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11. CKD LAB METHODS, PROGRESSION & RISK FACTORS 1

Author

Heisterkamp, M., primary, Titze, S., additional, Lorenzen, J., additional, Eckardt, K.-U., additional, Koettgen, A., additional, Kielstein, J. T., additional, Bouquegneau, A., additional, Vidal-Petiot, E., additional, Vrtovsnik, F., additional, Cavalier, E., additional, Krzesinski, J. M., additional, Flamant, M., additional, Delanaye, P., additional, Anguiano, L., additional, Riera, M., additional, Pascual, J., additional, Barrios, C., additional, Betriu, A., additional, Valdivielso, J. M., additional, Fernandez, E., additional, Soler, M. J., additional, Denys, M.-A., additional, Viaene, A., additional, Goessaert, A.-S., additional, Delanghe, J., additional, Everaert, K., additional, Kim, Y. S., additional, Choi, M. J., additional, Deok, J. Y., additional, Kim, S. G., additional, Bevc, S., additional, Hojs, N., additional, Hojs, R., additional, Ekart, R., additional, Gorenjak, M., additional, Puklavec, L., additional, Piskunowicz, M., additional, Hofmann, L., additional, Zurcher, E., additional, Bassi, I., additional, Zweiacker, C., additional, Stuber, M., additional, Narkiewicz, K., additional, Vogt, B., additional, Burnier, M., additional, Pruijm, M., additional, Rusu, E., additional, Zilisteanu, D., additional, Atasie, T., additional, Circiumaru, A., additional, Carstea, F., additional, Ecobici, M., additional, Rosca, M., additional, Tanase, C., additional, Mihai, S., additional, Voiculescu, M., additional, Jeon, Y. D., additional, Polenakovic, M., additional, Pop-Jordanova, N., additional, Hung, S.-C., additional, Tarng, D.-C., additional, Tuta, L., additional, Stanigut, A., additional, Mesiano, P., additional, Rollino, C., additional, Ferro, M., additional, Beltrame, G., additional, Massara, C., additional, Quattrocchio, G., additional, Borca, M., additional, Bazzan, M., additional, Roccatello, D., additional, Maksudova, A., additional, Urasaeva, L. I., additional, Khalfina, T. N., additional, Tekce, H., additional, Kin Tekce, B., additional, Aktas, G., additional, Alcelik, A., additional, Sengul, E., additional, Lindic, J., additional, Purg, D., additional, Skamen, J., additional, Krsnik, M., additional, Skoberne, A., additional, Pajek, J., additional, Kveder, R., additional, Bren, A., additional, Kovac, D., additional, Delgado, G., additional, Drechsler, C., additional, Wanner, C., additional, Blouin, K., additional, Pilz, S., additional, Tomaschitz, A., additional, Kleber, M. E., additional, Willmes, C., additional, Krane, V., additional, Marz, W., additional, Ritz, E., additional, Van Gilst, W. H., additional, Van Der Harst, P., additional, De Boer, R. A., additional, Scholze, A., additional, Petersen, L., additional, Hocher, B., additional, Rasmussen, L. M., additional, Tepel, M., additional, De Paula, E. A., additional, Vanelli, C. P., additional, Caminhas, M. S., additional, Soares, B. C., additional, Bassoli, F. A., additional, Da Costa, D. M. N., additional, Lanna, C. M. M., additional, Galil, A. G. S., additional, Colugnati, F. A. B., additional, Costa, M. B., additional, Bastos, M. G., additional, De Paula, R. B., additional, Santoro, D., additional, Zappulla, Z., additional, Alibrandi, A., additional, Tomasello Andulajevic, M., additional, Licari, M., additional, Baldari, S., additional, Buemi, M., additional, Cernaro, V., additional, Campenni, A., additional, Pallet, N., additional, Chauvet, S., additional, Levi, C., additional, Meas-Yedid, V., additional, Beaune, P., additional, Thevet, E., additional, Karras, A., additional, Santos, S., additional, Malheiro, J., additional, Campos, A., additional, Pedroso, S., additional, Santos, J., additional, Cabrita, A., additional, Mayor, M. M., additional, Ayala, R., additional, Ramos, C., additional, Franco, S., additional, Guillen, R., additional, Kim, J. S., additional, Yang, J. W., additional, Han, B. G., additional, Choi, S. O., additional, Tudor, M.-N., additional, Navajas Martinez, M. F., additional, Vaduva, C., additional, Maria, D. T., additional, Mota, E., additional, Clari, R., additional, Mongilardi, E., additional, Vigotti, F. N., additional, Consiglio, V., additional, Scognamiglio, S., additional, Nazha, M., additional, Roggero, S., additional, Piga, A., additional, Piccoli, G., additional, Mukhopadhyay, P., additional, Patar, K., additional, Chaterjee, N., additional, and Ganguly, K., additional

Published
2014
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13. Extracorporeal dialysis: techniques and adequacy - A

Author

Steckiph, D., primary, Calabrese, G., additional, Bertucci, A., additional, Mazzotta, A., additional, Vagelli, G., additional, Gonella, M., additional, Stamopoulos, D., additional, Manios, E., additional, Papachristos, N., additional, Grapsa, E., additional, Papageorgiou, G., additional, Gogola, V., additional, So, B., additional, Dey, V., additional, Spalding, E. M., additional, Libetta, C., additional, Esposito, P., additional, Margiotta, E., additional, Maffioli, P., additional, Bonaventura, A., additional, Bianchi, L., additional, Romano, D., additional, Rampino, T., additional, De Rosa, G., additional, Mauric, A., additional, Haug, U., additional, Enzinger, G., additional, Kern-Derstvenscheg, E., additional, Sluga, A., additional, Ausserwinkler, C., additional, Beck, W., additional, Rosenkranz, A. R., additional, Maheshwari, V., additional, Haroon, S., additional, Loy, Y., additional, Samavedham, L., additional, Rangaiah, G. P., additional, Lau, T., additional, Mpakirtzi, N., additional, Panagiotou, M., additional, Barbarousi, D., additional, Matsouka, C., additional, Bunani, A. D., additional, Kowalczyk, M., additional, Bartnicki, P., additional, Banach, M., additional, Rysz, J., additional, Lentini, P., additional, Zanoli, L., additional, Granata, A., additional, Contestabile, A., additional, Basso, A., additional, Berlingo, G., additional, Pellanda, V., additional, de Cal, M., additional, Grazia, V., additional, Clementi, A., additional, Insalaco, M., additional, Dell'Aquila, R., additional, Karkar, A., additional, Abdelrahman, M., additional, Martins, A. R., additional, Parreira, L., additional, Duque, A. S., additional, Rodrigues, I., additional, Baffoun, A. B., additional, Youssfi, M. A., additional, Sayeh, A., additional, Beji, M., additional, Ben Khadra, R., additional, Hmida, J., additional, Akazawa, M., additional, Horiuchi, H., additional, Hori, Y., additional, Yamada, A., additional, Satou, H., additional, Odamaki, S., additional, Nakai, S., additional, Satou, K., additional, Aoki, K., additional, Saito, I., additional, Kamijo, Y., additional, Ogata, S., additional, Ishibashi, Y., additional, Basso, F., additional, Wojewodzka-Zelezniakowicz, M., additional, Cruz, D., additional, Giuliani, A., additional, Blanca Martos, L., additional, Piccinni, P., additional, Ronco, C., additional, Potier, J., additional, Queffeulou, G., additional, Bouet, J., additional, Nilsson, A., additional, Sternby, J., additional, Grundstrom, G., additional, Alquist, M., additional, Ferraresi, M., additional, Di Vico, M. C., additional, Vigotti, F. N., additional, Deagostini, M., additional, Scognamiglio, S., additional, Consiglio, V., additional, Clari, R., additional, Moro, I., additional, Mongilardi, E., additional, Piccoli, G. B., additional, Hancock, V., additional, Huang, S., additional, Nilsson Ekdahl, K., additional, Steckiph, D., additional, Baldin, C., additional, Petrarulo, M., additional, Mancuso, D., additional, Inguaggiato, P., additional, Canepari, G., additional, Gigliola, G., additional, Ferrando, C., additional, Meinero, S., additional, Sicuso, C., additional, Pacitti, A., additional, Afentakis, N., additional, Tomo, T., additional, Matsuyama, K., additional, Nakata, T., additional, Ishida, K., additional, Takeno, T., additional, Kadota, J.-i., additional, Minakuchi, J., additional, Kastl, J., additional, Merello, M., additional, Boccato, C., additional, Giordana, G., additional, Mazzone, S., additional, Moscardo, V., additional, Reinhardt, B., additional, Knaup, R., additional, Kruger, W., additional, Tovbin, D., additional, Kim, S., additional, Avnon, L., additional, Zlotnik, M., additional, Storch, S., additional, Umimoto, K., additional, Shimamoto, Y., additional, Suyama, M., additional, Miyata, M., additional, Bosch Benitez-Parodi, E., additional, Baamonde Laborda, E. E., additional, Perez, G., additional, Ramirez, J. I., additional, Ramirez Puga, A., additional, Guerra, R., additional, Garcia Canton, C., additional, Lago Alonso, M. M., additional, Toledo, A., additional, Checa Andres, M. D., additional, Latif, F. E., additional, Mochida, Y., additional, Matsumoto, K., additional, Morita, K., additional, Tsutsumi, D., additional, Ishioka, K., additional, Maesato, K., additional, Oka, M., additional, Moriya, H., additional, Hidaka, S., additional, Ohtake, T., additional, Kobayashi, S., additional, Ficheux, A., additional, Gayrard, N., additional, Duranton, F., additional, Guzman, C., additional, Szwarc, I., additional, Bismuth-Mondolfo, J., additional, Brunet, P., additional, Servel, M.-F., additional, Argiles, A., additional, Tsikliras, N., additional, Mademtzoglou, S., additional, Balaskas, E., additional, Zeid, M., additional, Mostafa, A., additional, Mowafy, M. N., additional, Abdo, E. I., additional, Al Amin, O. M., additional, Ksiazek, A., additional, Zaluska, W., additional, Waniewski, J., additional, Debowska, M., additional, Wojcik-Zaluska, A., additional, Elias, M., additional, Francois, H., additional, Obada, E., additional, Lorenzo, H. K., additional, Charpentier, B., additional, Durrbach, A., additional, Beaudreuil, S., additional, Imamovic, G., additional, Marcelli, D., additional, Bayh, I., additional, Hrvacevic, R., additional, Kapun, S., additional, Grassmann, A., additional, Scatizzi, L., additional, Maslovaric, J., additional, Daelemans, R., additional, Mesens, S., additional, Mohamed, E. A., additional, Wafae, A., additional, Kawtar, H., additional, Mohamed Amine, H., additional, Driss, K., additional, and Mohammed, B., additional

Published
2013
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14. Lab methods / biomarkers

