asano, Javier Martin Broto, Ravin Ratan, Uta Flucke, Andrew J. Wagner, Ingvild Lobmaier, Emanuela Palmerini, Hans Gelderblom, Anna Maria Frezza, Mehdi Brahmi, Terrier Philippe, Wei Lien Wang, Michal Wagrodzki, Silvia Stacchiotti, Paolo G. Casali, Bruno Vincenzi, Marta Sbaraglia, Alessandro Gronchi, Piero Picci, Piotr Rutkowski, Jean-Yves Blay, Alexander Fedenko, Jason L. Hornick, Kirsten Sundby Hall, Ingrid M.E. Desar, Khin Thway, Salvatore Lorenzo Renne, Giovanni Grignani, Dominique Ranchère, Eytan Ben-Ami, Paola Collini, Luigi Mariani, Salvatore Lo Vullo, Paweł Teterycz, Akira Kawai, Akihiko Yoshida, Kjetil Boye, Robin L. Jones, Angelo Paolo Dei Tos, Antonella Brunello, Francesca Lucibello, Frezza, Anna Maria, Jones, Robin L., Vullo, Salvatore Lo, Asano, Naofumi, Lucibello, Francesca, Ben-Ami, Eytan, Ratan, Ravin, Teterycz, Pawel, Boye, Kjetil, Brahmi, Mehdi, Palmerini, Emanuela, Fedenko, Alexander, Vincenzi, Bruno, Brunello, Antonella, Desar, Ingrid M. E., Benjamin, Robert S., Blay, Jean Yve, Broto, Javier Martin, Casali, Paolo G., Gelderblom, Han, Grignani, Giovanni, Gronchi, Alessandro, Hall, Kirsten Sundby, Mir, Olivier, Rutkowski, Piotr, Wagner, Andrew J., Anurova, Olga, Collini, Paola, Tos, Angelo P. Dei, Flucke, Uta, Hornick, Jason L., Lobmaier, Ingvild, Philippe, Terrier, Picci, Piero, Ranchere, Dominique, Renne, Salvatore L., Sbaraglia, Marta, Thway, Khin, Wagrodzki, Michal, Wang, Wei-Lien, Yoshida, Akihiko, Mariani, Luigi, Kawai, Akira, and Stacchiotti, Silvia

Subjects
0301 basic medicine, Oncology, Adult, Male, Cancer Research, medicine.medical_specialty, Indazoles, Anthracycline, Adolescent, Epithelioid sarcoma, Kaplan-Meier Estimate, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Deoxycytidine, Pazopanib, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Anthracyclines, Response Evaluation Criteria in Solid Tumors, Aged, Retrospective Studies, Sulfonamides, business.industry, Brief Report, Remission Induction, Retrospective cohort study, Sarcoma, Middle Aged, medicine.disease, Gemcitabine, 030104 developmental biology, Pyrimidines, chemistry, 030220 oncology & carcinogenesis, Female, business, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], medicine.drug
Abstract

Item does not contain fulltext Importance: Epithelioid sarcoma (ES) is an exceedingly rare malignant neoplasm with distinctive pathologic, molecular, and clinical features as well as the potential to respond to new targeted drugs. Little is known on the activity of anthracycline-based regimens, gemcitabine-based regimens, and pazopanib in this disease. Objective: To report on the activity of anthracycline-based regimens, gemcitabine-based regimens, and pazopanib in patients with advanced ES. Design, Setting, and Participants: Seventeen sarcoma reference centers in Europe, the United States, and Japan contributed data to this retrospective analysis of patients with locally advanced/metastatic ES diagnosed between 1990 and 2016. Local pathological review was performed in all cases to confirm diagnosis according to most recent criteria. Exposures: All patients included in the study received anthracycline-based regimens, gemcitabine-based regimens, or pazopanib. Main Outcome and Measures: Response was assessed by RECIST. Progression-free survival (PFS) and overall survival (OS) were computed by Kaplan-Meier method. Classic and proximal subtypes were defined based on morphology (according to 2013 World Health Organization guidelines). Results: Overall, 115 patients were included, 80 (70%) were men and 35 (30%) were women, with a median age of 32 years (range, 15-77 years). Of the 115 patients with ES, 85 were treated with anthracycline-based regimens, 41 with gemcitabine-based regimens, and 18 with pazopanib. Twenty-four received more than 1 treatment. Median follow-up was 34 months. Response rate for anthracycline-based regimens was 22%, with a median PFS of 6 months. One complete response (CR) was reported. A trend toward a higher response rate was noticed in morphological proximal type (26%) vs classic type (19%) and in proximal vs distal primary site (26% vs 18%). The response rate for gemcitabine-based regimens was 27%, with 2 CR and a median PFS of 4 months. In this group, a trend toward a higher response rate was reported in classic vs proximal morphological type (30% vs 22%) and in distal vs proximal primary site (40% vs 14%). In the pazopanib group, no objective responses were seen, and median PFS was 3 months. Conclusions and Relevance: This is the largest retrospective series of systemic therapy in ES. We confirm a moderate activity of anthracycline-based and gemcitabine-based regimens in ES, with a similar response rate and PFS in both groups. The value of pazopanib was low. These data may serve as a benchmark for trials of novel agents in ES.

