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2. Nuove prospettive di analisi dei film di famiglia delle vacanze. Il paesaggio marino e lo sguardo del turista

Author

Andreatta, C, Argentina, M, Boldorini, G, Bosio, F, Bridi, E, Casarin, C, Chiocca, A, Daniele, F, Fecchio, M, Saretta, Y, Mosimann, FS, Urbani, G, Zanon, R, Agnoletto, P, Andreatta, C, Argentina, M, Boldorini, G, Bosio, F, Bridi, E, Casarin, C, Chiocca, A, Daniele, F, Fecchio, M, Saretta, Y, Mosimann, FS, Urbani, G, Zanon, R, and Agnoletto, P

Abstract

I film di famiglia, ossia tutti quei filmati amatoriali realizzati per essere mostrati tra amici e parenti, e che spesso ritraggono ricorrenze, eventi, o vacanze, da alcuni decenni hanno iniziato a riscuotere l’interesse dei ricercatori, anche grazie al lavoro di recupero di archivisti e artisti che hanno trasferito queste memorie da un contesto domestico e privato, ad uno pubblico (Aasman, Montrescu-Mayes, 2019). L’approccio di indagine più comune parte dal fondo, affrontando tempi quali la memoria e la genealogia (Cati, 2009), gli aspetti sociali (Zimmermann, 1995), o le identity politics (Montrescu-Mayes, Norris Nicholson, 2018). Una prospettiva innovativa è stata data, invece, da Paolo Simoni (2018), il quale si è soffermato sul rapporto tra la produzione amatoriale e lo spazio urbano. La mia ricerca si allinea al lavoro di Simoni, ma cerca di valorizzare una tipologia di film di famiglia spesso tralasciata e finora poco esplorata dal mondo accademico: i film di vacanze (Locatelli, 2005). Di natura interdisciplinare tra media studies e geografia, ha preso in esame più di duecento bobine digitalizzate e conservate presso l’Archivio Nazionale del Cinema d’Impresa di Ivrea, prodotte tra gli anni Cinquanta e l’inizio degli anni Ottanta, da cineoperatori residenti in Piemonte e Lombardia. Lo studio utilizza una mixed methodology: ad una content analysis quantitativa (Rose, 2012) dei numerosi materiali audiovisivi, affianca una analisi qualitativa di alcuni girati particolarmente significativi con l’approccio delle ecocritical geopolitics (dell’Agnese 2021). L’obiettivo è quello di esplorare la profonda evoluzione delle coste liguri avvenuta durante il boom economico del Secondo Dopoguerra e conseguente a uno sviluppo edilizio quasi incontrollato, legato al crescente fabbisogno di seconde case (dell’Agnese, Bagnoli, 2004). Le rappresentazioni dei turisti sono mutate assieme alla pratica turistica? Come si è evoluto il rapporto dei cineoperatori con lo spazio tur, Home movies are amateur films destined to a private use which often represent family celebrations, holidays or events. These documents are recently gaining the scholars interest after a the recovery works made by archivists and artists who transferred these memories from a domestic to a public context (Aasman, Montrescu-Mayes, 2019). The most frequent approaches adopted by scholars focus on fundamental themes like memory and genealogy, social and historical aspects, or the identity politics. A new perspective has been outlined centered on the relationship betweeen amateur production and urban space (Simoni, 2018) On one hand, this research is following the same perspective, on the other hand, it tries to valorize another kind of home movies still not explored and understimate: the holidays movies (Locatelli, 2005). With an interdisciplinare approach wich mix geography and media studies, more than two hundred digitalized films from the National Enterprise Cinema Archive have being analyzed. They have been produced between the Fifties and the early Eighties by filmmakers who were residing in Piedmont and Lumbardy. The research consisted in an exploration of the profound urban evolution of Ligurian coasts through the eyes of the tourists themselves. These trasformations happened during the economic boom of the Second Postwar in Italy and they were caused by the need of “second houses” (dell’Agnese, Bagnoli, 2004). Not only it was possible to highlight year by year the landscape mutation, but it was only possible to observe how the relationship between the touristic space and practice changed.

Published
2023

3. Architetture medievali fortificate e paesaggi rurali del potere: il contesto dell’Alto Brembo in alcuni casi studio

Author

Andreatta, C, Argentina, M, Boldorini, G, Bosio, F, Bridi, E, Casarin, C, Chiocca, A, Daniele, F, Fecchio, M, Saretta, Y, Mosimann, FS, Urbani, G, Zanon, R, Pupella, Chiara, Chiara Pupella (ORCID:0000-0003-0255-4026), Andreatta, C, Argentina, M, Boldorini, G, Bosio, F, Bridi, E, Casarin, C, Chiocca, A, Daniele, F, Fecchio, M, Saretta, Y, Mosimann, FS, Urbani, G, Zanon, R, Pupella, Chiara, and Chiara Pupella (ORCID:0000-0003-0255-4026)

Abstract

The territory of the Brembana Valley represents a privileged context for the study of late- medieval fortified buildings, which were intended as a vital prerequisite for the assertion of power at different levels, not only of high-ranking persons, but also of minor rural families. Architecture becomes the manifest of the role played in society and constitutes a key wit- ness to obtain information about the ways of living and dwelling in a specific reality. Pre- cisely, where there is a wish to declare a supremacy on the defense of territory, significant architectural traces can be found. From field to bibliographic and archival research, it’s possible to take a census and recon- struct both the concrete evidence still preserved today in the territory and within the hidden traces of fortified late-medieval contexts. There are several case studies that highlight the variety of fortified structures scattered throughout the valley, particularly in the “Alto Brem- bo” territory: the context of Averara preserves at least two structures (and probably a third), “Torre della Fontana” and “Torre sopra la Corna”, placed in an elevated position over the val- ley, which constituted a defensive and sighting system for controlling the valley floor; in the Mezzoldo area, at about 1350 meters above sea level, there is the “Castello” locality, mentioned in various documents starting from 1653; similarly, Cusio Superiore and Piazzatorre indicate the presence of areas with the toponym “Castello”; for the neighboring municipalities that de- limit the “Alta Valle”, Lenna and Piazza Brembana, sources attest two towers with a probable defensive function of the valley floor.

Published
2023

5. Unravelling racial differences in hypertensive heart disease by multiparametric cardiovascular magnetic resonance: a phenotype-wide association study

Author

Georgiopoulos, G, primary, Vennin, S, additional, Faconti, L, additional, Mc Nally, R, additional, Mohamed, A, additional, Hugelshofer, S, additional, Nicoli, F, additional, Alfakih, K, additional, Mughal, N, additional, Bosio, F, additional, Alastruey-Arimon, J, additional, Keehn, L, additional, Chiribiri, A, additional, Chowienczyk, P, additional, and Masci, PG, additional

Published
2021
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7. A standard test phantom for the performance assessment of magnetic resonance guided high intensity focused ultrasound (MRgHIFU) thermal therapy devices.

Author

Ambrogio, S., Bâesso, R. M., Bosio, F., Fedele, F., Ramnarine, K. V., Zeqiri, B., and Miloro, P.

Subjects
MAGNETIC resonance, ULTRASONIC imaging, THERMOCOUPLES, TEMPERATURE measurements, MAGNETIC materials
Abstract

Purpose: Test objects for High Intensity Focused Ultrasound (HIFU) are required for the standardization and definition of treatment, Quality Assurance (QA), comparison of results between centers and calibration of devices. This study describes a HIFU test object which provides temperature measurement as a function of time, in a reference material compatible with Magnetic Resonance (MR) and ultrasound. Materials and methods: T-Type fine wire thermocouples were used as sensors and 5 correction methods for viscous heating artifacts were assessed. The phantom was tested in a MR-HIFU Philips Sonalleve device over a period of 12 months, demonstrating stability and validity to evaluate the performance of the device. Results: The study furnished useful information regarding the MR-HIFU sessions and highlighted potential limitations of the existing QA and monitoring methods. The importance of temperature monitoring along the whole acoustic path was demonstrated as MR Thermometry readings differed in the three MR plane views (coronal, sagittal, transverse), in particular when the focus was near a soft-tissue/bone interface, where there can be an MR signal loss with significant temperature and thermal dose underestimation (138% variation between the three plane views). Conclusions: The test object was easy to use and has potential as a valid tool for training, QA, research and development for MR guided HIFU and potentially ultrasound guided devices. [ABSTRACT FROM AUTHOR]

Published
2022
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17. PATHOLOGY: IMMUNE AND INFLAMMATORY MECHANISMS

Author

Kozakowski, N., primary, Herkner, H., additional, Bohmig, G. A., additional, Kikic, Z., additional, Cooper, D. J., additional, Eller, K., additional, Kirsch, A. H., additional, Lane, P. J., additional, Neirynck, N., additional, Glorieux, G., additional, Schepers, E., additional, Dhondt, A., additional, Vanholder, R., additional, Corradetti, V., additional, Milanesi, S., additional, Rocca, C., additional, Avanzini, M. A., additional, Pattonieri, E. F., additional, Bosio, F., additional, Cannone, M., additional, Maggi, N., additional, Gregorini, M., additional, Esposito, P., additional, Rampino, T., additional, Dal Canton, A., additional, Roelofs, J. J., additional, Redecha, P., additional, Salmon, J. E., additional, Rho, E., additional, Artinger, K., additional, Schaubettl, C., additional, Aringer, I., additional, Rosenkranz, A. R., additional, Eller, P., additional, Perri, A., additional, Vizza, D., additional, Toteda, G., additional, Lupinacci, S., additional, Lofaro, D., additional, Leone, F., additional, Gigliotti, P., additional, La Russa, A., additional, Papalia, T., additional, Bonofilgio, R., additional, and Schabhuttl, C., additional