Author

Borras, M., primary, Roig, J., additional, Betriu, A., additional, Vilar, A., additional, Hernandez, M., additional, Martin, M., additional, Fernandez, E. D., additional, Dounousi, E., additional, Kiatou, V., additional, Papagianni, A., additional, Zikou, X., additional, Pappas, K., additional, Pappas, E., additional, Tatsioni, A., additional, Tsakiris, D., additional, Siamopoulos, K. C., additional, Kim, J.-K., additional, Kim, Y., additional, Kim, S. G., additional, Kim, H. J., additional, Ahn, S. Y., additional, Chin, H. J., additional, Oh, K.-H., additional, Ahn, C., additional, Chae, D.-W., additional, Yazici, R., additional, Altintepe, L., additional, Bakdik, S., additional, Guney, I., additional, Arslan, S., additional, Topal, M., additional, Karagoz, A., additional, Stefan, G., additional, Mircescu, G., additional, Capusa, C., additional, Stancu, S., additional, Petrescu, L., additional, Alecu, S., additional, Nedelcu, D., additional, Bennett, A. H. L., additional, Pham, H., additional, Garrity, M., additional, Magdeleyns, E., additional, Vermeer, C., additional, Zhang, M., additional, Ni, Z., additional, Zhu, M., additional, Yan, J., additional, Mou, S., additional, Wang, Q., additional, Qian, J., additional, Saade, A., additional, Karavetian, M., additional, ElZein, H., additional, de Vries, N., additional, de Haseth, D. E., additional, Lay Penne, E., additional, van Dam, B., additional, Bax, W. A., additional, Bots, M. L., additional, Grooteman, M. P. C., additional, van den Dorpel, R. A., additional, Blankenstijn, P. J., additional, Nube, M. J., additional, Wee, P. M., additional, Park, J. H., additional, Jo, Y.-I., additional, Lee, J. H., additional, Cianfrone, P., additional, Comi, N., additional, Lucisano, G., additional, Piraina, V., additional, Talarico, R., additional, Fuiano, G., additional, Toyonaga, M., additional, Fukami, K., additional, Yamagishi, S.-i., additional, Kaida, Y., additional, Nakayama, Y., additional, Ando, R., additional, Obara, N., additional, Ueda, S., additional, Okuda, S., additional, Granatova, J., additional, Havrda, M., additional, Hruskova, Z., additional, Tesar, V., additional, Viklicky, O., additional, Rysava, R., additional, Rychlik, I., additional, Kratka, K., additional, Honsova, E., additional, Vernerova, Z., additional, Maluskova, J., additional, Vranova, J., additional, Bolkova, M., additional, Borecka, K., additional, Benakova, H., additional, Zima, T., additional, Lu, K.-C., additional, Yang, H.-Y., additional, Su, S.-L., additional, Cao, Y.-H., additional, Lv, L.-L., additional, Liu, B.-C., additional, Zeng, R., additional, Gao, X.-F., additional, Deng, Y.-Y., additional, Boelaert, J., additional, t' Kindt, R., additional, Glorieux, G., additional, Schepers, E., additional, Jorge, L., additional, Neirynck, N., additional, Lynen, F., additional, Sandra, P., additional, Sandra, K., additional, Vanholder, R., additional, Yamamoto, T., additional, Nameta, M., additional, Yoshida, Y., additional, Uhlen, M., additional, Shi, Y., additional, Tang, J., additional, Zhang, J., additional, An, Y., additional, Liao, Y., additional, Li, Y., additional, Tao, Y., additional, Wang, L., additional, Koibuchi, K., additional, Tanaka, K., additional, Aoki, T., additional, Miyagi, M., additional, Sakai, K., additional, Aikawa, A., additional, Martins, A. R., additional, Branco, P. Q., additional, Serra, F. M., additional, Matias, P. J., additional, Lucas, C. P., additional, Adragao, T., additional, Duarte, J., additional, Oliveira, M. M., additional, Saraiva, A. M., additional, Barata, J. D., additional, Masola, V., additional, Zaza, G., additional, Granata, S., additional, Proglio, M., additional, Pontrelli, P., additional, Abaterusso, C., additional, Schena, F., additional, Gesualdo, L., additional, Gambaro, G., additional, Lupo, A., additional, Pruijm, M., additional, Hofmann, L., additional, Stuber, M., additional, Zweiacker, C., additional, Piskunowicz, M., additional, Muller, M.-E., additional, Vogt, B., additional, Burnier, M., additional, Togashi, N., additional, Yamashita, T., additional, Mita, T., additional, Ohnuma, Y., additional, Hasegawa, T., additional, Endo, T., additional, Tsuchida, A., additional, Ando, T., additional, Yoshida, H., additional, Miura, T., additional, Bevins, A., additional, Assi, L., additional, Ritchie, J., additional, Jesky, M., additional, Stringer, S., additional, Kalra, P., additional, Hutchison, C., additional, Harding, S., additional, Cockwell, P., additional, Viccica, G., additional, Cupisti, A., additional, Chiavistelli, S., additional, Borsari, S., additional, Pardi, E., additional, Centoni, R., additional, Fumagalli, G., additional, Cetani, F., additional, Marcocci, C., additional, Scully, P., additional, O'Flaherty, D., additional, Sankaralingam, A., additional, Hampson, G., additional, Goldsmith, D. J., additional, Pallet, N., additional, Chauvet, S., additional, Beaune, P., additional, Nochy, D., additional, Thervet, E., additional, Karras, A., additional, Bertho, G., additional, Gallyamov, M. G., additional, Saginova, E. A., additional, Severova, M. M., additional, Krasnova, T. N., additional, Kopylova, A. A., additional, Cho, E., additional, Jo, S.-K., additional, Kim, M.-G., additional, Cho, W.-Y., additional, kim, H. K., additional, Trivin, C., additional, Metzger, M., additional, Boffa, J.-J., additional, Vrtovsnik, F., additional, Houiller, P., additional, Haymann, J.-P., additional, Flamant, M., additional, Stengel, B., additional, Roozbeh, J., additional, Yavari, V., additional, Pakfetrat, M., additional, Zolghadr, A. A., additional, Kim, C. S., additional, Kim, M. J., additional, Kang, Y. U., additional, Choi, J. S., additional, Bae, E. H., additional, Ma, S. K., additional, Kim, S. W., additional, Lemoine, S., additional, Guebre-Egziabher, F., additional, Dubourg, L., additional, Hadj-Aissa, A., additional, Blumberg, S., additional, Katzir, Z., additional, Biro, A., additional, Cernes, R., additional, Barnea, Z., additional, Vasquez, D., additional, Gordillo, R., additional, Aller, C., additional, Fernandez, B., additional, Jabary, N., additional, Perez, V., additional, Mendiluce, A., additional, Bustamante, J., additional, Coca, A., additional, Goek, O.-N., additional, Sekula, P., additional, Prehn, C., additional, Meisinger, C., additional, Gieger, C., additional, Suhre, K., additional, Adamski, J., additional, Kastenmuller, G., additional, Kottgen, A., additional, Kuzniewski, M., additional, Fedak, D., additional, Dumnicka, P., additional, Solnica, B., additional, Kusnierz-Cabala, B., additional, Kapusta, M., additional, Sulowicz, W., additional, Drozdz, R., additional, Zawada, A. M., additional, Rogacev, K. S., additional, Hummel, B., additional, Fliser, D., additional, Geisel, J., additional, Heine, G. H., additional, Kretschmer, A., additional, Volsek, M., additional, Krahn, T., additional, Kolkhof, P., additional, Kribben, A., additional, Bruck, H., additional, Koh, E. S., additional, Chung, S., additional, Yoon, H. E., additional, Park, C. W., additional, Chang, Y. S., additional, Shin, S. J., additional, Deagostini, M. C., additional, Vigotti, F. N., additional, Ferraresi, M., additional, Consiglio, V., additional, Scognamiglio, S., additional, Moro, I., additional, Clari, R., additional, Daidola, G., additional, Versino, E., additional, Piccoli, G. B., additional, Mammadrahim Agayev, M., additional, Mehrali Mammadova, I., additional, Qarib Ismayilova, S., additional, Anguiano, L., additional, Riera, M., additional, Pascual, J., additional, Barrios, C., additional, Valdivielso, J. M., additional, Fernandez, E., additional, Soler, M. J., additional, Tsarpali, V., additional, Liakopoulos, V., additional, Panagopoulou, E., additional, Kapoukranidou, D., additional, Spaia, S., additional, Kostopoulou, M., additional, Michalaki, A., additional, Nikitidou, O., additional, Dombros, N., additional, Zhu, F., additional, Abba, S., additional, Flores-Gama, C., additional, Williams, C., additional, Cartagena, C., additional, Carter, M., additional, Kotanko, P., additional, Levin, N. W., additional, Kolesnyk, M., additional, Stepanova, N., additional, Driyanska, V., additional, Stashevska, N., additional, Kundin, V., additional, Shifris, I., additional, Dudar, I., additional, Zaporozhets, O., additional, Keda, T., additional, Ishchenko, M., additional, Khil, M., additional, Choe, J.-Y., additional, Nam, S.-A., additional, Kim, J., additional, Cha, J.-H., additional, Gliga, M. L., additional, Irimescu, C. G., additional, Caldararu, C. D., additional, Gliga, M. G., additional, Toma, L. V., additional, Gomotarceanu, A., additional, Park, Y., additional, Jeon, J., additional, Kwon, S. K., additional, Kim, S. J., additional, Kim, S. M., additional, Kim, H.-Y., additional, Montero, N., additional, Marquez, E., additional, Berrada, A., additional, Arias, C., additional, Prada, J. A., additional, Orfila, M. A., additional, Mojal, S., additional, Vilaplana, C., additional, Attini, R., additional, Parisi, S., additional, Fassio, F., additional, Ghiotto, S., additional, Biolcati, M., additional, Todros, T., additional, Jin, K., additional, Vaziri, N. D., additional, Tramonti, G., additional, Romiti, N., additional, Chieli, E., additional, Maksudova, A. N., additional, Khusnutdinova, L. A., additional, Reque, J. E., additional, Quiroga, B., additional, Lopez, J. M., additional, Verdallez, U. G., additional, Garcia de Vinuesa, M., additional, Goicoechea, M., additional, Nayara, P. G., additional, Arroyo, D. R., additional, Luno, J., additional, Tanaka, H., additional, Abbas, S. R., additional, Thijssen, S., additional, Berthoux, F. C., additional, Azzouz, L., additional, Afiani, A., additional, Ziane, A., additional, Mariat, C., additional, Fournier, H., additional, Kusztal, M., additional, Dzierzek, P., additional, Witkowski, G., additional, Nurzynski, M., additional, Golebiowski, T., additional, Weyde, W., additional, Klinger, M., additional, Altiparmak, M. R., additional, Seyahi, N., additional, Trabulus, S., additional, Bolayirli, M., additional, Andican, Z. G., additional, Suleymanlar, G., additional, Serdengecti, K., additional, Niculae, A., additional, Checherita, I.-A., additional, Neagoe, D.-N., additional, Ciocalteu, A., additional, Seiler, S., additional, Pickering, J. W., additional, Emrich, I., additional, Heine, G., additional, Bargnoux, A.-S., additional, Obiols, J., additional, Kuster, N., additional, Fessler, P., additional, Badiou, S., additional, Dupuy, A.-M., additional, Ribstein, J., additional, Cristol, J.-P., additional, Yanagisawa, N., additional, Ando, M., additional, Ajisawa, A., additional, Tsuchiya, K., additional, Nitta, K., additional, Bouquegneau, A., additional, Cavalier, E., additional, Krzesinski, J.-M., additional, Delanaye, P., additional, Tominaga, N., additional, Shibagaki, Y., additional, Kida, K., additional, Miyake, F., additional, Kimura, K., additional, Ayvazyan, A., additional, Rameev, V., additional, Kozlovskaya, L., additional, Simonyan, A., additional, Scholze, A., additional, Marckmann, P., additional, Tepel, M., additional, Rasmussen, L. M., additional, Hara, M., additional, Kanai, H., additional, Harada, K., additional, Tamura, Y., additional, Kawai, Y., additional, Al-Jebouri, M. M., additional, Madash, S. A., additional, Leonidovna Berezinets, O., additional, and Nicolaevich Rossolovskiy, A., additional