Published
2018

48. Evolution of Dermatofibrosarcoma Protuberans to DFSP-Derived Fibrosarcoma: An Event Marked by Epithelial-Mesenchymal Transition-like Process and 22q Loss

Author

Stefano Radaelli, Roberta Maestro, Andrea Fontana, Milena Urbini, Silvana Pilotti, Silvia Stacchiotti, Annalisa Astolfi, Chiara Castelli, Tiziana Negri, Silvia Brich, Gianpaolo Dagrada, Chiara Colombo, Paolo G. Casali, Maria Abbondanza Pantaleo, Monica Brenca, Marcella Tazzari, Angelo Paolo Dei Tos, Alessandro Gronchi, Valentina Indio, Stacchiotti, Silvia, Astolfi, Annalisa, Gronchi, Alessandro, Fontana, Andrea, Pantaleo, MARIA ABBONDANZA, Negri, Tiziana, Brenca, Monica, Tazzari, Marcella, Urbini, Milena, Indio, Valentina, Colombo, Chiara, Radaelli, Stefano, Brich, Silvia, Tos, Angelo P. Dei, Casali, Paolo G., Castelli, Chiara, Dagrada, Gian Paolo, Pilotti, Silvana, Maestro, Roberta, Maestro, R, Pilotti, S, Dagrada, Gp, Castelli, C, Casali, Pg, Dei Tos, Ap, Radaelli, S, Colombo, C, Indio, V, Urbini, M, Tazzari, M, Brenca, M, Negri, T, Pantaleo, Ma, Fontana, A, Gronchi, A, Astolfi, A, and Stacchiotti, S.

Subjects
Adult, Male, 0301 basic medicine, Cancer Research, Epithelial-Mesenchymal Transition, Skin Neoplasms, Molecular Biology, Oncology, Adolescent, Chromosomes, Human, Pair 22, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Copy number analysis, Biology, Polymorphism, Single Nucleotide, Fibrosarcomatou, NO, Metastasis, Young Adult, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, Dermatofibrosarcoma Protuberans, Fibrosarcomatous, Dermatofibrosarcoma protuberans, medicine, Humans, DFSP, Epithelial–mesenchymal transition, Fibrosarcoma, Aged, Aged, 80 and over, Dermatofibrosarcoma, Middle Aged, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Disease Progression, Cancer research, Immunohistochemistry, Female, Dermatofibrosarcoma Protuberan
Abstract