Published
2014
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18. TRANSPLANTATION BASIC SCIENCE, ALLOGENIC AND XENOGENIC TOLERANCE

Author

Berthelot, L., primary, Robert, T., additional, Tabary, T., additional, Vuiblet, V., additional, Drame, M., additional, Toupance, O., additional, Rieu, P., additional, Monteiro, R. C., additional, Toure, F., additional, Ferrario, S., additional, Cantaluppi, V., additional, De Lena, M., additional, Dellepiane, S., additional, Beltramo, S., additional, Rossetti, M., additional, Manzione, A. M., additional, Messina, M., additional, Gai, M., additional, Dolla, C., additional, Biancone, L., additional, Camussi, G., additional, Pontrelli, P., additional, Oranger, A. R., additional, Accetturo, M., additional, Rascio, F., additional, Gigante, M., additional, Castellano, G., additional, Schena, A., additional, Fiorentino, M., additional, Zito, A., additional, Zaza, G., additional, Stallone, G., additional, Gesualdo, L., additional, Grandaliano, G., additional, Pattonieri, E. F., additional, Gregorini, M., additional, Corradetti, V., additional, Rocca, C., additional, Milanesi, S., additional, Peloso, A., additional, Ferrario, J., additional, Cannone, M., additional, Bosio, F., additional, Maggi, N., additional, Avanzini, M. A., additional, Minutillo, P., additional, Paulli, M., additional, Maestri, M., additional, Rampino, T., additional, Dal Canton, A., additional, Wu, K. S. T., additional, Coxall, O., additional, Luque, Y., additional, Candon, S., additional, Rabant, M., additional, Noel, L.-H., additional, Thervet, E., additional, Chatenoud, L., additional, Snanoudj, R., additional, Anglicheau, D., additional, Legendre, C., additional, Zuber, J., additional, Hruba, P., additional, Brabcova, I., additional, Krepsova, E., additional, Slatinska, J., additional, Sekerkova, A., additional, Striz, I., additional, Zachoval, R., additional, Viklicky, O., additional, Scholbach, T. M., additional, Wang, H.-K., additional, Loong, C.-C., additional, Yang, A.-H., additional, Wu, T.-H., additional, Guberina, H., additional, Rebmann, V., additional, Dziallas, P., additional, Dolff, S., additional, Wohlschlaeger, J., additional, Heinemann, F. M., additional, Witzke, O., additional, Zoet, Y. M., additional, Claas, F. H. J., additional, Horn, P. A., additional, Kribben, A., additional, Doxiadis, I. I. N., additional, Prasad, N., additional, Yadav, B., additional, Agarwal, V., additional, Jaiswal, A., additional, Rai, M., additional, Hope, C. M., additional, Coates, P. T., additional, Heeger, P. S., additional, Carroll, R., additional, Masola, V., additional, Secchi, M. F., additional, Onisto, M., additional, Gambaro, G., additional, Lupo, A., additional, Matsuyama, M., additional, Kobayashi, T., additional, Yoneda, Y., additional, Chargui, J., additional, Touraine, J. L., additional, Yoshimura, R., additional, Vizza, D., additional, Perri, A., additional, Lupinacci, S., additional, Toteda, G., additional, Lofaro, D., additional, Leone, F., additional, Gigliotti, P., additional, La Russa, A., additional, Papalia, T., additional, Bonofilgio, R., additional, Sentis Fuster, A., additional, Kers, J., additional, Yapici, U., additional, Claessen, N., additional, Bemelman, F. J., additional, Ten Berge, I. J. M., additional, Florquin, S., additional, Glotz, D., additional, Rostaing, L., additional, Squifflet, J.-P., additional, Merville, P., additional, Belmokhtar, C., additional, Le Ny, G., additional, Lebranchu, Y., additional, Papazova, D. A., additional, Friederich-Persson, M., additional, Koeners, M. P., additional, Joles, J. A., additional, Verhaar, M. C., additional, Trivedi, H. L., additional, Vanikar, A. V., additional, Dave, S. D., additional, Suarez Alvarez, B., additional, Garcia Melendreras, S., additional, Carvajal Palao, R., additional, Diaz Corte, C., additional, Ruiz Ortega, M., additional, Lopez-Larrea, C., additional, Yadav, A. K., additional, Bansal, D., additional, Kumar, V., additional, Minz, M., additional, Jha, V., additional, Kaminska, D., additional, Koscielska-Kasprzak, K., additional, Chudoba, P., additional, Mazanowska, O., additional, Banasik, M., additional, Zabinska, M., additional, Boratynska, M., additional, Lepiesza, A., additional, Korta, K., additional, Klinger, M., additional, Csohany, R., additional, Prokai, A., additional, Pap, D., additional, Balicza-Himer, N., additional, Vannay, A., additional, Fekete, A., additional, Kis-Petik, K., additional, Peti-Peterdi, J., additional, Szabo, A., additional, Masajtis-Zagajewska, A., additional, Muras, K., additional, Niewodniczy, M., additional, Nowicki, M., additional, Pascual, J., additional, Srinivas, T. R., additional, Chadban, S., additional, Citterio, F., additional, Henry, M., additional, Oppenheimer, F., additional, Lee, P.-C., additional, Tedesco-Silva, H., additional, Zeier, M., additional, Watarai, Y., additional, Dong, G., additional, Hexham, M., additional, Bernhardt, P., additional, Vincenti, F., additional, Rocchetti, M. T., additional, Su owicz, J., additional, Wojas-Pelc, A., additional, Ignacak, E., additional, Janda, K., additional, Krzanowski, M., additional, Su owicz, W., additional, Mitsuhashi, M., additional, Murakami, T., additional, Benso, A., additional, Leuning, D., additional, Reinders, M., additional, Lievers, E., additional, Duijs, J., additional, Van Zonneveld, A. J., additional, Van Kooten, C., additional, Engelse, M., additional, Rabelink, T., additional, Assounga, A., additional, Omarjee, S., additional, Ngema, Z., additional, Ersoy, A., additional, Gultepe, A., additional, Isiktas Sayilar, E., additional, Akalin, H., additional, Coskun, F., additional, Oner Torlak, M., additional, Ayar, Y., additional, Riegersperger, M., additional, Plischke, M., additional, Steinhauser, C., additional, Jallitsch-Halper, A., additional, Sengoelge, G., additional, Winkelmayer, W. C., additional, Sunder-Plassmann, G., additional, Foedinger, M., additional, Kaziuk, M., additional, Kuz'Niewski, M., additional, B Tkowska- Prokop, A., additional, Pa Ka, K., additional, Dumnicka, P., additional, Kolber, W., additional, and Su Owicz, W., additional

Published
2014
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20. Experimental pathology