Published
2013
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15. Clinical Nephrology - Lab methods and other markers

Author

Kleophas, W., primary, Bieber, B., additional, Robinson, B., additional, Duttlinger, J., additional, Fliser, D., additional, Lonneman, G., additional, Rump, L., additional, Pisoni, R., additional, Port, F., additional, Reichel, H., additional, Daniela, R., additional, Ciocalteu, A., additional, Checherita, I. A., additional, Peride, I., additional, Spataru, D. M., additional, Niculae, A., additional, Laetitia, K., additional, Amna, K., additional, Laurence, D., additional, Aoumeur, H.-A., additional, Flamant, M., additional, Haymann, J.-P., additional, Letavernier, E., additional, Vidal-Petiot, E., additional, Boffa, J.-J., additional, Vrtovsnik, F., additional, Bianco, F., additional, Pessolano, G., additional, Carraro, M., additional, Panzetta, G. O., additional, Ebert, N., additional, Gaedeke, J., additional, Jakob, O., additional, Kuhlmann, M., additional, Martus, P., additional, Van der Giet, M., additional, Scha  ner, E., additional, Khan, I., additional, Law, Y., additional, Turgutalp, K., additional, Ozhan, O., additional, Gok Oguz, E., additional, Kiykim, A., additional, Donadio, C., additional, Hatmi, Z. N., additional, Mahdavi-Mazdeh, M., additional, Morales, E., additional, Gutierrez-Millet, V., additional, Rojas-Rivera, J., additional, Huerta, A., additional, Gutierrez, E., additional, Gutierrez-Solis, E., additional, Polanco, N., additional, Caro, J., additional, Gonza z, E., additional, Praga, M., additional, Marco Mayayo, M., additional, Valdivielso, J., additional, Marti  z, M., additional, Fernaez Giraez, E., additional, Obrador, G., additional, Olvera, N., additional, Ortiz de la Pe, D., additional, Gutie ez, V., additional, Villa, A., additional, Redal-Baigorri, B., additional, Sombolos, K., additional, Tsakiris, D., additional, Boletis, J., additional, Vlahakos, D., additional, Siamopoulos, K., additional, Vargiemezis, V., additional, Nikolaidis, P., additional, Iatrou, C., additional, Dafnis, E., additional, Argyropoulos, C., additional, Xynos, K., additional, Schock-Kusch, D., additional, Shulhevich, Y., additional, Geraci, S., additional, Hesser, J., additional, Stsepankou, D., additional, Neudecker, S., additional, Koenig, S., additional, Hoecklin, F., additional, Pill, J., additional, Gretz, N., additional, Schweda, F., additional, Schreiber, A., additional, Kudo, K., additional, Konta, T., additional, Choi, S. O., additional, Kim, J. S., additional, Kim, M. K., additional, Yang, J. W., additional, Han, B. G., additional, Delanaye, P., additional, Cavalier, E., additional, Masson, I., additional, Mehdi, M., additional, Nicolas, M., additional, Lambermont, B., additional, Dubois, B., additional, Damas, P., additional, Krzesinski, J.-M., additional, Morel, J., additional, Lautrette, A., additional, Christophe, M., additional, Gagneux-Brunon, A., additional, Anne, F., additional, Fre (C)ric, L., additional, Bevc, S., additional, Ekart, R., additional, Hojs, R., additional, Gorenjak, M., additional, Puklavec, L., additional, Hashimoto, N., additional, Suzuki, A., additional, Mitsumoto, K., additional, Shimizu, M., additional, Niihata, K., additional, Kawabata, A., additional, Sakaguchi, Y., additional, Hayashi, T., additional, Shoji, T., additional, Okada, N., additional, Tsubakihara, Y., additional, Hamano, T., additional, Nakano, C., additional, Fujii, N., additional, Obi, Y., additional, Mikami, S., additional, Inoue, K., additional, Matsui, I., additional, Isaka, Y., additional, Rakugi, H., additional, Edvardsson, V., additional, Siguron, B., additional, Thorsteinsdottir, M., additional, Palsson, R., additional, Matsumoto, J., additional, Miyazaki, N., additional, Murata, I., additional, Yoshida, G., additional, Morishita, K., additional, Ushikoshi, H., additional, Nishigaki, K., additional, Ogura, S., additional, Minatoguchi, S., additional, Werneke, U., additional, Ott, M., additional, Salander-Renberg, E., additional, Taylor, D., additional, Stegmayr, B., additional, Surel, S., additional, Wenzlova, M., additional, Silva Junior, G., additional, Vieira, A. P., additional, Couto Bem, A., additional, Alves, M., additional, Torres, A., additional, Meneses, G., additional, Martins, A., additional, Liborio, A., additional, Daher, E., additional, Gluhovschi, G., additional, Modilca, M., additional, Daminescu, L., additional, Gluhovschi, C., additional, Velciov, S., additional, Petrica, L., additional, Gadalean, F., additional, Balgradean, C., additional, Schmeiser, H. H., additional, Kolesnyk, M., additional, Stepanova, N., additional, Surzhko, L., additional, Stashevska, N., additional, Filiopoulos, V., additional, Hadjiyannakos, D., additional, Arvanitis, D., additional, Panagiotopoulos, K., additional, Vlassopoulos, D., additional, Kaesler, N., additional, Schettgen, T., additional, Magdeleyns, E., additional, Brandenburg, V., additional, Vermeer, C., additional, Floege, J., additional, Kr, T., additional, Randone, O., additional, Ferraresi, M., additional, Aroasio, E., additional, Depascale, A., additional, Scognamiglio, S., additional, Consiglio, V., additional, Piccoli, G. B., additional, Jensen, L. V., additional, Lizakowski, S., additional, Rutkowski, P., additional, Tylicki, L., additional, Renke, M., additional, Sulikowska, B., additional, Donderski, R., additional, Bednarski, R., additional, Heleniak, Z., additional, Przybylska, M., additional, Manitius, J., additional, Rutkowski, B., additional, Bobrova, L., additional, Kozlovskaya, N., additional, Kanayama, K., additional, Hasegawa, M., additional, Kitagawa, F., additional, Ishii, J., additional, Yuzawa, Y., additional, Tanaka, K., additional, Sakai, K., additional, Hara, S., additional, Suzuki, Y., additional, Tanaka, Y., additional, Aikawa, A., additional, Hinoshita, F., additional, Hamano, N., additional, Sasaki, E., additional, Kato, A., additional, Katsuki, T., additional, Katsuma, A., additional, Imai, E., additional, Shibata, M., additional, Tada, M., additional, Shimbo, T., additional, Kikuchi, Y., additional, Oka, S., additional, Muramatsu, T., additional, Yanagisawa, N., additional, Fukutake, K., additional, Yamamoto, Y., additional, Ajisawa, A., additional, Tsuchiya, K., additional, Nitta, K., additional, Ando, M., additional, Liang, X., additional, Wang, P., additional, Liu, Z., additional, Zhao, Z., additional, Luyckx, V., additional, Bowker, S., additional, Miekle, A., additional, Toth, E., additional, Heguilen, R., additional, Malvar, A., additional, Hermes, R., additional, Cohen, L., additional, Muguerza, G., additional, Lococo, B., additional, Bernasconi, A., additional, Loboda, O., additional, Dudar, I., additional, Krot, V., additional, Alekseeva, V., additional, Ichinose, M., additional, Sasagawa, N., additional, Toyama, K., additional, Saito, A., additional, Kayamori, Y., additional, Kang, D., additional, Kim, H. W., additional, Yoshioka, K., additional, Hara, M., additional, Ohashi, K., additional, Maksudova, A., additional, Khalfina, T., additional, Cuoghi, A., additional, Bellei, E., additional, Caiazzo, M., additional, Bergamini, S., additional, Palladino, G., additional, Monari, E., additional, Tomasi, A., additional, Loiacono, E., additional, Camilla, R., additional, Dapr, V., additional, Morando, L., additional, Gallo, R., additional, Peruzzi, L., additional, Conrieri, M., additional, Bianciotto, M., additional, Bosetti, F. M., additional, Coppo, R., additional, DI Lullo, L., additional, Floccari, F., additional, Rivera, R., additional, Granata, A., additional, Faiola, R., additional, Feliziani, C., additional, Villani, A., additional, Malaguti, M., additional, Santoboni, A., additional, Kyriaki, K., additional, Droulias, J., additional, Bogdanova, M., additional, Rameev, V. V., additional, Simonyan, A. H., additional, Kozlovskaya, L. V., additional, Altiparmak, M. R., additional, Trabulus, S., additional, Akalin, N., additional, Yalin, A. S., additional, Esenkaya, A., additional, Yalin, S. F., additional, Serdengeae(C), K., additional, Arita, D., additional, Cunha, T., additional, Perez, J., additional, Sakata, M., additional, Arita, L., additional, Nogueira, M., additional, Jara, Z., additional, Souza, N., additional, Casarini, D., additional, Metzger, M., additional, Vallet, M., additional, Karras, A., additional, Froissart, M., additional, Stengel, B., additional, Houillier, P., additional, Paul, K., additional, Kretzschmar, D., additional, Yilmaz, A., additional, Ba hlein, B., additional, Titze, S., additional, Figulla, H.-R., additional, Wolf, G., additional, Busch, M., additional, Korotchaeva, Y., additional, Gordovskaya, N., additional, Kozlovskaya, L., additional, Ng, K. P., additional, Sharma, P., additional, Stringer, S., additional, Jesky, M., additional, Dutton, M., additional, Ferro, C., additional, Cockwell, P., additional, Moon, S. J., additional, Lee, S. C., additional, Yoon, S. Y., additional, Lee, J. E., additional, Han, S. J., additional, Anna, B., additional, Kirsch, T., additional, Svjetlana, L., additional, Joon-Keun, P., additional, Jan, B., additional, Johanna, K., additional, Haller, H., additional, Haubitz, M., additional, Smirnov, A., additional, Kayukov, I., additional, Rafrafi, N., additional, Degtereva, O., additional, Dobronravov, V., additional, Koch, M., additional, Stefan, H., additional, Dika, G., additional, Antoine, M.-H., additional, Husson, C., additional, Kos, J., additional, Milic, M., additional, Fucek, M., additional, Cvoriocec, D., additional, Bourgeade, M.-F., additional, Nortier, J. L., additional, Jelakovic, B., additional, Nawal, E. H., additional, Naoufal, M., additional, Nabila, M., additional, Fadwa, E. M., additional, Salma, E. K., additional, Nisrine, B., additional, Mohamed, Z., additional, Guislaine, M., additional, Mohamed Gharbi, B., additional, Benyounes, R., additional, Sotila, G. G., additional, Sorin, R., additional, Irina Magdalena, D., additional, Roxana, C., additional, Claudia, R., additional, Correa Barcellos, F., additional, Hallal, P. H., additional, Bohlke, M., additional, Boscolo Del Vechio, F., additional, Reges, A., additional, Santos, I., additional, Mielke, G., additional, Fortes, M., additional, Antunez, B., additional, Laganovic, M., additional, Vukovic Lela, I., additional, Karanovic, S., additional, Seric, J., additional, Premuic, V., additional, Fitrek, M., additional, Fodor, L., additional, Meljkovic Vrkic, T., additional, Bansal, V., additional, Hoppensteadt, D., additional, and Fareed, J., additional

Published
2012
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22. Mailbag.