Dermatofibrosarcoma protuberans (DFSP) is a rare and indolent cutaneous sarcoma. At times, a fibrosarcomatous transformation marked by a more aggressive clinical behavior may be present. We investigated the natural history and the molecular bases of progression from classic DFSP to the fibrosarcomatous form (FS-DFSP), looking, retrospectively, at the outcome of all patients affected by primary DFSP treated at our institution from 1993 to 2012 and analyzing the molecular profile of 5 DFSPs and 5 FS-DFSPs by an integrated genomics approach (whole transcriptome sequencing, copy number analysis, FISH, qRT-PCR, IHC). The presence of fibrosarcomatous features was identified in 20 (7.6%) patients out of 263 DFSP. All cases were treated with macroscopic complete surgery. A local relapse occurred in 4 of 23 patients who received a microscopic marginal surgery (2 classic DFSP, 2 FS-DFSP), while metastasis affected 2 patients, both FS-DFSP (10% of FS-DFSP), being the first event. DFSP evolution to FS-DFSP was paralleled by a transcriptional reprogramming. The recurrent loss of chromosome 22q appeared to contribute to this phenomenon by promoting the expression of epigenetic regulators, such as EZH2. Loss of the p16/CDKN2A/INK4A locus at 9p was also observed in two FS-DFSP metastatic cases. Implications: FS-DFSP is a rare subgroup among DFSP, with a 10% metastatic risk, that was independent from local recurrence and that was not observed in DFSP, that were all cured by wide surgery. Chromosome 22q deletion might play a role in FS-DFSP, and p16 loss may convey a poor outcome. EZH2 dysregulation was also found and represents a druggable target. Mol Cancer Res; 14(9); 820–9. ©2016 AACR.

Published
2016
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49. Rare neoplasm mimicking neuoroendocrine pancreatic tumor: A case report of solitary fibrous tumor with review of the literature

Author

Angelo Paolo Dei Tos, Iccolò Bassi, Francesco D'Amico, Antonio Giordano, Maurizio Romano, Marina Di Domenico, Marta Sbaraglia, Marco Massani, Cesare Ruffolo, Tiziana Garofalo, D'Amico, Francesco E., Ruffolo, Cesare, Romano, Maurizio, Di Domenico, Marina, Sbaraglia, Marta, Tos, Angelo P. Dei, Garofalo, Tiziana, Giordano, Antonio, Bassi, Niccolã², and Massani, Marco

Subjects
Male, Solitary fibrous tumor, medicine.medical_specialty, Pathology, Cancer Research, Enucleation, CD34, 03 medical and health sciences, 0302 clinical medicine, Solitary Fibrous Tumor, Pancreatic tumor, medicine, Carcinoma, Humans, Neoplasm, Tomography, business.industry, Pancreatic Neoplasm, General Medicine, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Carcinoma, Neuroendocrine, Pancreatic Neoplasms, Solitary Fibrous Tumors, Tomography, X-Ray Computed, Oncology, X-Ray Computed, Neuroendocrine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunohistochemistry, 030211 gastroenterology & hepatology, Radiology, Pancreas, business, Human
Abstract

Background: Solitary fibrous tumors (SFTs) are rare biological entities described mainly in the pleura. To date, in the pancreas, only 14 cases have been reported in the English literature. Case Report: A 52-year-old male was diagnosed incidentally with a suspected neuroendocrine tumor (NET) of the pancreas. He underwent pancreatic enucleation of the mass, which, at final pathology, showed spindle cell proliferation set in a collagenous background and featuring the presence of hemangiopericytoma-like blood. Immunohistochemistry showed cytoplasmic expression of CD34 and nuclear expression of STAT6. As mitotic activity was of 1 mitoses/10 high-power fields (HPFs) a diagnosis of conventional SFT was made. The patient was discharged without major complications and is alive and free of disease after 24 months. Conclusion: SFTs of pancreas are rare tumors, often mimicking pancreatic NET.

Published
2017

50. Bone sarcomas: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up.

Author

Hogendoorn, P. C. W., Athanasou, N., Bielack, S., De Alava, E., Tos, A. P. Dei, Ferrari, S., Gelderblom, H., Grimer, R., Hall, K. Sundby, Hassan, B., Jurgens, H., Paulussen, M., Rozeman, L., Taminiau, A.H.M., Whelan, J., and Vanel, D.

Subjects
*MEDICAL protocols, *PHYSICIAN practice patterns, *OSTEOSARCOMA, *BONE cancer treatment, *BIOPSY, *CLINICAL medicine, *DIAGNOSIS
Abstract

The article focuses on the clinical practice guidelines for bone sarcomas diagnosis, and treatment by the European Society for Medical Oncology (ESMO). It recommends the reference of patients with suspected primary malignant bone tumour to centers that specialize in bone sarcoma network prior to biopsy. It deiscusse the primary malignant bone tumour types based on the World Health Organization (WHO) classification including osteocarcinoma, Ewing carcinoma, and spindle cell sarcomas of bone.

Published
2010
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