Author

Yi Chun, D. X., primary, Alexandre, H., additional, Edith, B., additional, Nacera, O., additional, Julie, P., additional, Chantal, J., additional, Eric, R., additional, Zhang, X., additional, Jin, Y., additional, Miravete, M., additional, Dissard, R., additional, Klein, J., additional, Gonzalez, J., additional, Caubet, C., additional, Pecher, C., additional, Pipy, B., additional, Bascands, J.-L., additional, Mercier-Bonin, M., additional, Schanstra, J., additional, Buffin-Meyer, B., additional, Claire, R., additional, Rigothier, C., additional, Richard, D., additional, Sebastien, L., additional, Moin, S., additional, Chantal, B., additional, Christian, C., additional, Jean, R., additional, Migliori, M., additional, Cantaluppi, V., additional, Mannari, C., additional, Medica, D., additional, Giovannini, L., additional, Panichi, V., additional, Goldwich, A., additional, Alexander, S., additional, Andre, G., additional, Amann, K., additional, Migliorini, A., additional, Sagrinati, C., additional, Angelotti, M. L., additional, Mulay, S. R., additional, Ronconi, E., additional, Peired, A., additional, Romagnani, P., additional, Anders, H.-J., additional, Chiang, W. C., additional, Lai, C. F., additional, Peng, W.-H., additional, Wu, C. F., additional, Chang, F.-C., additional, Chen, Y.-T., additional, Lin, S.-L., additional, Chen, Y. M., additional, Wu, K. D., additional, Lu, K.-S., additional, Tsai, T. J., additional, Virgine, O., additional, Qing Feng, F., additional, Zhang, S.-Y., additional, Dominique, D., additional, Vincent, A., additional, Marina, C., additional, Philippe, L., additional, Georges, G., additional, Pawlak, A., additional, Sahali, D., additional, Matsumoto, S., additional, Kiyomoto, H., additional, Ichimura, A., additional, Dan, T., additional, Nakamichi, T., additional, Tsujita, T., additional, Akahori, K., additional, Ito, S., additional, Miyata, T., additional, Xie, S., additional, Zhang, B., additional, Shi, W., additional, Yang, Y., additional, Nagasu, H., additional, Satoh, M., additional, Kidokoro, K., additional, Nishi, Y., additional, Ihoriya, C., additional, Kadoya, H., additional, Sasaki, T., additional, Kashihara, N., additional, Wu, C.-F., additional, Chou, Y.-H., additional, Duffield, J., additional, Rocca, C., additional, Gregorini, M., additional, Corradetti, V., additional, Valsania, T., additional, Bedino, G., additional, Bosio, F., additional, Pattonieri, E. F., additional, Esposito, P., additional, Sepe, V., additional, Libetta, C., additional, Rampino, T., additional, Dal Canton, A., additional, Omori, H., additional, Kawada, N., additional, Inoue, K., additional, Ueda, Y., additional, Yamamoto, R., additional, Matsui, I., additional, Kaimori, J., additional, Takabatake, Y., additional, Moriyama, T., additional, Isaka, Y., additional, Rakugi, H., additional, Wasilewska, A., additional, Taranta-Janusz, K., additional, Deebek, W., additional, Kuroczycka-Saniutycz, E., additional, Lee, A. S., additional, Lee, J. E., additional, Jung, Y. J., additional, Kang, K. P., additional, Lee, S., additional, Kim, W., additional, Arfian, N., additional, Emoto, N., additional, Yagi, K., additional, Nakayama, K., additional, Hartopo, A. B., additional, Nugrahaningsih, D. A., additional, Yanagisawa, M., additional, Hirata, K.-I., additional, Munoz-Felix, J. M., additional, Lopez-Novoa, J. M., additional, Martinez-Salgado, C., additional, Oujo, B., additional, Arevalo, M., additional, Bernabeu, C., additional, Perez-Barriocanal, F., additional, Jesper, K., additional, Nathalie, V., additional, Pierre, G., additional, Yi Chun, D. X., additional, Iyoda, M., additional, Shibata, T., additional, Matsumoto, K., additional, Shindo-Hirai, Y., additional, Kuno, Y., additional, Wada, Y., additional, Akizawa, T., additional, Schwartz, I., additional, Schwartz, D., additional, Prot Bertoye, C., additional, Terryn, S., additional, Claver, J., additional, Beghdadi, W. B., additional, Monteiro, R., additional, Blank, U., additional, Devuyst, O., additional, Daugas, E., additional, Van Beneden, K., additional, Geers, C., additional, Pauwels, M., additional, Mannaerts, I., additional, Van den Branden, C., additional, Van Grunsven, L. A., additional, Seckin, I., additional, Pekpak, M., additional, Uzunalan, M., additional, Uruluer, B., additional, Kokturk, S., additional, Ozturk, Z., additional, Sonmez, H., additional, Yaprak, E., additional, Furuno, Y., additional, Tsutsui, M., additional, Morishita, T., additional, Shimokawa, H., additional, Otsuji, Y., additional, Yanagihara, N., additional, Kabashima, N., additional, Ryota, S., additional, Kanegae, K., additional, Miyamoto, T., additional, Nakamata, J., additional, Ishimatsu, N., additional, Tamura, M., additional, Nakagawa, T., additional, Ichikawa, K., additional, Miyamoto, M., additional, Takabayashi, D., additional, Yamazaki, H., additional, Kakeshita, K., additional, Koike, T., additional, Kagitani, S., additional, Tomoda, F., additional, Hamashima, T., additional, Ishii, Y., additional, Inoue, H., additional, Sasahara, M., additional, El Machhour, F., additional, Kerroch, M., additional, Mesnard, L., additional, Chatziantoniou, C., additional, Dussaule, J.-C., additional, Inui, K., additional, Sasai, F., additional, Maruta, Y., additional, Nishiwaki, H., additional, Kawashima, E., additional, Inoue, Y., additional, Yoshimura, A., additional, Musacchio, E., additional, Priante, G., additional, Valvason, C., additional, Sartori, L., additional, Baggio, B., additional, Kim, J. H., additional, Gross, O., additional, Diana, R., additional, Gry, D. H., additional, Asimal, B., additional, Johanna, T., additional, Imke, S.-E., additional, Lydia, W., additional, Gerhard-Anton, M., additional, Hassan, D., additional, Cano, J. L., additional, Griera, M., additional, Olmos, G., additional, Martin, P., additional, Cortes, M. A., additional, Lopez-Ongil, S., additional, Rodriguez-Puyol, D., additional, DE Frutos, S., additional, Gonzalez, M., additional, Luengo, A., additional, Rodriguez-Puyol, M., additional, Calleros, L., additional, Lupica, R., additional, Lacquaniti, A., additional, Donato, V., additional, Maggio, R., additional, Mastroeni, C., additional, Lucisano, S., additional, Cernaro, V., additional, Fazio, M. R., additional, Quartarone, A., additional, Buemi, M., additional, Kacik, M., additional, Goedicke, S., additional, Eggert, H., additional, Hoyer, J. D., additional, Wurm, S., additional, Steege, A., additional, Banas, M., additional, Kurtz, A., additional, Banas, B., additional, Lasagni, L., additional, Lazzeri, E., additional, Romoli, S., additional, Schaefer, I., additional, Teng, B., additional, Worthmann, K., additional, Haller, H., additional, Schiffer, M., additional, Prattichizzo, C., additional, Netti, G. S., additional, Rocchetti, M. T., additional, Cormio, L., additional, Carrieri, G., additional, Stallone, G., additional, Grandaliano, G., additional, Ranieri, E., additional, Gesualdo, L., additional, Kucher, A., additional, Smirnov, A., additional, Parastayeva, M., additional, Beresneva, O., additional, Kayukov, I., additional, Zubina, I., additional, Ivanova, G., additional, Abed, A., additional, Schlekenbach, L., additional, Foglia, B., additional, Kwak, B., additional, Chadjichristos, C., additional, Queisser, N., additional, Schupp, N., additional, Brand, S., additional, Himer, L., additional, Szebeni, B., additional, Sziksz, E., additional, Saijo, S., additional, Kis, E., additional, Prokai, A., additional, Banki, N. F., additional, Fekete, A., additional, Tulassay, T., additional, Vannay, A., additional, Hegner, B., additional, Schaub, T., additional, Lange, C., additional, Dragun, D., additional, Klinkhammer, B. M., additional, Rafael, K., additional, Monika, M., additional, Anna, M., additional, Van Roeyen, C., additional, Boor, P., additional, Eva Bettina, B., additional, Simon, O., additional, Esther, S., additional, Floege, J., additional, Kunter, U., additional, Janke, D., additional, Jankowski, J., additional, Hayashi, M., additional, Takamatsu, I., additional, Horimai, C., additional, Yoshida, T., additional, Seno DI Marco, G., additional, Koenig, M., additional, Stock, C., additional, Reiermann, S., additional, Amler, S., additional, Koehler, G., additional, Fobker, M., additional, Buck, F., additional, Pavenstaedt, H., additional, Lang, D., additional, Brand, M., additional, Plotnikov, E., additional, Morosanova, M., additional, Pevzner, I., additional, Zorova, L., additional, Pulkova, N., additional, Zorov, D., additional, Wornle, M., additional, Ribeiro, A., additional, Belling, F., additional, Merkle, M., additional, Nakazawa, D., additional, Nishio, S., additional, Shibasaki, S., additional, Tomaru, U., additional, Akihiro, I., additional, Kobayashi, I., additional, Imanishi, Y., additional, Kurajoh, M., additional, Nagata, Y., additional, Yamagata, M., additional, Emoto, M., additional, Michigami, T., additional, Ishimura, E., additional, Inaba, M., additional, Wu, C.-C., additional, Lu, K.-C., additional, Chen, J.-S., additional, Chu, P., additional, Lin, Y.-F., additional, Eller, K., additional, Schroll, A., additional, Kirsch, A., additional, Huber, J., additional, Weiss, G., additional, Theurl, I., additional, Rosenkranz, A. R., additional, Zawada, A., additional, Rogacev, K., additional, Achenbach, M., additional, Fliser, D., additional, Held, G., additional, Heine, G. H., additional, Miyamoto, Y., additional, Iwao, Y., additional, Watanabe, H., additional, Kadowaki, D., additional, Ishima, Y., additional, Chuang, V. T. G., additional, Sato, K., additional, Otagiri, M., additional, Maruyama, T., additional, Iwatani, H., additional, Honda, D., additional, Noguchi, T., additional, Tanaka, M., additional, Tanaka, H., additional, Fukagawa, M., additional, Pircher, J., additional, Koppel, S., additional, Mannell, H., additional, Krotz, F., additional, Virzi, G. M., additional, Bolin, C., additional, Cruz, D., additional, Scalzotto, E., additional, De Cal, M., additional, Vescovo, G., additional, Ronco, C., additional, Grobmayr, R., additional, Lech, M., additional, Ryu, M., additional, Aoshima, Y., additional, Mizobuchi, M., additional, Ogata, H., additional, Kumata, C., additional, Nakazawa, A., additional, Kondo, F., additional, Ono, N., additional, Koiwa, F., additional, Kinugasa, E., additional, Freisinger, W., additional, Lale, N., additional, Lampert, A., additional, Ditting, T., additional, Heinlein, S., additional, Schmieder, R. E., additional, Veelken, R., additional, Nave, H., additional, Perthel, R., additional, Suntharalingam, M., additional, Bode-Boger, S., additional, Beutel, G., additional, Kielstein, J., additional, Rodrigues-Diez, R., additional, Rayego-Mateos, S., additional, Lavoz, C., additional, Stark Aroeira, L. G., additional, Orejudo, M., additional, Alique, M., additional, Ortiz, A., additional, Egido, J., additional, Ruiz-Ortega, M., additional, Oskar, W., additional, Rusan, C., additional, Padberg, J.-S., additional, Wiesinger, A., additional, Reuter, S., additional, Grabner, A., additional, Kentrup, D., additional, Lukasz, A., additional, Oberleithner, H., additional, Pavenstadt, H., additional, Kumpers, P., additional, Eberhardt, H. U., additional, Skerka, C., additional, Chen, Q., additional, Hallstroem, T., additional, Hartmann, A., additional, Kemper, M. J., additional, Zipfel, P. F., additional, N'gome-Sendeyo, K., additional, Fan, Q.-F., additional, Toblli, J., additional, Cao, G., additional, Giani, J. F., additional, Dominici, F. P., additional, Kim, J. S., additional, Yang, J. W., additional, Kim, M. K., additional, Han, B. G., additional, and Choi, S. O., additional