Author

Everett, Morris, Collura, Joe, Smith, Larry, Hagen, Ray, Jones, Preston Neal, Catt, George L., Plaxen, Barry, Cindrich, John "Drive.-In Jack", Bartoletti, Mario D., Marootian, Charles, Scognamiglio, S., Steelman, Nena, Hewus, Kevin, Milroy, Robert, Gray, William, Hudkins, Jim, Stahler, Earle E., Desiderio, Elio, and Schorr, Don

Abstract

Several letters to the editor are presented in response to topics in previous issues including the 50th Anniversary of the periodical "Classic Images," plans of Paramount and Universal to release DVDs as part of their 100th anniversaries and the 1935 film "Kind Lady," starring Aline MacMahon.

Published
2012

23. [Study of the descending phase of the aortic pressure curve. Possible applications to the monitoring of peripheral resistance and arterial compliance (author's transl)]

Author

Razzolini, Renato, Daliento, Luciano, Boffa, Giovanni, Corbara, F, Chioin, Raffaello, Stritoni, P, Scognamiglio, S, and Volta, Sd

Subjects
Evaluation Studies as Topic, Humans, Regression Analysis, Blood Pressure Determination, Vascular Resistance, Arteries, Cardiac Output, Mathematics, Monitoring, Physiologic
Abstract

In 21 patients aortic pressure was recorded just above the diaphragm. The curve after the dicrotic notch is an exponential function of the time, and it is possible to characterize it by a unique time-constant. This constnat is shown to depend on aortic compliance and peripheral resistance: as aortic compliance does not vary abruptly in physiological conditions, this allows monitoring of peripheral resistance by monitoring time constant. Mathematical bases of time constant and of the peripheral resistance are briefly discussed.

Published
1976

25. l1-Regularization in Portfolio Selection with Machine Learning

Author

Stefania Corsaro, Valentina De Simone, Zelda Marino, Salvatore Scognamiglio, Corsaro, S., De Simone, V., Marino, Z., and Scognamiglio, S.

Subjects
Split Bregman, General Mathematics, Computer Science (miscellaneous), Deep learning, norm, Engineering (miscellaneous), L, 1, Multi-period portfolio optimization, deep learning, multi-period portfolio optimization, l1-norm, split Bregman
Abstract

In this work, we investigate the application of Deep Learning in Portfolio selection in a Markowitz mean-variance framework. We refer to a l1 regularized multi-period model; the choice of the l1 norm aims at producing sparse solutions. A crucial issue is the choice of the regularization parameter, which must realize a trade-off between fidelity to data and regularization. We propose an algorithm based on neural networks for the automatic selection of the regularization parameter. Once the neural network training is completed, an estimate of the regularization parameter can be computed via forward propagation. Numerical experiments and comparisons performed on real data validate the approach.

Published
2022

26. Dal controllo dei traffici marittimi al potere politico: Achille Lauro e la gestione dell'amministrazione a Napoli nel dopoguerra

Author

Gianluca Luise, Scognamiglio S., and Luise, Gianluca

Abstract

Tra il 1952 ed il 1960, la vita politica e amministrativa a Napoli fu dominata dalla figura incontrastata di Achille Lauro e del movimento politico a lui collegato. Affermato e scaltro armatore, fu capace di sfruttare i punti deboli di un sistema di consenso quale era quello della DC nel Mezzogiorno. A capo di una solida realtà imprenditoriale collegata alle principali rotte mercantili del Mediterraneo e detentore di un patrimonio personale tra i più cospicui d’Italia, Lauro collegò affari e politica dando vita ad un sistema di potere di stampo clientelare che fortemente influenzò le origini e i successivi sviluppi della vita politica della Napoli repubblicana.

Published
2020

27. Andic soils and flow-like landslides: Cause–effect evidence from Italy

Author

Giuliano Langella, Domenico Calcaterra, Pierpaolo Moretti, Angelo Basile, Fabio Terribile, Michela Iamarino, Solange Scognamiglio, Simona Vingiani, Scognamiglio, S., Basile, A., Calcaterra, D., Iamarino, M., Langella, G., Moretti, P., Vingiani, S., and Terribile, F.

Subjects
010504 meteorology & atmospheric sciences, Cause effect, Andosols, Flow (psychology), rainfall-triggered landslides, Soil Science, Landslide, Soil science, Development, 010502 geochemistry & geophysics, complex mixtures, 01 natural sciences, debris flows, rainfall-triggered landslide, soil water retention, Soil water, debris flow, Environmental Chemistry, Environmental science, short-range ordered clay minerals, short-range ordered clay mineral, Andosol, 0105 earth and related environmental sciences, General Environmental Science
Abstract

Flow-like landslides are extremely hazardous phenomena that cause fatalities and damage to natural environments, such as loss of fertile soil cover and vegetation and damage to infrastructure. In the Campania region (southern Italy), previous studies have proved that the most catastrophic flow-like mass movements involve and evolve within a specific soil type: Andosols. Recent findings show that both Andosols and andic soils are widely diffused in the mountain ecosystems of Italy. In this framework, we aim to evaluate whether catastrophic flow-like landslides, historically recorded in Italy, took place where these soils are settled. Soils collected in 12 flow-like landslides that occurred in Italy in the last 70 years were investigated. Chemical, physical and hydrological properties of soil samples collected from the detachment areas under different environmental and geological settings were analysed. Soils showed evidences of the andosolization process that enabled their identification as andic soils. Topsoils were well developed, demonstrating low soil erosion in spite of the high-to-moderate slope steepness and the anthropic stress due to land management. High water-retention capacity, marked chemical and physical fertility, high organic carbon content and prevalent loamy texture are common properties of all the studied soils. Therefore, despite the lithological heterogeneity of the bedrock and other environmental factors, the 12 soils revealed considerably homogeneous properties. Our study suggests a direct relationship between flow-like mass movements and andic soils in the studied environments. These findings shed new light on the pedological similarity of the materials involved in flow-like landslides in Italy.

Published
2019
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28. From theory to the complex geospatial ground-truth of contaminated soils

Author

Simona Vingiani, Paola Adamo, Agrillo Antonietta, Angelo Basile, Roberto De Mascellis, Massimo Fagnano, Giuliano Langella, Piero Manna, Pierpaolo Moretti, Florindo Antonio Mileti, Solange Scognamiglio, Fabio Terribile, EGU General Assembly 2018 © Author(s) 2018. CC Attribution 4.0 license, Vingiani, S., Adamo, P., Agrillo, A., Basile, A., De Mascellis, R., Fagnano, M., Langella, G., Manna, P., Moretti, P., Mileti, F. A., Scognamiglio, S., and Terribile, F.

Subjects
contaminatio, XRF, Soil contamination, regulation, geospatial distributio
Abstract

Characterization and subsequent reclamation of contaminated sites require detailed knowledge of the geospatial distribution of contamination. In Italy, a potentially contaminated site is an area where the concentration of one or more contaminants in soils is above land-use legal limits (CSC according to Italian law 152/06). Four main phases have to be followed to assess contamination and then reclamation: 1) preliminary conceptual model, 2) characterization plan, 3) site specific risk analysis (by Risk-net software) setting the contamination threshold concentration (CSR), 4) assessment of contamination and therefore reclamation action by comparison between CSC and CSR. The geospatial distribution of contaminants is considered in the characterization plan. It is mandatory to sample at least three samples for each surveyed point (one sample in the 0 to 1 m depth, one sample in the capillary fringe zone and one in between). There aren’t clear indications on the sampling strategy and spatial density. According to Italian law (D.M. 471/99), it is usual to identify 5 to 15 sampling points for areas of 1 to 5 hectares. In this work we attempt to answer the question: “After more than a decade from the introduction of law 152/06 and considering the progress of scientific knowledge, are these soil sampling criteria suitable for assessing the spatial and volumetric distribution of site contamination? We considered the analytical and spatial dataset obtained from two rural and industrial potentially polluted sites of south Italy, formerly interested by past disposal of industrial sludge and wastes. In both sites results showed that: (i) the geospatial variability of contamination is always much more complex than expected and depends by the history of the contamination; (ii) the sampling of the first meter - as a single body - is not satisfactory because it does not take into account the real vertical distribution of pollutants and the soil stratigraphy (such as the presence of centimeter horizons). The work illustrates the use of proximal sensing sensors, such as EMI, ARP, portable gamma-ray spectrometers and portable XRFs to obtain detailed mappings for homogeneous areas identification, where to address subsequent pedological and chemical investigations. Moreover, the pedological observation - guided by these technologies - often provides essential information to understand the process of emplacement and possible migration of pollutants towards other environmental sectors. The applied integrated approach, which was found very relevant for the site characterization, can assume even greater importance in the subsequent phase of reclamation.

Published
2018

29. Claude-Marie Raudot: la difesa delle libertà locali nelle pagine del 'Correspondant' (1858-1870)

Author

GIURINTANO C., D'Agostino, G, Di Napoli, M, Guerrieri, S, Soddu, F., Agirreazkuenaga , J, Aglietti, M, Alibrandi, R, Ambrosino, G, Andrini, S., Astuto, G, Benussi, S, Bixio, A, Bonini, F, Calabrò, V, Cardia, M, Compagna, L, Del Cornò, A, De Nardi, L, De Salvo, P, Di Donato, F, Di Rienzo, E, Falaschi, P.L., Fazio, S, Ferrari, V, Ferrari Zumbini, R, Giurato, R, Giurintano, C, Grassi Orsini, F, Guccione, E, Guerra Medici, M.T, Isoni, A, Karvunaki, G, Lanchester, F, Lucarini, F, Marsala, R, Martucci, R, Massari, O, Melis, G, Meniconi, A, Meriggi, M, Morelli, M.T.A, Novarese, D, Pelleriti, E, Polsi, A, Povolo, C, Romano, A, Rossetto, L, Rossi, F, Scognamiglio, S, Scuccimarra, L, Senigaglia, C, Serra, T, Silvestrini, F, Soddu, F, Soffietti, I, Tabacchi, S, Tosatti, G, Trimarchi, C, Valle, R, Vallone, G, Zani, L, and GIURINTANO C.

Subjects
Claude-Marie Raudot, Correspondant, decentramento amministrativo, Settore SPS/02 - Storia Delle Dottrine Politiche
Abstract

L'articolo esamina il contributo del giurista Claude-Marie Raudot , deputato della Droite durante la Seconda Repubblica, al dibattuto sul decentramento, da lui condotto nelle pagine della rivista "Correspondant" con la competenza del giurista, ma anche con l’esperienza maturata come sindaco d’Avallon, nel cuore della Borgogna, durante gli anni della monarchia orleanista.

Published
2017

30. The role of antitissue transglutaminase assay for the diagnosis and monitoring of coeliac disease: A French-Italian multicentre study

Author

Tonutti E., Visentini D., Bizzaro N., Caradonna M., Cerni L., Villalta D., Tozzoli R. F Ferrara, M Barraco, E Migali, D Mariotti, G Danzi, ML Martino, M Danzi, M Baldassarre, G Di Bitonto, M Ciccarelli, D Riello, G Bertiato, G Pedicini, RC Bocchino, F Moccia, G Alessio, P Amboni, C Ottomano, U Volta, A Granito, N Carabellese, R Amato, G Aurnia, C Spagnulo, P Clemen, F Coppola, G Spagnoletti, M Spina, T Trigilia, F Branciforte, L Giancotti, M Apollini, B Malamisura, A Sofia, M Boffardi, F Antico, P Arigliano, G Marcer, E Sala, ML Grassi, G Giana, C Staffa, V Cova, M Martinelli, A Calabrò, D Renzi, D Nigro, D Macchia, M Manfredi, E Cammelli, G Castellucci, L Ferraro, L Marchetti, G Garelli, M Colombo, E Castellano, M Cingolani, A Sabatino, A Di Blasi, M Golato, A Carlucci, G Spagnuolo, G Trivisonno, V Castelli, S Babbini, V Marrè, G Meli, S Amoroso, M Montesanti, E Mei, S Armelloni, C Gerosa, C Marcellino, C Gallo, R Pozzoli, M Peracchi, MT Bardella, C Trovato, VS Arosio, R Malberti, F Rea, MR Di Domenico, A Sergio, P Iardino, V Formicola, G Tamburro, A Massari, M Cirella, E Rondinella, A Pignero, D Scognamiglio, S Spagnuolo, S Orefice, V Romano, B Pennucci, A Maglione, S Lavecchia, A Rubino, O Leone, N Cantieri, F Michelutti, G Guariso, D Basso, S Teresi, E Gucciardino, M Di Gregorio, MA Trippiedi, P Greco, R Guadagna, E Maltese, T Imbastaro, G Lombardi, A Rossi, E Savi, L Spada, D Villalta, G Tabellini, M Saccarola, P Palumbo, G Marinucci, PM Strappini, F Viola, M Barbato, Roma, N Bizzaro, P Pasini, F Minetti, M Scogna, M Vascotto, G Morgese, F Bascietto, P Cantelmi, F Bulacanti, D Bassetti, S Santer, D Prizzon, S Loperfido, S Martelossi, T Not, A Ventura, E Tonutti, D Visentini, S Finazzi, S Salvatore, GV Melzi d’Eril, D Wolf, M Montesanto, M Negri, MG Azzeni, R Giordano, M Farina, S Micieli, V Gouilleux, O Bandin, A Tridon, M Meyer, F Bienvenu, G Beaune, S Jego, M San Marco, D Bernard, J Sarles, J Sahel, D Carre, S Benzaken, JF Demarquay, C Johanet, JJ Baudon., Tonutti E., Visentini D., Bizzaro N., Caradonna M., Cerni L., Villalta D., Tozzoli R. F Ferrara, M Barraco, E Migali, D Mariotti, G Danzi, ML Martino, M Danzi, M Baldassarre, G Di Bitonto, M Ciccarelli, D Riello, G Bertiato, G Pedicini, RC Bocchino, F Moccia, G Alessio, P Amboni, C Ottomano, U Volta, A Granito, N Carabellese, R Amato, G Aurnia, C Spagnulo, P Clemen, F Coppola, G Spagnoletti, M Spina, T Trigilia, F Branciforte, L Giancotti, M Apollini, B Malamisura, A Sofia, M Boffardi, F Antico, P Arigliano, G Marcer, E Sala, ML Grassi, G Giana, C Staffa, V Cova, M Martinelli, A Calabrò, D Renzi, D Nigro, D Macchia, M Manfredi, E Cammelli, G Castellucci, L Ferraro, L Marchetti, G Garelli, M Colombo, E Castellano, M Cingolani, A Sabatino, A Di Blasi, M Golato, A Carlucci, G Spagnuolo, G Trivisonno, V Castelli, S Babbini, V Marrè, G Meli, S Amoroso, M Montesanti, E Mei, S Armelloni, C Gerosa, C Marcellino, C Gallo, R Pozzoli, M Peracchi, MT Bardella, C Trovato, VS Arosio, R Malberti, F Rea, MR Di Domenico, A Sergio, P Iardino, V Formicola, G Tamburro, A Massari, M Cirella, E Rondinella, A Pignero, D Scognamiglio, S Spagnuolo, S Orefice, V Romano, B Pennucci, A Maglione, S Lavecchia, A Rubino, O Leone, N Cantieri, F Michelutti, G Guariso, D Basso, S Teresi, E Gucciardino, M Di Gregorio, MA Trippiedi, P Greco, R Guadagna, E Maltese, T Imbastaro, G Lombardi, A Rossi, E Savi, L Spada, D Villalta, G Tabellini, M Saccarola, P Palumbo, G Marinucci, PM Strappini, F Viola, M Barbato, Roma, and N Bizzaro, P Pasini, F Minetti, M Scogna, M Vascotto, G Morgese, F Bascietto, P Cantelmi, F Bulacanti, D Bassetti, S Santer, D Prizzon, S Loperfido, S Martelossi, T Not, A Ventura, E Tonutti, D Visentini, S Finazzi, S Salvatore, GV Melzi d’Eril, D Wolf, M Montesanto, M Negri, MG Azzeni, R Giordano, M Farina, S Micieli, V Gouilleux, O Bandin, A Tridon, M Meyer, F Bienvenu, G Beaune, S Jego, M San Marco, D Bernard, J Sarles, J Sahel, D Carre, S Benzaken, JF Demarquay, C Johanet, JJ Baudon.

Subjects
Immunoglobulin A, Adult, Male, Adolescent, Tissue transglutaminase, Reproducibility of Result, Enzyme-Linked Immunosorbent Assay, Autoantigens, Sensitivity and Specificity, Coeliac disease, Pathology and Forensic Medicine, Serology, Antigen, Autoantigen, Immunopathology, Humans, Medicine, Age Factor, Child, Autoantibodies, Transglutaminases, biology, business.industry, Age Factors, Reproducibility of Results, Infant, Original Articles, General Medicine, Biomarker, medicine.disease, Autoantibodie, Celiac Disease, Child, Preschool, Immunoglobulin G, Immunology, biology.protein, Gluten free, Female, Antibody, business, Biomarkers, Human
Abstract

Aims: Tissue transglutaminase (tTG) was recently identified as the major autoantigen in coeliac disease. The aim of this multicentre study was to evaluate the impact of a new immunoenzymatic assay for the detection of IgA anti-tGT antibodies. Methods: Seventy four Italian and French clinical laboratories participated in this study; anti-tTG IgA with an enzyme linked immunosorbent assay (ELISA) method using guinea pig liver extract as the coating antigen, anti-endomysium IgA autoantibodies (EMA), and total serum IgA were determined in 7948 patients, 1162 of whom had coeliac disease (737 untreated cases and 425 on a gluten free diet). A proportion of the sera were then sent to a reference laboratory for anti-tTG retesting with an ELISA method using recombinant human tTG antigen. Results: Seven thousand four hundred and fifty eight (93.8%) sera were EMA/antiguinea pig tTG concordant (positive or negative); 490 (6.2%) were non-concordant. The sensitivity of EMA and antiguinea pig tTG in the 737 untreated patients with coeliac disease was 92.1% and 94.8%, respectively, and the specificity was 99.8% and 99.2%, respectively. Retesting of the discordant sera showed that of the 162 sera classified as EMA negative/antiguinea pig tTG positive, only 49 were positive for human recombinant anti-tTG, and that 39 of these were also EMA positive. Furthermore, of the 36 sera classified as EMA positive/antiguinea pig tTG negative, only two were confirmed as EMA positive. Conclusions: The antiguinea pig tTG assay is more sensitive but less specific than EMA, whereas the antihuman recombinant tTG assay is far more specific and just as sensitive as antiguinea pig tTG. Testing for EMA presents considerable interpretative problems and is difficult to standardise.

Published
2003

31. The impact of insularity on SARS-CoV-2 diffusion: Recapitulating three years of COVID-19 pandemic in the island of Sardinia.

Author

Grandi N, Cusano R, Piras G, Fiamma M, Monne MI, Fancello T, Milia J, Orrù S, Scognamiglio S, Serra C, Mameli G, Uzzau S, Orrù G, Palmas AD, Rubino S, and Tramontano E

Subjects
Humans, Italy epidemiology, Genetic Variation, High-Throughput Nucleotide Sequencing, Pneumonia, Viral epidemiology, Pneumonia, Viral virology, Betacoronavirus genetics, COVID-19 epidemiology, COVID-19 virology, SARS-CoV-2 genetics, Pandemics, Phylogeny, Genome, Viral
Abstract

Background: Italy has been the first European Country dealing with SARS-CoV-2, whose diffusion on the territory has not been homogeneous. Among Italian regions, Sardinia represented one of the lowest incidence areas, likely due to its insular nature. Despite this, the impact of insularity on SARS-CoV-2 genetic diversity has not been comprehensively described., Methods: In the present study, we performed the high throughput sequencing of 888 SARS-CoV-2 genomes collected in Sardinia during the first 23 months of pandemics. In addition, 1439 high-coverage SARS-CoV-2 genomes circulating in Sardinia along three years (December 2019 - January 2023) were downloaded from GISAID, for a total of 2327 viral sequences that were characterized in terms of phylogeny and genomic diversity., Results: Overall, COVID-19 pandemic in Sardinia showed substantial differences with respect to the national panorama, with additional peaks of infections and uncommon lineages that reflects the national and regional policies of re-opening and the subsequent touristic arrivals. Sardinia has been interested by the circulation of at least 87 SARS-CoV-2 lineages, including some that were poorly represented at national and European level, likely linked to multiple importation events. The relative frequency of Sardinian SARS-CoV-2 lineages has been compared to other Mediterranean Islands, revealing a unique composition., Conclusions: The genomic diversity of SARS-CoV-2 in Sardinia has been shaped by a complex interplay of insular geography, low population density, and touristic arrivals, leading on the one side to the importation of lineages remaining rare at the national level, and resulting on the other side in the delayed entry of otherwise common variants., Competing Interests: Declaration of Competing Interest The 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 Ltd.. All rights reserved.)

Published
2024
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32. New Thiazolidine-4-One Derivatives as SARS-CoV-2 Main Protease Inhibitors.

Author

Messore A, Malune P, Patacchini E, Madia VN, Ialongo D, Arpacioglu M, Albano A, Ruggieri G, Saccoliti F, Scipione L, Tramontano E, Canton S, Corona A, Scognamiglio S, Paulis A, Suleiman M, Al-Maqtari HM, Abid FMA, Kawsar SMA, Sankaranarayanan M, Di Santo R, Esposito F, and Costi R

Abstract

It has been more than four years since the first report of SARS-CoV-2, and humankind has experienced a pandemic with an unprecedented impact. Moreover, the new variants have made the situation even worse. Among viral enzymes, the SARS-CoV-2 main protease (M pro ) has been deemed a promising drug target vs. COVID-19. Indeed, M pro is a pivotal enzyme for viral replication, and it is highly conserved within coronaviruses. It showed a high extent of conservation of the protease residues essential to the enzymatic activity, emphasizing its potential as a drug target to develop wide-spectrum antiviral agents effective not only vs. SARS-CoV-2 variants but also against other coronaviruses. Even though the FDA-approved drug nirmatrelvir, a M pro inhibitor, has boosted the antiviral therapy for the treatment of COVID-19, the drug shows several drawbacks that hinder its clinical application. Herein, we report the synthesis of new thiazolidine-4-one derivatives endowed with inhibitory potencies in the micromolar range against SARS-CoV-2 M pro . In silico studies shed light on the key structural requirements responsible for binding to highly conserved enzymatic residues, showing that the thiazolidinone core acts as a mimetic of the Gln amino acid of the natural substrate and the central role of the nitro-substituted aromatic portion in establishing π-π stacking interactions with the catalytic His-41 residue.