Published
2012
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21. Transplantation / Basic research

Author

Wornle, M., primary, Ribeiro, A., additional, Motamedi, N., additional, Nitschko, H., additional, Cohen, C. D., additional, Grone, H. J., additional, Schlondorff, D., additional, Schmid, H., additional, Kislat, C., additional, Schmidt, T., additional, Janssen, M., additional, Wolf, M., additional, Dirks, J., additional, Ahlenstiel, T., additional, Pape, L., additional, Fliser, D., additional, Sester, M., additional, Sester, U., additional, Urbanova, M., additional, Brabcova, I., additional, Girmanova, E., additional, Ondrej, V., additional, Gregorini, M., additional, Rampino, T., additional, Rocca, C., additional, Valsania, T., additional, Corradetti, V., additional, Bosio, F., additional, Bedino, G., additional, Carrara, C., additional, Pattonieri, E. F., additional, Soccio, G., additional, Esposito, P., additional, Dal Canton, A., additional, Becker, L. E., additional, Morath, C., additional, Schaier, M., additional, Gross, M.-L., additional, Bierhaus, A., additional, Waldherr, R., additional, Nawroth, P., additional, Zeier, M., additional, Tataranni, T., additional, Biondi, G., additional, Cariello, M., additional, Mangino, M., additional, Colucci, G., additional, Rutigliano, M., additional, Ditonno, P., additional, Schena, F. P., additional, Pertosa, G., additional, Gesualdo, L., additional, and Grandaliano, G., additional

Published
2011
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22. Experimental pathology

Author

Noh, H., primary, Kim, H. J., additional, Yu, M. R., additional, Ryu, J. H., additional, Kim, J. H., additional, Kim, E., additional, Han, D. C., additional, Bedino, G., additional, Rampino, T., additional, Gregorini, M., additional, Valsania, T., additional, Rocca, C., additional, Corradetti, V., additional, Pattonieri, E. F., additional, Carrara, C., additional, Bosio, F., additional, Piotti, G., additional, Soccio, G., additional, Esposito, P., additional, Albertini, R., additional, Dal Canton, A., additional, Schaefer, I., additional, Himmelseher, E., additional, Haller, H., additional, Schiffer, M., additional, Ryu, M., additional, Mulay, S. R., additional, Miosge, N., additional, Gross, O., additional, Anders, H.-J., additional, Zarzecki, M., additional, Adamczak, M., additional, Wystrychowski, A., additional, Gross, M.-L., additional, Ritz, E., additional, and Wiecek, A., additional

Published
2011
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32. Enhanced current and voltage regulators for stand-alone applications

Author

De Bosio, F., Pastorei, M., Ribeiro, L. A. De S., Freijedo, F. D., and Guerrero, J. M.

Subjects
voltage control, uninterruptible power systems, current control, power quality
Abstract

State feedback decoupling permits to achieve a better dynamic response for Voltage Source in stand-alone applications. The design of current and voltage regulators is performed in the discrete-time domain since it provides better accuracy and allows direct pole placement. As the attainable bandwidth of the current loop is mainly limited by computational and PWM delays, a lead compensator structure is proposed to overcome this limitation. The design of the voltage regulator is based on the Nyquist criterion, verifying to guarantee a high sensitivity peak. Discrete-time domain implementation issues of an anti-wind up scheme are discussed as well. Laboratory tests in compliance with the standard for UPS systems (IEC 62040-3) are performed to validate the theoretical analysis.

33. Frequency constrained optimal Power Flow based on Glow-worm Swarm Optimization in Islanded Microgrids

Author

N.Q. Nguyen, F. de Bosio, Gaetano Zizzo, E. Riva Sanseverino, Quynh T. Tran, M. L. Di Silvestre, RIVA SANSEVERINO, E., NGUYEN QUANG, N., DI SILVESTRE, M., Zizzo, G., De Bosio, F., and Tran, Q.

Subjects
Mathematical optimization, Engineering, frequency constraint, Interface (computing), Islanded microgrid, glow-worm swarm optimization, Biomedical Engineering, Energy Engineering and Power Technology, Control theory, Power electronics, Ampacity, Voltage droop, three phase systems, islanded microgrids, business.industry, Renewable Energy, Sustainability and the Environment, line ampacity constraint, Optimal power flow, Particle swarm optimization, Swarm behaviour, Constraint (information theory), Three phase system, Settore ING-IND/33 - Sistemi Elettrici Per L'Energia, Line (geometry), business
Abstract

This work presents an application of a swarm optimization method to solve the optimal power flow problem taking into account the constraints of frequency and line ampacity in three-phase islanded Microgrids. Each generation unit is equipped with a Power Electronics Interface. In the considered formulation, the droop control parameters are considered as variables to be adjusted by a higher control level, while the frequency is kept in rated bounds. Another typical constraint for OPF formulation, the max ampacity of each line, is also considered. Two case studies with different dimensions and electrical features have been considered and the obtained results show the efficiency of the proposed approach that can be straightforward extended to unbalanced systems.

Published
2015

34. Evaluation of myocarditis with a free-breathing three-dimensional isotropic whole-heart joint T1 and T2 mapping sequence.

Author

Hua A, Velasco C, Munoz C, Milotta G, Fotaki A, Bosio F, Granlund I, Sularz A, Chiribiri A, Kunze KP, Botnar R, Prieto C, and Ismail TF

Subjects
Humans, Male, Adult, Female, Reproducibility of Results, Case-Control Studies, Middle Aged, Young Adult, Respiration, Magnetic Resonance Imaging, Cine, Magnetic Resonance Imaging, Myocardium pathology, Breath Holding, Myocarditis diagnostic imaging, Myocarditis physiopathology, Predictive Value of Tests, Imaging, Three-Dimensional, Image Interpretation, Computer-Assisted
Abstract

Background: The diagnosis of myocarditis by cardiovascular magnetic resonance (CMR) requires the use of T2 and T1 weighted imaging, ideally incorporating parametric mapping. Current two-dimensional (2D) mapping sequences are acquired sequentially and involve multiple breath-holds resulting in prolonged scan times and anisotropic image resolution. We developed an isotropic free-breathing three-dimensional (3D) whole-heart sequence that allows simultaneous T1 and T2 mapping and validated it in patients with suspected myocarditis., Methods: Eighteen healthy volunteers and 28 patients with suspected myocarditis underwent conventional 2D T1 and T2 mapping with whole-heart coverage and 3D joint T1/T2 mapping on a 1.5T scanner. Acquisition time, image quality, and diagnostic performance were compared. Qualitative analysis was performed using a 4-point Likert scale. Bland-Altman plots were used to assess the quantitative agreement between 2D and 3D sequences., Results: The 3D T1/T2 sequence was acquired in 8 min 26 s under free breathing, whereas 2D T1 and T2 sequences were acquired with breath-holds in 11 min 44 s (p = 0.0001). All 2D images were diagnostic. For 3D images, 89% (25/28) of T1 and 96% (27/28) of T2 images were diagnostic with no significant difference in the proportion of diagnostic images for the 3D and 2D T1 (p = 0.2482) and T2 maps (p = 1.0000). Systematic bias in T1 was noted with biases of 102, 115, and 152 ms for basal-apical segments, with a larger bias for higher T1 values. Good agreement between T2 values for 3D and 2D techniques was found (bias of 1.8, 3.9, and 3.6 ms for basal-apical segments). The sensitivity and specificity of the 3D sequence for diagnosing acute myocarditis were 74% (95% confidence interval [CI] 49%-91%) and 83% (36%-100%), respectively, with a c-statistic (95% CI) of 0.85 (0.79-0.91) and no statistically significant difference between the 2D and 3D sequences for the detection of acute myocarditis for T1 (p = 0.2207) or T2 (p = 1.0000)., Conclusion: Free-breathing whole-heart 3D joint T1/T2 mapping was comparable to 2D mapping sequences with respect to diagnostic performance, but with the added advantages of free breathing and shorter scan times. Further work is required to address the bias noted at high T1 values, but this did not significantly impact diagnostic accuracy., Competing Interests: Declaration of competing interests The authors declare the following financial interests/personal relationships which may be considered as potential competing interests. Alina Hua reports financial support was provided by the British Heart Foundation. The Institution reports infrastructure financial support was provided by the National Institute for Health and Care Research (UK). Dr. Karl P. Kunze is an employee of Siemens Healthcare Limited. The other authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2024
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35. Retrospective motion correction through multi-average k-space data elimination (REMAKE) for free-breathing cardiac cine imaging.