Published
2024
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33. Restoration of norepinephrine release, cognitive performance, and dendritic spines by amphetamine in aged rat brain.

Author

Scognamiglio S, Aljohani YM, Olson TT, Forcelli PA, Dezfuli G, and Kellar KJ

Subjects
Rats, Animals, Norepinephrine pharmacology, Rats, Sprague-Dawley, Dendritic Spines metabolism, Cerebral Cortex metabolism, Receptors, N-Methyl-D-Aspartate metabolism, Hippocampus metabolism, Rats, Inbred F344, Glutamic Acid, Cognition, Amphetamine pharmacology, Central Nervous System Stimulants pharmacology
Abstract

Age-related dysfunctions in specific neurotransmitter systems likely play an important role in cognitive decline even in its most subtle forms. Therefore, preservation or improvement of cognition via augmentation of neurotransmission is a potential therapeutic strategy to prevent further cognitive deficits. Here we identified a particular neuronal vulnerability in the aged Fischer 344 rat brain, an animal model of neurocognitive aging. Specifically, we demonstrated a marked impairment in glutamate-stimulated release of norepinephrine (NE) in the hippocampus and cerebral cortex of aged rats, and established that this release was mediated by N-methyl-D-aspartate (NMDA) receptors. Further, we also demonstrated that this decrease in NE release is fully rescued by the psychostimulant drug amphetamine (AMPH). Moreover, we showed that AMPH increases dendritic spine maturation, and importantly shows preclinical efficacy in restoring memory deficits in the aged rat through its actions to potentiate NE neurotransmission at β-adrenergic receptors. Taken together, our results suggest that deficits in glutamate-stimulated release of NE may contribute to and possibly be a determinant of neuronal vulnerability underlying cognitive decline during aging, and that these deficits can be corrected with currently available drugs. Overall these studies suggest that repurposing of psychostimulants for age-associated cognitive deficits is a potential avenue to delay or prevent cognitive decline and/or frank dementia later in life., (© 2024 The Authors. Aging Cell published by Anatomical Society and John Wiley & Sons Ltd.)

Published
2024
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34. COVID-19 Genomic Surveillance in Bangui (Central African Republic) Reveals a Landscape of Circulating Variants Linked to Validated Antiviral Targets of SARS-CoV-2 Proteome.

Author

Vickos U, Camasta M, Grandi N, Scognamiglio S, Schindler T, Belizaire MRD, Lango-Yaya E, Koyaweda GW, Senzongo O, Pounguinza S, Estimé KKJF, N'yetobouko S, Gadia CLB, Feiganazoui DA, Le Faou A, Orsini M, Perno CF, Zinzula L, and Rafaï CD

Subjects
Humans, Proteome, Central African Republic epidemiology, Phylogeny, Genomics, Antiviral Agents, SARS-CoV-2 genetics, COVID-19 epidemiology
Abstract

Since its outbreak, Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) spread rapidly, causing the Coronavirus Disease 19 (COVID-19) pandemic. Even with the vaccines' administration, the virus continued to circulate due to inequal access to prevention and therapeutic measures in African countries. Information about COVID-19 in Africa has been limited and contradictory, and thus regional studies are important. On this premise, we conducted a genomic surveillance study about COVID-19 lineages circulating in Bangui, Central African Republic (CAR). We collected 2687 nasopharyngeal samples at four checkpoints in Bangui from 2 to 22 July 2021. Fifty-three samples tested positive for SARS-CoV-2, and viral genomes were sequenced to look for the presence of different viral strains. We performed phylogenetic analysis and described the lineage landscape of SARS-CoV-2 circulating in the CAR along 15 months of pandemics and in Africa during the study period, finding the Delta variant as the predominant Variant of Concern (VoC). The deduced aminoacidic sequences of structural and non-structural genes were determined and compared to reference and reported isolates from Africa. Despite the limited number of positive samples obtained, this study provides valuable information about COVID-19 evolution at the regional level and allows for a better understanding of SARS-CoV-2 circulation in the CAR.

Published
2023
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35. Broad-spectrum coronavirus 3C-like protease peptidomimetic inhibitors effectively block SARS-CoV-2 replication in cells: Design, synthesis, biological evaluation, and X-ray structure determination.

Author

Stefanelli I, Corona A, Cerchia C, Cassese E, Improta S, Costanzi E, Pelliccia S, Morasso S, Esposito F, Paulis A, Scognamiglio S, Di Leva FS, Storici P, Brindisi M, Tramontano E, Cannalire R, and Summa V

Subjects
Humans, SARS-CoV-2, Protease Inhibitors chemistry, X-Rays, Peptide Hydrolases, Antiviral Agents chemistry, Peptidomimetics pharmacology, Peptidomimetics chemistry, COVID-19, Middle East Respiratory Syndrome Coronavirus
Abstract

Despite the approval of vaccines, monoclonal antibodies and restrictions during the pandemic, the demand for new efficacious and safe antivirals is compelling to boost the therapeutic arsenal against the COVID-19. The viral 3-chymotrypsin-like protease (3CL pro ) is an essential enzyme for replication with high homology in the active site across CoVs and variants showing an almost unique specificity for Leu-Gln as P2-P1 residues, allowing the development of broad-spectrum inhibitors. The design, synthesis, biological activity, and cocrystal structural information of newly conceived peptidomimetic covalent reversible inhibitors are herein described. The inhibitors display an aldehyde warhead, a Gln mimetic at P1 and modified P2-P3 residues. Particularly, functionalized proline residues were inserted at P2 to stabilize the β-turn like bioactive conformation, modulating the affinity. The most potent compounds displayed low/sub-nM potency against the 3CL pro of SARS-CoV-2 and MERS-CoV and inhibited viral replication of three human CoVs, i.e. SARS-CoV-2, MERS-CoV, and HCoV 229 in different cell lines. Particularly, derivative 12 exhibited nM-low μM antiviral activity depending on the virus, and the highest selectivity index. Some compounds were co-crystallized with SARS-CoV-2 3CL pro validating our design. Altogether, these results foster future work toward broad-spectrum 3CL pro inhibitors to challenge CoVs related pandemics., Competing Interests: Declaration of competing interest The 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 © 2023 Elsevier Masson SAS. All rights reserved.)

Published
2023
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36. Human Endogenous Retrovirus (HERV) Transcriptome Is Dynamically Modulated during SARS-CoV-2 Infection and Allows Discrimination of COVID-19 Clinical Stages.

Author

Grandi N, Erbì MC, Scognamiglio S, and Tramontano E

Subjects
Humans, Transcriptome, Leukocytes, Mononuclear, Convalescence, SARS-CoV-2 genetics, Endogenous Retroviruses genetics, COVID-19 genetics
Abstract

SARS-CoV-2 infection is known to trigger an important inflammatory response, which has a major role in COVID-19 pathogenesis. In infectious and inflammatory contexts, the modulation of human endogenous retroviruses (HERV) has been broadly reported, being able to further sustain innate immune responses due to the expression of immunogenic viral transcripts, including double-stranded DNA (dsRNA), and eventually, immunogenic proteins. To gain insights on this poorly characterized interplay, we performed a high-throughput expression analysis of ~3,300 specific HERV loci in the peripheral blood mononuclear cells (PBMCs) of 10 healthy controls and 16 individuals being either convalescent after the infection (6) or retesting positive after convalescence (10) (Gene Expression Onmibus [GEO] data set GSE166253). Results showed that the exposure to SARS-CoV-2 infection modulates HERV expression according to the disease stage and reflecting COVID-19 immune signatures. The differential expression analysis between healthy control (HC) and COVID-19 patients allowed us to identify a total of 282 differentially expressed HERV loci (deHERV) in the individuals exposed to SARS-CoV-2 infection, independently from the clinical form. In addition, 278 and 60 deHERV loci that were specifically modulated in individuals convalescent after COVID19 infection (C) and patients that retested positive to SARS-CoV-2 after convalescence (RTP) as individually compared to HC, respectively, as well as 164 deHERV loci between C and RTP patients were identified. The identified HERV loci belonged to 36 different HERV groups, including members of all three classes. The present study provides an exhaustive picture of the HERV transcriptome in PBMCs and its dynamic variation in the presence of COVID-19, revealing specific modulation patterns according to the infection stage that can be relevant to the disease clinical manifestation and outcome. IMPORTANCE We report here the first high-throughput analysis of HERV loci expression along SARS-CoV-2 infection, as performed with peripheral blood mononuclear cells (PBMCs). Such cells are not directly infected by the virus but have a crucial role in the plethora of inflammatory and immune events that constitute a major hallmark of COVID-19 pathogenesis. Results provide a novel and exhaustive picture of HERV expression in PBMCs, revealing specific modulation patterns according to the disease condition and the concomitant immune activation. To our knowledge, this is the first set of deHERVs whose expression is dynamically modulated across COVID-19 stages, confirming a tight interplay between HERV and cellular immunity and revealing specific transcriptional signatures that can have an impact on the disease clinical manifestation and outcome.

Published
2023
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37. Identification, comprehensive characterization, and comparative genomics of the HERV-K(HML8) integrations in the human genome.

Author

Scognamiglio S, Grandi N, Pessiu E, and Tramontano E

Abstract

Around 8% of the human genome is composed by Human Endogenous Retroviruses (HERVs), ancient viral sequences inherited from the primate germ line after their infection by now extinct retroviruses. Given the still underexplored physiological and pathological roles of HERVs, it is fundamental to increase our information about the genomic composition of the different groups, to lay reliable foundation for functional studies. Among HERVs, the most characterized elements belong to the beta-like superfamily HERV-K, comprising 10 groups (HML1-10) with HML2 being the most recent and studied one. Among HMLs, the HML8 group is the only one still lacking a comprehensive genomic description. In the present work, we investigated HML8 sequences' distribution in the human genome (GRCh38/hg38), identifying 23 novel proviruses and characterizing the overall 78 HML8 proviruses in terms of genome structure, phylogeny, and integration pattern. HML8 elements were significantly enriched in human chromosomes 8 and X (p<0.005) while chromosomes 17 and 20 showed fewer integrations than expected (p<0.025 and p<0.005, respectively). Phylogenetic analyses classified HML8 members into 3 clusters, corresponding to the three LTR types MER11A, MER11B and MER11C. Besides different LTR types, common signatures in the internal structure suggested the potential existence of three different ancestral HML8 variants. Accordingly, time of integration estimation coupled with comparative genomics revealed that these three clusters have a different time of integration in the primates' genome, with MER11C elements being significantly younger than MER11A- and MER11B associated proviruses (p<0.005 and p<0.05, respectively). Approximately 30% of the HML8 elements were found co-localized within human genes, sometimes in exonic portions and with the same orientation, deserving further studies for their possible effects on gene expression. Overall, we provide the first detailed picture of the HML8 group distribution and variety among the genome, creating the backbone for the specific analysis of their transcriptional activity in healthy and diseased conditions., Competing Interests: Declaration of Competing Interest The 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 © 2022 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2023
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38. HERV-K(HML7) Integrations in the Human Genome: Comprehensive Characterization and Comparative Analysis in Non-Human Primates.

Author

Grandi N, Pisano MP, Pessiu E, Scognamiglio S, and Tramontano E

Abstract

Endogenous Retroviruses (ERVs) are ancient relics of infections that affected the primate germ line and constitute about 8% of our genome. Growing evidence indicates that ERVs had a major role in vertebrate evolution, being occasionally domesticated by the host physiology. In addition, human ERV (HERV) expression is highly investigated for a possible pathological role, even if no clear associations have been reported yet. In fact, on the one side, the study of HERV expression in high-throughput data is a powerful and promising tool to assess their actual dysregulation in diseased conditions; but, on the other side, the poor knowledge about the various HERV group genomic diversity and individual members somehow prevented the association between specific HERV loci and a given molecular mechanism of pathogenesis. The present study is focused on the HERV-K(HML7) group that-differently from the other HERV-K members-still remains poorly characterized. Starting from an initial identification performed with the software RetroTector, we collected 23 HML7 proviral insertions and about 160 HML7 solitary LTRs that were analyzed in terms of genomic distribution, revealing a significant enrichment in chromosome X and the frequent localization within human gene introns as well as in pericentromeric and centromeric regions. Phylogenetic analyses showed that HML7 members form a monophyletic group, which based on age estimation and comparative localization in non-human primates had its major diffusion between 20 and 30 million years ago. Structural characterization revealed that besides 3 complete HML7 proviruses, the other group members shared a highly defective structure that, however, still presents recognizable functional domains, making it worth further investigation in the human population to assess the presence of residual coding potential.

Published
2021
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39. Comprehensive Analysis of HERV Transcriptome in HIV+ Cells: Absence of HML2 Activation and General Downregulation of Individual HERV Loci.

Author

Grandi N, Pisano MP, Scognamiglio S, Pessiu E, and Tramontano E

Subjects
Computational Biology methods, Humans, Software, T-Lymphocytes metabolism, T-Lymphocytes virology, Transcriptional Activation, Transcriptome, Endogenous Retroviruses genetics, Gene Expression Regulation, Viral, Genetic Loci, HIV Infections virology, HIV-1 physiology, Proviruses genetics
Abstract

Human endogenous retrovirus (HERV) expression is currently studied for its possible activation by HIV infection. In this context, the HERV-K(HML2) group is the most investigated: it has been proposed that HIV-1 infection can prompt HML2 transcription, and that HML2 proteins can affect HIV-1 replication, either complementing HIV or possibly influencing antiretroviral therapy. However, little information is available on the expression of other HERV groups in HIV infection. In the present study, we used a bioinformatics pipeline to investigate the transcriptional modulation of approximately 3250 well-characterized HERV loci, comparing their expression in a public RNA-seq profile, including a HIV-1-infected and a control T cell culture. In our pilot study, we found approximately 200 HERV loci belonging to 35 HERV groups that were expressed in one or both conditions, with transcripts per million (TPM) values from 1 to >500. Intriguingly, HML2 elements constituted only the 3% of expressed HERV loci, and in most cases (160) HERV expression was downregulated in the HIV-infected culture, showing from a 1- to 14-fold decrease as compared to uninfected cells. HERV transcriptome has been inferred de novo and employed to predict a total of about 950 HERV open reading frames (ORFs). These have been validated according to the coding potential and estimated abundance of the corresponding transcripts, leading to a set of 57 putative proteins potentially encoded by 23 HERV loci. Analysis showed that some individual loci have a coding potential that deserves further investigation. Among them, a HML6 provirus at locus 19q13.43 was predicted to produce a transcript showing the highest TPM among HERV-derived transcripts, being upregulated in HIV+ cells and inferred to produce Gag and Env puteins with possible biological activity.

Published
2020
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40. Reversal of Cognitive Impairment in gp120 Transgenic Mice by the Removal of the p75 Neurotrophin Receptor.

Author

Speidell A, Asuni GP, Avdoshina V, Scognamiglio S, Forcelli P, and Mocchetti I

Abstract

Activation of the p75 neurotrophin receptor (p75NTR), by the proneurotrophin brain-derived neurotrophic factor (proBDNF), triggers loss of synapses and promotes neuronal death. These pathological features are also caused by the human immunodeficiency virus-1 (HIV) envelope protein gp120, which increases the levels of proBDNF. To establish whether p75NTR plays a role in gp120-mediated neurite pruning, we exposed primary cultures of cortical neurons from p75NTR -/- mice to gp120. We found that the lack of p75NTR expression significantly reduced gp120-mediated neuronal cell death. To determine whether knocking down p75NTR is neuroprotective in vivo , we intercrossed gp120 transgenic (tg) mice with p75NTR heterozygous mice to obtain gp120tg mice lacking one or two p75NTR alleles. The removal of p75NTR alleles inhibited gp120-mediated decrease of excitatory synapses in the hippocampus, as measured by the levels of PSD95 and subunits of the N -methyl-D-Aspartate receptor in synaptosomes. Moreover, the deletion of only one copy of the p75NTR gene was sufficient to restore the cognitive impairment observed in gp120tg mice. Our data suggest that activation of p75NTR is one of the mechanisms crucial for the neurotoxic effect of gp120. These data indicate that p75NTR antagonists could provide an adjunct therapy against synaptic simplification caused by HIV.

Published
2019
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41. Weight Loss in Advanced Chronic Kidney Disease: Should We Consider Individualised, Qualitative, ad Libitum Diets? A Narrative Review and Case Study.

Author

Capizzi I, Teta L, Vigotti FN, Tognarelli G, Consiglio V, Scognamiglio S, and Piccoli GB

Subjects
Aged, Body Mass Index, Clinical Decision-Making, Counseling, Humans, Male, Obesity complications, Obesity diagnosis, Obesity physiopathology, Patient Selection, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic diagnosis, Renal Insufficiency, Chronic physiopathology, Time Factors, Treatment Outcome, Waiting Lists, Caloric Restriction, Diet, Protein-Restricted, Kidney Transplantation, Nutritional Status, Obesity diet therapy, Renal Dialysis, Renal Insufficiency, Chronic therapy, Weight Loss
Abstract

In advanced chronic kidney disease, obesity may bring a survival advantage, but many transplant centres demand weight loss before wait-listing for kidney graft. The case here described regards a 71-year-old man, with obesity-related glomerulopathy; referral data were: weight 110 kg, Body Mass Index (BMI) 37 kg/m², serum creatinine (sCr) 5 mg/dL, estimated glomerular filtration rate (eGFR) 23 mL/min, blood urea nitrogen (BUN) 75 mg/dL, proteinuria 2.3 g/day. A moderately restricted, low-protein diet allowed reduction in BUN (45-55 mg/dL) and good metabolic and kidney function stability, with a weight increase of 6 kg. Therefore, he asked to be enrolled in a weight-loss program to be wait-listed (the two nearest transplant centres required a BMI below 30 or 35 kg/m²). Since previous low-calorie diets were not successful and he was against a surgical approach, we chose a qualitative, ad libitum coach-assisted diet, freely available in our unit. In the first phase, the diet is dissociated; he lost 16 kg in 2 months, without need for dialysis. In the second maintenance phase, in which foods are progressively combined, he lost 4 kg in 5 months, allowing wait-listing. Dialysis started one year later, and was followed by weight gain of about 5 kg. He resumed the maintenance diet, and his current body weight, 35 months after the start of the diet, is 94 kg, with a BMI of 31.7 kg/m², without clinical or biochemical signs of malnutrition. This case suggests that our patients can benefit from the same options available to non-CKD (chronic kidney disease) individuals, provided that strict multidisciplinary surveillance is assured., Competing Interests: Luigi Teta works for as consultant for the Bioimis Accademia Alimentatre; Irene Capizzi received and unrestricted grant from the Bioimis Accademia Alimentare, through the University of Torino, under the responsibility of Giorgina B Piccoli. None of the other Authors had any conflict of interst.

Published
2017
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42. Diet as a system: an observational study investigating a multi-choice system of moderately restricted low-protein diets.

Author

Piccoli GB, Nazha M, Capizzi I, Vigotti FN, Scognamiglio S, Consiglio V, Mongilardi E, Bilocati M, Avagnina P, and Versino E

Subjects
Adult, Age Factors, Aged, Aged, 80 and over, Amino Acids administration & dosage, Comorbidity, Diet, Vegan, Dietary Supplements, Female, Glomerular Filtration Rate, Humans, Keto Acids administration & dosage, Male, Middle Aged, Patient Preference, Proteinuria etiology, Renal Dialysis, Renal Insufficiency, Chronic complications, Renal Insufficiency, Chronic physiopathology, Young Adult, Diet, Protein-Restricted methods, Dietary Proteins administration & dosage, Patient Compliance, Renal Insufficiency, Chronic diet therapy
Abstract

Background: There is no single, gold-standard, low-protein diet (LPD) for CKD patients; the best compliance is probably obtained by personalization. This study tests the hypothesis that a multiple choice diet network allows patients to attain a good compliance level, and that, in an open-choice system, overall results are not dependent upon the specific diet, but upon the clinical characteristics of the patients., Methods: Observational study: Three LPD options were offered to all patients with severe or rapidly progressive CKD: vegan diets supplemented with alpha-ketoacids and essential aminoacids; protein-free food in substitution of normal bread and pasta; other (traditional, vegan non supplemented and tailored). Dialysis-free follow-up and survival were analyzed by Kaplan Meier curves according to diet, comorbidity and age. Compliance and metabolic control were estimated in 147 subjects on diet at March 2015, with recent complete data, prescribed protein intake 0.6 g/Kg/day. Protein intake was assessed by Maroni Mitch formula., Results: Four hundreds and forty nine patients followed a LPD in December, 2007- March, 2015 (90% moderately restricted LPDs, 0.6 g/Kg/day of protein, 10% at lower targets); age (median 70 (19-97)) and comorbidity (Charlson index: 7) characterized our population as being in line with the usual CKD European population. Median e-GFR at start of the diet was 20 mL/min, 33.2% of the patients were diabetics. Baseline data differ significantly across diets: protein-free schemas are preferred by older, high-comorbidity patients (median age 76 years, Charlson index 8, GFR 20.5 mL/min, Proteinuria: 0.3 g/day), supplemented vegan diets by younger patients with lower GFR and higher proteinuria (median age 65 years, Charlson index 6, GFR 18.9 mL/min; Proteinuria: 1.2 g/day); other diets are chosen by an intermediate population (median age 71 years, Charlson index 6; GFR 22.5 mL/min; Proteinuria: 0.9 g/day); (p <0.001 for age, Charlson index, proteinuria, GFR). Adherence was good, only 1.1% of the patients were lost to follow-up and protein intake was at target in most of the cases with no differences among LPDs (protein intake: 0.47 (0.26-0.86) g/Kg/day). After adjustment for confounders, and/or selection of similar populations, no difference in mortality or dialysis start was observed on the different LPDs. Below the threshold of e-GFR 15 mL/min, 50% of the patients remain dialysis free for at least two years., Conclusion: A multiple choice LPD system may allow reaching good adherence, without competition among diets, and with promising results in terms of dialysis-free follow-up. The advantages with respect to a non-customized approach deserve confirmation in further comparative studies or RCTs.

Published
2016
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43. Revisiting nephrocalcinosis: A single-centre perspective. A northern Italian experience.