Author

Neofytou AP, Neji R, Kowalik GT, Mooiweer R, Wong J, Fotaki A, Ferreira J, Evans C, Bosio F, Mughal N, Razavi R, Pushparajah K, and Roujol S

Subjects
Humans, Retrospective Studies, Respiration, Motion, Artifacts, Magnetic Resonance Imaging, Cine methods, Heart diagnostic imaging
Abstract

Purpose: To develop a motion-robust reconstruction technique for free-breathing cine imaging with multiple averages., Method: Retrospective motion correction through multiple average k-space data elimination (REMAKE) was developed using iterative removal of k-space segments (from individual k-space samples) that contribute most to motion corruption while combining any remaining segments across multiple signal averages. A variant of REMAKE, termed REMAKE+, was developed to address any losses in SNR due to k-space information removal. With REMAKE+, multiple reconstructions using different initial conditions were performed, co-registered, and averaged. Both techniques were validated against clinical "standard" signal averaging reconstruction in a static phantom (with simulated motion) and 15 patients undergoing free-breathing cine imaging with multiple averages. Quantitative analysis of myocardial sharpness, blood/myocardial SNR, myocardial-blood contrast-to-noise ratio (CNR), as well as subjective assessment of image quality and rate of diagnostic quality images were performed., Results: In phantom, motion artifacts using "standard" (RMS error [RMSE]: 2.2 ± 0.5) were substantially reduced using REMAKE/REMAKE+ (RMSE: 1.5 ± 0.4/1.0 ± 0.4, p < 0.01). In patients, REMAKE/REMAKE+ led to higher myocardial sharpness (0.79 ± 0.09/0.79 ± 0.1 vs. 0.74 ± 0.12 for "standard", p = 0.004/0.04), higher image quality (1.8 ± 0.2/1.9 ± 0.2 vs. 1.6 ± 0.4 for "standard", p = 0.02/0.008), and a higher rate of diagnostic quality images (99%/100% vs. 94% for "standard"). Blood/myocardial SNR for "standard" (94 ± 30/33 ± 10) was higher vs. REMAKE (80 ± 25/28 ± 8, p = 0.002/0.005) and tended to be lower vs. REMAKE+ (105 ± 33/36 ± 12, p = 0.02/0.06). Myocardial-blood CNR for "standard" (61 ± 22) was higher vs. REMAKE (53 ± 19, p = 0.003) and lower vs. REMAKE+ (69 ± 24, p = 0.007)., Conclusions: Compared to "standard" signal averaging reconstruction, REMAKE and REMAKE+ provide improved myocardial sharpness, image quality, and rate of diagnostic quality images., (© 2023 The Authors. Magnetic Resonance in Medicine published by Wiley Periodicals LLC on behalf of International Society for Magnetic Resonance in Medicine.)

Published
2023
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36. Incidental finding of primary cardiac lymphoma after cardiac arrest and percutaneous coronary intervention.

Author

Kane C, Bosio F, Wrench D, and Webb J

Subjects
Coronary Angiography, Humans, Incidental Findings, Treatment Outcome, Cardiopulmonary Resuscitation, Heart Arrest etiology, Heart Arrest therapy, Lymphoma diagnostic imaging, Out-of-Hospital Cardiac Arrest, Percutaneous Coronary Intervention
Abstract

Competing Interests: Conflicts of interest: None declared.

Published
2022
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37. Simultaneous multislice steady-state free precession myocardial perfusion with full left ventricular coverage and high resolution at 1.5 T.

Author

McElroy S, Ferrazzi G, Nazir MS, Evans C, Ferreira J, Bosio F, Mughal N, Kunze KP, Neji R, Speier P, Stäb D, Ismail TF, Masci PG, Villa ADM, Razavi R, Chiribiri A, and Roujol S

Subjects
Heart Ventricles diagnostic imaging, Humans, Perfusion, Reproducibility of Results, Image Enhancement methods, Image Interpretation, Computer-Assisted methods
Abstract

Purpose: To implement and evaluate a simultaneous multi-slice balanced SSFP (SMS-bSSFP) perfusion sequence and compressed sensing reconstruction for cardiac MR perfusion imaging with full left ventricular (LV) coverage (nine slices/heartbeat) and high spatial resolution (1.4 × 1.4 mm 2 ) at 1.5T., Methods: A preliminary study was performed to evaluate the performance of blipped controlled aliasing in parallel imaging (CAIPI) and RF-CAIPI with gradient-controlled local Larmor adjustment (GC-LOLA) in the presence of fat. A nine-slice SMS-bSSFP sequence using RF-CAIPI with GC-LOLA with high spatial resolution (1.4 × 1.4 mm 2 ) and a conventional three-slice sequence with conventional spatial resolution (1.9 × 1.9 mm 2 ) were then acquired in 10 patients under rest conditions. Qualitative assessment was performed to assess image quality and perceived signal-to-noise ratio (SNR) on a 4-point scale (0: poor image quality/low SNR; 3: excellent image quality/high SNR), and the number of myocardial segments with diagnostic image quality was recorded. Quantitative measurements of myocardial sharpness and upslope index were performed., Results: Fat signal leakage was significantly higher for blipped CAIPI than for RF-CAIPI with GC-LOLA (7.9% vs. 1.2%, p = 0.010). All 10 SMS-bSSFP perfusion datasets resulted in 16/16 diagnostic myocardial segments. There were no significant differences between the SMS and conventional acquisitions in terms of image quality (2.6 ± 0.6 vs. 2.7 ± 0.2, p = 0.8) or perceived SNR (2.8 ± 0.3 vs. 2.7 ± 0.3, p = 0.3). Inter-reader variability was good for both image quality (ICC = 0.84) and perceived SNR (ICC = 0.70). Myocardial sharpness was improved using the SMS sequence compared to the conventional sequence (0.37 ± 0.08 vs 0.32 ± 0.05, p < 0.001). There was no significant difference between measurements of upslope index for the SMS and conventional sequences (0.11 ± 0.04 vs. 0.11 ± 0.03, p = 0.84)., Conclusion: SMS-bSSFP with multiband factor 3 and compressed sensing reconstruction enables cardiac MR perfusion imaging with three-fold increased spatial coverage and improved myocardial sharpness compared to a conventional sequence, without compromising perceived SNR, image quality, upslope index or number of diagnostic segments., (© 2022 The Authors. Magnetic Resonance in Medicine published by Wiley Periodicals LLC on behalf of International Society for Magnetic Resonance in Medicine.)

Published
2022
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38. Assessment of Myocardial Stiffness in Patients With Left Ventricular Hypertrophy: CMR Elastography Using Intrinsic Actuation.

Author

Burnhope E, Polcaro A, Runge JH, Granlund I, Bosio F, Troelstra MA, Villa ADM, Chiribiri A, Carr-White G, Webb J, Razavi R, Martorell J, Sinkus R, and Ismail TF

Subjects
Humans, Myocardium, Predictive Value of Tests, Ventricular Function, Left, Elasticity Imaging Techniques, Hypertrophy, Left Ventricular diagnostic imaging
Published
2022
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39. High-Resolution Free-Breathing Quantitative First-Pass Perfusion Cardiac MR Using Dual-Echo Dixon With Spatio-Temporal Acceleration.

Author

Tourais J, Scannell CM, Schneider T, Alskaf E, Crawley R, Bosio F, Sanchez-Gonzalez J, Doneva M, Schülke C, Meineke J, Keupp J, Smink J, Breeuwer M, Chiribiri A, Henningsson M, and Correia T

Abstract

Introduction: To develop and test the feasibility of free-breathing (FB), high-resolution quantitative first-pass perfusion cardiac MR (FPP-CMR) using dual-echo Dixon (FOSTERS; Fat-water separation for mOtion-corrected Spatio-TEmporally accelerated myocardial peRfuSion)., Materials and Methods: FOSTERS was performed in FB using a dual-saturation single-bolus acquisition with dual-echo Dixon and a dynamically variable Cartesian k-t undersampling (8-fold) approach, with low-rank and sparsity constrained reconstruction, to achieve high-resolution FPP-CMR images. FOSTERS also included automatic in-plane motion estimation and T 2 * correction to obtain quantitative myocardial blood flow (MBF) maps. High-resolution (1.6 x 1.6 mm 2 ) FB FOSTERS was evaluated in eleven patients, during rest, against standard-resolution (2.6 x 2.6 mm 2 ) 2-fold SENSE-accelerated breath-hold (BH) FPP-CMR. In addition, MBF was computed for FOSTERS and spatial wavelet-based compressed sensing (CS) reconstruction. Two cardiologists scored the image quality (IQ) of FOSTERS, CS, and standard BH FPP-CMR images using a 4-point scale (1-4, non-diagnostic - fully diagnostic)., Results: FOSTERS produced high-quality images without dark-rim and with reduced motion-related artifacts, using an 8x accelerated FB acquisition. FOSTERS and standard BH FPP-CMR exhibited excellent IQ with an average score of 3.5 ± 0.6 and 3.4 ± 0.6 (no statistical difference, p > 0.05), respectively. CS images exhibited severe artifacts and high levels of noise, resulting in an average IQ score of 2.9 ± 0.5. MBF values obtained with FOSTERS presented a lower variance than those obtained with CS., Discussion: FOSTERS enabled high-resolution FB FPP-CMR with MBF quantification. Combining motion correction with a low-rank and sparsity-constrained reconstruction results in excellent image quality., Competing Interests: JT, TS, JS-G, JS, and MB are Philips Healthcare employees. MD, CS, JM, and JK are employees of Philips Research Europe. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Tourais, Scannell, Schneider, Alskaf, Crawley, Bosio, Sanchez-Gonzalez, Doneva, Schülke, Meineke, Keupp, Smink, Breeuwer, Chiribiri, Henningsson and Correia.)

Published
2022
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40. Quantification of balanced SSFP myocardial perfusion imaging at 1.5 T: Impact of the reference image.

Author

McElroy S, Kunze KP, Milidonis X, Huang L, Nazir MS, Evans C, Bosio F, Mughal N, Masci PG, Neji R, Razavi R, Chiribiri A, and Roujol S

Subjects
Coronary Circulation, Humans, Magnetic Resonance Imaging, Reproducibility of Results, Coronary Artery Disease, Myocardial Perfusion Imaging
Abstract

Purpose: To investigate the use of a high flip-angle (HFA) balanced SSFP (bSSFP) reference image (in comparison to conventional proton density [PD]-weighted reference images) for conversion of bSSFP myocardial perfusion images into dynamic T 1 maps for improved myocardial blood flow (MBF) quantification at 1.5 T., Methods: The HFA-bSSFP (flip angle [FA] = 50°), PD gradient-echo (PD-GRE; FA = 5°), and PD-bSSFP (FA = 8°) reference images were acquired before a dual-sequence bSSFP perfusion acquisition. Simulations were used to study accuracy and precision of T 1 and MBF quantification using the three techniques. The accuracy and precision of T 1 , and the precision and intersegment variability of MBF were compared among the three techniques in 8 patients under rest conditions., Results: In simulations, HFA-bSSFP demonstrated improved T 1 /MBF precision (higher T 1 /MBF SD of 30%-80%/50%-100% and 30%-90%/60%-115% for PD-GRE and PD-bSSFP, respectively). Proton density-GRE and PD-bSSFP were more sensitive to effective FA than HFA-bSSFP (maximum T 1 /MBF errors of 13%/43%, 20%/43%, and 1%/3%, respectively). Sensitivity of all techniques (defined as T 1 /MBF errors) to native T 1 , native T 2 , and effective saturation efficiency were negligible (<1%/<1%), moderate (<14%/<19%), and high (<63%/<94%), respectively. In vivo, no difference in T 1 accuracy was observed among HFA-bSSFP, PD-GRE, and PD-bSSFP (-9 ± 44 ms vs -28 ± 55 ms vs -22 ± 71 ms, respectively; p > .08). The HFA-bSSFP led to improved T 1 /MBF precision (T 1 /MBF SD: 41 ± 19 ms/0.24 ± 0.08 mL/g/min vs PD-GRE: 48 ± 20 ms/0.29 ± 0.09 mL/g/min and PD-bSSFP: 59 ± 23 ms/0.33 ± 0.11 mL/g/min; p ≤ .02) and lower MBF intersegment variability (0.14 ± 0.09 mL/g/min vs PD-GRE: 0.21 ± 0.09 mL/g/min and PD-bSSFP: 0.20 ± 0.10 mL/g/min; p ≤ .046)., Conclusion: We have demonstrated the feasibility of using a HFA-bSSFP reference image for MBF quantification of bSSFP perfusion imaging at 1.5 T. Results from simulations demonstrate that the HFA-bSSFP reference image results in improved precision and reduced sensitivity to effective FA compared with conventional techniques using a PD reference image. Preliminary in vivo data acquired at rest also demonstrate improved precision and intersegment variability using the HFA-bSSFP technique compared with PD techniques; however, a clinical study in patients with coronary artery disease under stress conditions is required to determine the clinical significance of this finding., (© 2021 The Authors. Magnetic Resonance in Medicine published by Wiley Periodicals LLC on behalf of International Society for Magnetic Resonance in Medicine.)

Published
2022
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41. Efficient non-contrast enhanced 3D Cartesian cardiovascular magnetic resonance angiography of the thoracic aorta in 3 min.

Author

Fotaki A, Munoz C, Emanuel Y, Hua A, Bosio F, Kunze KP, Neji R, Masci PG, Botnar RM, and Prieto C

Subjects
Female, Heart, Humans, Imaging, Three-Dimensional, Predictive Value of Tests, Reproducibility of Results, Aorta, Thoracic diagnostic imaging, Magnetic Resonance Angiography
Abstract

Background: The application of cardiovascular magnetic resonance angiography (CMRA) for the assessment of thoracic aortic disease is often associated with prolonged and unpredictable acquisition times and residual motion artefacts. To overcome these limitations, we have integrated undersampled acquisition with image-based navigators and inline non-rigid motion correction to enable a free-breathing, contrast-free Cartesian CMRA framework for the visualization of the thoracic aorta in a short and predictable scan of 3 min., Methods: 35 patients with thoracic aortic disease (36 ± 13y, 14 female) were prospectively enrolled in this single-center study. The proposed 3D T2-prepared balanced steady state free precession (bSSFP) sequence with image-based navigator (iNAV) was compared to the clinical 3D T2-prepared bSSFP with diaphragmatic-navigator gating (dNAV), in terms of image acquisition time. Three cardiologists blinded to iNAV vs. dNAV acquisition, recorded image quality scores across four aortic segments and their overall diagnostic confidence. Contrast ratio (CR) and relative standard deviation (RSD) of signal intensity (SI) in the corresponding segments were estimated. Co-axial aortic dimensions in six landmarks were measured by two readers to evaluate the agreement between the two methods, along with inter-observer and intra-observer agreement. Kolmogorov-Smirnov test, Mann-Whitney U (MWU), Bland-Altman analysis (BAA), intraclass correlation coefficient (ICC) were used for statistical analysis., Results: The scan time for the iNAV-based approach was significantly shorter (3.1 ± 0.5 min vs. 12.0 ± 3.0 min for dNAV, P = 0.005). Reconstruction was performed inline in 3.0 ± 0.3 min. Diagnostic confidence was similar for the proposed iNAV versus dNAV for all three reviewers (Reviewer 1: 3.9 ± 0.3 vs. 3.8 ± 0.4, P = 0.7; Reviewer 2: 4.0 ± 0.2 vs. 3.9 ± 0.3, P = 0.4; Reviewer 3: 3.8 ± 0.4 vs. 3.7 ± 0.6, P = 0.3). The proposed method yielded higher image quality scores in terms of artefacts from respiratory motion, and non-diagnostic images due to signal inhomogeneity were observed less frequently. While the dNAV approach outperformed the iNAV method in the CR assessment, the iNAV sequence showed improved signal homogeneity along the entire thoracic aorta [RSD SI 5.1 (4.4, 6.5) vs. 6.5 (4.6, 8.6), P = 0.002]. BAA showed a mean difference of < 0.05 cm across the 6 landmarks between the two datasets. ICC showed excellent inter- and intra-observer reproducibility., Conclusions: Thoracic aortic iNAV-based CMRA with fast acquisition (~ 3 min) and inline reconstruction (3 min) is proposed, resulting in high diagnostic confidence and reproducible aortic measurements., (© 2021. The Author(s).)

Published
2022
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42. FASt single-breathhold 2D multislice myocardial T 1 mapping (FAST1) at 1.5T for full left ventricular coverage in three breathholds.

Author

Huang L, Neji R, Nazir MS, Whitaker J, Duong P, Reid F, Bosio F, Chiribiri A, Razavi R, and Roujol S

Subjects
Humans, Myocardium, Phantoms, Imaging, Prospective Studies, Reproducibility of Results, Heart, Magnetic Resonance Imaging
Abstract

Background: Conventional myocardial T 1 mapping techniques such as modified Look-Locker inversion recovery (MOLLI) generate one T 1 map per breathhold. T 1 mapping with full left ventricular coverage may be desirable when spatial T 1 variations are expected. This would require multiple breathholds, increasing patient discomfort and prolonging scan time., Purpose: To develop and characterize a novel FASt single-breathhold 2D multislice myocardial T 1 mapping (FAST1) technique for full left ventricular coverage., Study Type: Prospective., Population/phantom: Numerical simulation, agarose/NiCl 2 phantom, 9 healthy volunteers, and 17 patients., Field Strength/sequence: 1.5T/FAST1., Assessment: Two FAST1 approaches, FAST1-BS and FAST1-IR, were characterized and compared with standard 5-(3)-3 MOLLI in terms of accuracy, precision/spatial variability, and repeatability., Statistical Tests: Kruskal-Wallis, Wilcoxon signed rank tests, intraclass correlation coefficient analysis, analysis of variance, Student's t-tests, Pearson correlation analysis, and Bland-Altman analysis., Results: In simulation/phantom, FAST1-BS, FAST1-IR, and MOLLI had an accuracy (expressed as T 1 error) of 0.2%/4%, 6%/9%, and 4%/7%, respectively, while FAST1-BS and FAST1-IR had a precision penalty of 1.7/1.5 and 1.5/1.4 in comparison with MOLLI, respectively. In healthy volunteers, FAST1-BS/FAST1-IR/MOLLI led to different native myocardial T 1 times (1016 ± 27 msec/952 ±22 msec/987 ± 23 msec, P < 0.0001) and spatial variability (66 ± 10 msec/57 ± 8 msec/46 ± 7 msec, P < 0.001). There were no statistically significant differences between all techniques for T 1 repeatability (P = 0.18). In vivo native and postcontrast myocardial T 1 times in both healthy volunteers and patients using FAST1-BS/FAST1-IR were highly correlated with MOLLI (Pearson correlation coefficient ≥0.93)., Data Conclusion: FAST1 enables myocardial T 1 mapping with full left ventricular coverage in three separated breathholds. In comparison with MOLLI, FAST1 yield a 5-fold increase of spatial coverage, limited penalty of T 1 precision/spatial variability, no significant difference of T 1 repeatability, and highly correlated T 1 times. FAST1-IR provides improved T 1 precision/spatial variability but reduced accuracy when compared with FAST1-BS., Level of Evidence: 1 Technical Efficacy: Stage 3 J. Magn. Reson. Imaging 2020;51:492-504., (© 2019 The Authors. Journal of Magnetic Resonance Imaging published by Wiley Periodicals, Inc. on behalf of International Society for Magnetic Resonance in Medicine.)

Published
2020
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43. Fast myocardial T 1 mapping using shortened inversion recovery based schemes.

Author

Huang L, Neji R, Nazir MS, Whitaker J, Reid F, Bosio F, Chiribiri A, Razavi R, and Roujol S

Subjects
Computer Simulation, Female, Heart diagnostic imaging, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Prospective Studies, Reproducibility of Results, Time, Cardiomyopathies diagnostic imaging, Image Interpretation, Computer-Assisted methods
Abstract

Background: Myocardial T 1 mapping shows promise for assessment of cardiomyopathies. Most myocardial T 1 mapping techniques, such as modified Look-Locker inversion recovery (MOLLI), generate one T 1 map per breath-held acquisition (9-17 heartbeats), which prolongs multislice protocols and may be unsuitable for patients with breath-holding difficulties., Purpose: To develop and characterize novel shortened inversion recovery based T 1 mapping schemes of 2-5 heartbeats., Study Type: Prospective., Population/phantom: Numerical simulations, agarose/NiCl 2 phantom, 16 healthy volunteers, and 24 patients., Field Strength/sequence: 1.5T/MOLLI., Assessment: All shortened T 1 mapping schemes were characterized and compared with a conventional MOLLI scheme (5-(3)-3) in terms of accuracy, precision, spatial variability, and repeatability., Statistical Tests: Kruskal-Wallis, Wilcoxon rank sum tests, analysis of variance, Student's t-tests, Bland-Altman analysis, and Pearson correlation analysis., Results: All shortened schemes provided limited T 1 time variations (≤2% for T 1 times ≤1200 msec) and limited penalty of precision (by a factor of ~1.4-1.5) when compared with MOLLI in numerical simulations. In phantom, differences between all schemes in terms of accuracy, spatial variability, and repeatability did not reach statistical significance (P > 0.71). In healthy volunteers, there were no statistically significant differences between all schemes in terms of native T 1 times and repeatability for myocardium (P = 0.21 and P = 0.87, respectively) and blood (P = 0.79 and P = 0.41, respectively). All shortened schemes led to a limited increase of spatial variability for native myocardial T 1 mapping with respect to MOLLI (by a factor of 1.2) (P < 0.0001). In both healthy volunteers and patients, the two-heartbeat scheme and MOLLI led to highly linearly correlated T 1 times (correlation coefficients ≥0.83)., Data Conclusion: The proposed two-heartbeat T 1 mapping scheme yields a 5-fold acceleration compared with MOLLI, with highly linearly correlated T 1 times, no significant difference of repeatability, and limited spatial variability penalty at 1.5T. This approach may enable myocardial T 1 mapping in patients with severe breath-holding difficulties and reduce the examination time of multislice protocols., Level of Evidence: 1 Technical Efficacy Stage: 3 J. Magn. Reson. Imaging 2019;50:641-654., (© 2019 The Authors. Journal of Magnetic Resonance Imaging published by Wiley Periodicals, Inc. on behalf of International Society for Magnetic Resonance in Medicine.)

Published
2019
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44. Prognostic Value of Quantitative Stress Perfusion Cardiac Magnetic Resonance.

Author

Sammut EC, Villa ADM, Di Giovine G, Dancy L, Bosio F, Gibbs T, Jeyabraba S, Schwenke S, Williams SE, Marber M, Alfakih K, Ismail TF, Razavi R, and Chiribiri A

Subjects
Adult, Aged, Coronary Artery Disease mortality, Coronary Artery Disease physiopathology, Coronary Artery Disease therapy, Disease Progression, Female, Humans, Male, Middle Aged, Predictive Value of Tests, Prognosis, Risk Factors, Time Factors, Adenosine administration & dosage, Coronary Artery Disease diagnostic imaging, Coronary Circulation, Magnetic Resonance Imaging, Cine, Myocardial Perfusion Imaging methods, Vasodilator Agents administration & dosage
Abstract

Objectives: This study sought to evaluate the prognostic usefulness of visual and quantitative perfusion cardiac magnetic resonance (CMR) ischemic burden in an unselected group of patients and to assess the validity of consensus-based ischemic burden thresholds extrapolated from nuclear studies., Background: There are limited data on the prognostic value of assessing myocardial ischemic burden by CMR, and there are none using quantitative perfusion analysis., Methods: Patients with suspected coronary artery disease referred for adenosine-stress perfusion CMR were included (n = 395; 70% male; age 58 ± 13 years). The primary endpoint was a composite of cardiovascular death, nonfatal myocardial infarction, aborted sudden death, and revascularization after 90 days. Perfusion scans were assessed visually and with quantitative analysis. Cross-validated Cox regression analysis and net reclassification improvement were used to assess the incremental prognostic value of visual or quantitative perfusion analysis over a baseline clinical model, initially as continuous covariates, then using accepted thresholds of ≥2 segments or ≥10% myocardium., Results: After a median 460 days (interquartile range: 190 to 869 days) follow-up, 52 patients reached the primary endpoint. At 2 years, the addition of ischemic burden was found to increase prognostic value over a baseline model of age, sex, and late gadolinium enhancement (baseline model area under the curve [AUC]: 0.75; visual AUC: 0.84; quantitative AUC: 0.85). Dichotomized quantitative ischemic burden performed better than visual assessment (net reclassification improvement 0.043 vs. 0.003 against baseline model)., Conclusions: This study was the first to address the prognostic benefit of quantitative analysis of perfusion CMR and to support the use of consensus-based ischemic burden thresholds by perfusion CMR for prognostic evaluation of patients with suspected coronary artery disease. Quantitative analysis provided incremental prognostic value to visual assessment and established risk factors, potentially representing an important step forward in the translation of quantitative CMR perfusion analysis to the clinical setting., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2018
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45. Prevalence, treatment and outcome of patellar luxation in dogs in Italy. A retrospective multicentric study (2009-2014).

Author

Bosio F, Bufalari A, Peirone B, Petazzoni M, and Vezzoni A

Subjects
Animals, Dog Diseases epidemiology, Dogs, Italy, Joint Dislocations epidemiology, Joint Dislocations surgery, Patellar Dislocation epidemiology, Patellar Dislocation surgery, Prevalence, Retrospective Studies, Stifle surgery, Treatment Outcome, Dog Diseases surgery, Joint Dislocations veterinary, Patellar Dislocation veterinary, Stifle injuries
Abstract

Objective: To determine the prevalence of patellar luxation in dogs in Italy and its relation to signalment, the frequency and the type of postoperative complications and the outcome of treatment, and to compare the findings with those of other studies., Materials and Methods: The medical records from four referral clinics were searched for dogs with orthopaedic disorders referred from 2009 to 2014. From these data, the records of dogs with patellar luxation were identified, and the signalment, age and body weight, grade, side and direction of patellar luxation, treatment, postoperative complications, and outcome were retrieved. Univariate and multivariate statistical analyses were used to evaluate the data., Results: Of 8,694 canine orthopaedic cases, fractures not included, patellar luxation was diagnosed in 559 dogs (801 stifles). Mixed breed dogs were most commonly affected (18%), 85% of the luxations were medial, and 52% of the dogs were female. Of the 559 dogs examined, 400 (574 stifles) met the inclusion criteria for treatment evaluation. Minor complications occurred in five percent of the dogs, and major complications in 16%, including recurrence of patellar luxation in seven percent of the dogs. The outcome was good in 88% of stifles, fair in two percent, and poor in 10%., Clinical Significance: Although patellar luxation was more common in small breed dogs, it also was diagnosed in a significant number of large breed dogs, which included medial patellar luxation in 73% and lateral patellar luxation in 27% of stifles. Body weight and grade of luxation were the only variables statistically correlated with surgical complications.

Published
2017
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46. Mesenchymal stromal cells reset the scatter factor system and cytokine network in experimental kidney transplantation.

Author

Gregorini M, Bosio F, Rocca C, Corradetti V, Valsania T, Pattonieri EF, Esposito P, Bedino G, Collesi C, Libetta C, Frassoni F, Dal Canton A, and Rampino T

Subjects
Allografts, Animals, Cell Proliferation, Cytokines blood, Forkhead Transcription Factors metabolism, Hepatocyte Growth Factor blood, Hepatocyte Growth Factor genetics, Kidney Tubules pathology, Monocytes metabolism, Necrosis, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-met genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Rats, Inbred F344, Receptor Protein-Tyrosine Kinases genetics, Cytokines metabolism, Hepatocyte Growth Factor metabolism, Kidney Transplantation, Mesenchymal Stem Cells metabolism, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-met metabolism, Receptor Protein-Tyrosine Kinases metabolism
Abstract

Background: In former studies we showed in a rat model of renal transplantation that Mesenchymal Stromal Cells (MSC) prevent acute rejection in an independent way of their endowing in the graft. In this study we investigated whether MSC operate by resetting cytokine network and Scatter Factor systems, i.e. Hepatocyte Growth Factor (HGF), Macrophage Stimulating Protein (MSP) and their receptors Met and RON, respectively., Methods: MSC were injected into the renal artery soon after reperfusion. Controls were grafted untreated and normal rats. Rats were sacrificed 7 days after grafting. Serum and renal tissue levels of IFN-γ, IL-1, IL-2, IL-4, IL-6, IL-10, MSP/RON, HGF/Met systems, Treg lymphocytes were investigated., Results: In grafted untreated rats IFN-γ increased in serum and renal tissue and IL-6 rose in serum. MSC prevented both the phenomena, increased IL-10 serum levels and Treg number in the graft. Furthermore MSC increased serum and tissue HGF levels, Met tubular expression and prevented the suppression of tubular MSP/RON expression., Conclusions: Our results demonstrate that MSC modify cytokine network to a tolerogenic setting, they suppress Th1 cells, inactivate monocytes/macrophage, recruit Tregs. In addition, MSC sustain the expression of the Scatter Factor systems expression, i.e. systems that are committed to defend survival and stimulate regeneration of tubular cells.

Published
2014
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47. Toxoplasma gondii in sympatric wild herbivores and carnivores: epidemiology of infection in the Western Alps.

Author

Ferroglio E, Bosio F, Trisciuoglio A, and Zanet S

Subjects
Animals, Animals, Wild, DNA, Protozoan isolation & purification, Species Specificity, Deer, Foxes, Rupicapra, Sus scrofa, Toxoplasma isolation & purification, Toxoplasmosis, Animal epidemiology
Abstract

Background: Toxoplasma gondii is an apicomplexan parasite that is able to infect almost all warm blooded animals. In Europe, the domestic cat is the main definitive host. Worldwide, 6 billion people are infected with this parasite. The goal of our research is to evaluate the prevalence of T. gondii infection in wild animals from a previously unsampled area in Northern Italy where 0.1% of women seroconvert during pregnancy each year., Methods: We sampled and tested skeletal muscle and central nervous system tissue of 355 wild animals by PCR (n = 121 roe deer Capreolus capreolus, n = 105 wild boar Sus scrofa, n = 94 red fox Vulpes vulpes, n = 22 alpine chamois Rupicapra rupicapra, n = 13 red deer Cervus elaphus)., Results: The overall prevalence of infection with T. gondii was 10.99% (confidence interval (CI) 95% 8.14%-14.67%). A higher rate of infection was recorded in carnivores and omnivores (red fox 20.21%, CI 95% 13.34%-29.43%; wild boar 16.19%, CI 95% 10.36%-24.41%) compared to ruminants (2.48%, CI 95% 0.85%-7.04% in roe deer; 0.00%, CI 95% 0.00%-22.81% in red deer, and 0.00% alpine chamois (CI 95% 0.00%-14.87%) confirming the importance of tissue cysts in transmitting infection., Conclusions: The relatively high prevalence of T. gondii DNA in highly consumed game species (wild boar and roe deer) gives valuable insights into T. gondii epidemiology and may contribute to improve prevention and control of foodborne toxoplasmosis in humans.

Published
2014
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48. The role of therapeutic drug monitoring in the treatment of cytomegalovirus disease in kidney transplantation.

Author

Bedino G, Esposito P, Bosio F, Corradetti V, Valsania T, Rocca C, Pattonieri EF, Gregorini M, Rampino T, and Dal Canton A

Subjects
Cytomegalovirus genetics, Drug Resistance, Viral, Female, Humans, Middle Aged, Antiviral Agents administration & dosage, Cytomegalovirus Infections drug therapy, DNA, Viral blood, Drug Monitoring, Ganciclovir administration & dosage, Kidney Transplantation
Abstract

Cytomegalovirus (CMV) infection is a common complication following solid organ transplantation that may severely affect the outcome of transplantation. Ganciclovir (GCV) and its prodrug valganciclovir are successfully used to prevent and treat CMV infection; however, in a small percentage of patients, CMV gene mutations may lead to drug resistance. GCV resistance is defined as increasing CMV viremia or progressive clinical disease during prolonged antiviral therapy, due to CMV gene mutation. This has emerged as a new challenge, especially because alternative drugs such as cidofovir and foscarnet have a number of important side effects. Here we report the case of a kidney transplanted patient who experienced life-threatening CMV disease, which initially appeared to be GCV-resistant, but was instead found to be associated with inadequate antiviral drug levels. The patient was then successfully treated by monitoring plasma GCV levels. We suggest using plasma GCV monitoring in the management of all cases of critical CMV disease, in which GCV resistance is suspected.

Published
2013
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49. Antineutrophil cytoplasmic antibody-associated renal vasculitis treated with autologous mesenchymal stromal cells: evaluation of the contribution of immune-mediated mechanisms.

Author

Gregorini M, Maccario R, Avanzini MA, Corradetti V, Moretta A, Libetta C, Esposito P, Bosio F, Dal Canton A, and Rampino T

Subjects
Aged, Humans, Male, Transplantation, Autologous, Anti-Neutrophil Cytoplasmic Antibody-Associated Vasculitis surgery, Mesenchymal Stem Cell Transplantation methods
Abstract

We report the first case of renal antineutrophil cytoplasmic antibody (ANCA)-associated vasculitis treated with autologous mesenchymal stromal cells (MSCs). A 73-year-old man was admitted to the hospital for malaise, weight loss, and oliguria. His serum creatinine level was 2.7 mg/dL but it rapidly increased to 7.8 mg/dL; urinalysis showed proteinuria and hematuria, and the ANCA to myeloperoxidase with a perinuclear pattern (pANCA) titer was high (132 IU/mL). Renal biopsy showed necrotizing crescentic glomerulonephritis. Standard immunosuppressive therapy (cyclophosphamide and corticosteroids) was ineffective. Rituximab therapy was started, but it was discontinued after the third dose to minimize the risk of systemic spread of a severe oral Candida infection and to prevent superinfections that were facilitated by leukopenia. The patient received autologous MSCs, 1.5 × 10(6) cells/kg body weight, intravenously. After 7 days, his serum creatinine level decreased to 2.2 mg/dL, pANCA titer decreased to 75 IU/mL, and urinalysis findings normalized. Eight months later, he received a second MSC infusion because his serum creatinine level increased. In 1 week, his creatinine level decreased to 1.9 mg/dL and his pANCA titer decreased to 14 IU/mL. Immunosuppressive therapy was subsequently withdrawn. At the last follow-up visit, 12 months after the second MSC infusion, the patient remained in clinical remission without any therapy. Infusion of MSCs induced expansion of the T-lymphocyte subset expressing a regulatory T-cell phenotype (CD4(+)CD25(+)Foxp3(+)) and a notable reduction in interferon-γ, interleukin 6, and tumor necrosis factor serum levels., (Copyright © 2013 Mayo Foundation for Medical Education and Research. Published by Elsevier Inc. All rights reserved.)

Published
2013
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50. Multiple electrolyte disorders in a neurosurgical patient: solving the rebus.

Author

Corradetti V, Esposito P, Rampino T, Gregorini M, Libetta C, Bosio F, Valsania T, Pattonieri EF, Rocca C, Bianzina S, and Dal Canton A

Subjects
Aged, Humans, Hypokalemia complications, Hypokalemia diagnosis, Hyponatremia complications, Hyponatremia diagnosis, Male, Polydipsia complications, Polydipsia diagnosis, Polyuria complications, Water-Electrolyte Imbalance complications, Neurosurgical Procedures adverse effects, Polyuria diagnosis, Water-Electrolyte Imbalance diagnosis
Abstract

Background: It is important to ensure an adequate sodium and volume balance in neurosurgical patients in order to avoid the worsening of brain injury.Indeed, hyponatremia and polyuria, that are frequent in this patient population, are potentially harmful, especially if not promptly recognized.Differential diagnosis is often challenging, including disorders, which, in view of similar clinical pictures, present very different pathophysiological bases, such as syndrome of inappropriate antidiuresis, cerebral/renal salt wasting syndrome and diabetes insipidus., Case Presentation: Here we present the clinical report of a 67-year-old man with a recent episode of acute subarachnoid haemorrhage, admitted to our ward because of severe hyponatremia, hypokalemia and huge polyuria.We performed a complete workup to identify the underlying causes of these alterations and found a complex picture of salt wasting syndrome associated to primary polydipsia. The appropriate diagnosis allowed us to correct the patient hydro-electrolyte balance., Conclusion: The comprehension of the pathophysiological mechanisms is essential to adequately recognize and treat hydro-electrolyte disorders, also solving the most complex clinical problems.

Published
2013
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