Author

Piccoli GB, De Pascale A, Randone O, Vigotti FN, Priola AM, Naretto C, Ferraresi M, Aroasio E, Gonella S, Mongilardi E, Scognamiglio S, Consiglio V, Roggero S, Piga A, Roccatello D, and Veltri A

Subjects
Adolescent, Adult, Age Distribution, Aged, Aged, 80 and over, Autoimmune Diseases epidemiology, Child, Female, Genetic Predisposition to Disease, Heredity, Humans, Italy epidemiology, Male, Middle Aged, Nephrocalcinosis diagnostic imaging, Nephrocalcinosis therapy, Nephrology, Outpatient Clinics, Hospital, Prevalence, Referral and Consultation, Retrospective Studies, Risk Factors, Sex Distribution, Thalassemia epidemiology, Time Factors, Young Adult, Nephrocalcinosis epidemiology
Abstract

Aim: Nephrocalcinosis is a clinical-pathological entity characterized by the deposition of calcium salts within the kidney parenchyma. Both the protean presentation and multiple causes may explain the lack of data regarding its prevalence. The aim of this study is to report the prevalence and main clinical features of nephrocalcinosis diagnosed in a newly opened nephrology outpatient unit., Methods: Analysis on the data we prospectively gathered from the start of activity (2007-2013) was carried out. Clinical and laboratory data were collected from the medical records and from the general laboratory; diagnosis was based upon imaging data reviewed by the same radiologists., Results: Sixty-five of 2695 patients referred to our unit were diagnosed with nephrocalcinosis (2.4%). The affected patients were younger than the overall out-patient population (median: 37.7 (min-max: 8-82) vs 63 years (2-102) P < 0.001), with higher female prevalence (68% vs 51.4%: P < 0.05) and better preserved kidney function (CKD-EPI 103 (23-165) vs 60 mL/min (3.2-169) P < 0.001). Kidney stones were the main reason for referral (35.4%), followed by electrolyte disturbances (22.7%), acute pyelonephritis (4.6%), AKI or CKD (4.6%). Nephrocalcinosis was associated with autoimmune diseases in 29% and with microcythaemia in 23%, while positive family history was present in 23% of patients. Various electrolyte disturbances were observed, with hypercalciuria being the hallmark of beta thalassaemic patients., Conclusions: Nephrocalcinosis is a rare, but not exceptional disease in nephrology. In Mediterranean countries, microcythaemia would appear to be a major cause of this disease. Greater awareness of nephrocalcinosis is needed for an integrated approach involving various branches of internal medicine and radiology., (© 2015 Asian Pacific Society of Nephrology.)

Published
2016
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44. Which low-protein diet for which CKD patient? An observational, personalized approach.

Author

Piccoli GB, Deagostini MC, Vigotti FN, Ferraresi M, Moro I, Consiglio V, Scognamiglio S, Mongilardi E, Clari R, Aroasio E, Versino E, and Porpiglia F

Subjects
Age Factors, Aged, Aged, 80 and over, Cause of Death, Comorbidity, Disease Progression, Female, Glomerular Filtration Rate, Humans, Male, Middle Aged, Patient Compliance, Proteinuria epidemiology, Renal Dialysis, Diet, Protein-Restricted, Diet, Vegetarian, Dietary Proteins administration & dosage, Renal Insufficiency, Chronic diet therapy
Abstract

Objectives: Low protein diets (LPDs) are milestones in chronic kidney disease (CKD). Concerns over compliance and safety limit their use. The aim of this study was to test the feasibility and main results of a multiple-choice approach to LPDs, adapted to patient preferences., Methods: From December 2007 to January 2013, all CKD patients (stages 4/5; progressive stage 3) without contraindications (malnutrition, short life expectancy), were offered two main LPDs (proteins 0.6 g/kg daily): Vegan supplemented (LPD-KA) or with "aproteic" commercial food (LPD-ACF). LPDs followed a qualitative approach based on forbidden and allowed food; one to three free meals per week, and flexible control policy (1-3 mo). Start of dialysis, death, and combined outcome (death-dialysis) were analyzed by Kaplan-Meier curves and Cox model. Comparison with dialysis in patients with glomerular filtration rate (GRF) <15 mL/min, (corresponding to "early" dialysis start) employed standardized mortality rates, with respect to the Italian and the United States Dialysis Registry., Results: One hundred eighty-five patients (222 patient-years) started at least a trial of LPD-KA, 122 (177 patients-years) LPD-ACF; only 3 patients with GFR <30 mL/min denied an LPD trial. Patients who chose LPD-KA were younger than those on LPD-ACF (63 versus 74 y), had less comorbidity (82% versus 93%), higher proteinuria (1.4 versus 0.7 g/d) and lower GFR (17 versus 23 mL/min) (P < 0.001). Median daily protein intake was 0.7 g/kg on both diets (Maroni-Mitch formula). The combined outcome (death or dialysis) was not influenced by the diet chosen (Cox analysis). Relative risk for death on the diet (patients with GFR <15 mL/min) was 0.5 with respect to the Italian Registry and 0.3 to the United States Dialysis Registry. The diets had comparable costs (1 y on dialysis: 50 patient-years on LPD)., Conclusions: The choice of diet is strictly linked to patient characteristics, thus supporting a multiple-choice offer. Once corrected for baseline data, both LPDs led to similar results, suggesting at least survival equivalence with dialysis, at lesser cost., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published
2014
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45. Chronic dialysis discontinuation: a systematic narrative review of the literature in the new millennium.

Author

Piccoli GB, Guzzo G, Vigotti FN, Scognamiglio S, Consiglio V, Aroasio E, Gonella S, Castelluccia N, Mauro G, and Colombi N

Subjects
Humans, Kidney Failure, Chronic physiopathology, Withholding Treatment, Kidney physiopathology, Kidney Failure, Chronic therapy, Recovery of Function physiology, Renal Dialysis
Abstract

Introduction and Aims: Renal function recovery (RFR), defined as the discontinuation of dialysis after 3 months of replacement therapy, is an uncommon occurrence. At a time when the "too early" start of dialysis is in discussion, a systematic review of the literature for cases in which patients recovered renal function after starting dialysis with chronic indications, including single cases and large series, may lead to attention being focused on this interesting issue., Methods: The search strategy was built in Medline on Pubmed, in EMBASE and in the Cochrane Collaboration (August 2013) combining Mesh, Emtree and free terms: dialysis or hemodialysis, kidney function, renal function and recovery (publication date 2000-2013). The following tasks were performed in duplicate: titles and abstracts were manually screened, the data were extracted: title, author, objective, year, journal, period of study, multi-center, country, type of study., Results: The systematic review retrieved 1,894 titles; 58 full papers were retrieved and the final selection included 24 papers: 11 case series or Registry data (4 from ANZdata) and 13 case reports. In spite of the high heterogeneity of the studies, overall they suggest that RFR occurs in about 1% of patients, without differences between PD and HD. RFR appears to be more frequent in elderly patients with renal vascular disease (up to 10% RFR in cholesterol emboli or scleroderma), but is reported in all types of primary and secondary kidney diseases., Conclusions: RFR is a clinical event that should be looked for, particularly in elderly patients with vascular comorbidity.

Published
2014
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46. Tailoring dialysis and resuming low-protein diets may favor chronic dialysis discontinuation: report on three cases.

Author

Piccoli GB, Guzzo G, Vigotti FN, Capizzi I, Clari R, Scognamiglio S, Consiglio V, Aroasio E, Gonella S, Veltri A, and Avagnina P

Subjects
Aged, Female, Humans, Kidney Failure, Chronic diet therapy, Diet, Protein-Restricted, Kidney Failure, Chronic therapy, Renal Dialysis methods
Abstract

Renal function recovery (RFR), defined as the discontinuation of dialysis after 3 months of replacement therapy, is reported in about 1% of chronic dialysis patients. The role of personalized, intensive dialysis schedules and of resuming low-protein diets has not been studied to date. This report describes three patients with RFR who were recently treated at a new dialysis unit set up to offer intensive hemodialysis. All three patients were females, aged 73, 75, and 78 years. Kidney disease included vascular-cholesterol emboli, diabetic nephropathy and vascular and dysmetabolic disease. At time of RFR, the patients had been dialysis-dependent from 3 months to 1 year. Dialysis was started with different schedules and was progressively discontinued with a "decremental" policy, progressively decreasing number and duration of the sessions. A moderately restricted low-protein diet (proteins 0.6 g/kg/day) was started immediately after dialysis discontinuation. The most recent update showed that two patients are well off dialysis for 5 and 6 months; the diabetic patient died (sudden death) 3 months after dialysis discontinuation. Within the limits of small numbers, our case series may suggest a role for personalized dialysis treatments and for including low-protein diets in the therapy, in enhancing long-term RFR in elderly dialysis patients., (© 2014 International Society for Hemodialysis.)

Published
2014
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47. Home dialysis and the Internet: designing an e-learning platform via brainstorming sessions.

Author

Piccoli GB, Ferraresi M, Murciano A, Pereno A, Consiglio V, Scognamiglio S, Deagostini MC, Randone O, Digiorgio G, and Calderale MP

Subjects
Adult, Aged, Aged, 80 and over, Caregivers psychology, Computer Graphics, Cooperative Behavior, Diffusion of Innovation, Female, Humans, Male, Middle Aged, Nursing, Supervisory, Program Development, Renal Insufficiency, Chronic psychology, Software Design, Students, Medical psychology, Terminology as Topic, Video Recording, Young Adult, Computer-Assisted Instruction methods, Health Knowledge, Attitudes, Practice, Hemodialysis, Home methods, Interdisciplinary Communication, Internet, Kidney Diseases therapy, Patient Education as Topic methods, Renal Insufficiency, Chronic therapy
Abstract

Background: The resurgence of home hemodialysis (HHD) underlines the importance of educational programs. Brainstorming is a powerful tool for innovation, widely employed in industry but seldom used in medicine. The aim of this study was to define an e-learning Web platform for HHD patients via a brainstorming approach., Methods: Four brainstorming sessions were held 2-6 weeks apart. Twelve people were involved: 2 dialysis physicians, 2 nurses, 2 HHD patients, 2 caregivers, a filmmaker, 2 computer experts (1 with a psychology degree) and a senior engineer. Each session was summarized as the starting point for the following one. The topics discussed were the platform structure and its logo., Results: For the platform, the following requirements were defined: teaching should be extensive and tailored to different levels of knowledge; all available teaching tools (tutorials, demonstrations, recorded and written materials) should be used; films enhance emotional participation and can be used to reduce fears; the contents should include general information on chronic kidney disease, details of all types of renal replacement therapy (RRT) (how and why), dialysis accidents, blood and imaging tests, laws and reimbursements, direct experiences and history of RRT. Remote monitoring and visual interactions are important for reassurance about HHD and should be provided. The requirements for the logo were that it be innovative, related to daily life, representative of a holistic approach and convey happiness. The logo "Hom-e-hem" was created, playing on the assonance between the religious term Om and the word home, with the e of electronic linking it with hem, short for hemodialysis., Conclusion: Brainstorming sessions can be used to design patient-tailored educational interventions. The key message, "self-care is a bridge from illness back to life," may apply to a wider context.

Published
2012
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48. Why home hemodialysis? A systematic "marketing" analysis.

Author

Piccoli GB, Ferraresi M, Consiglio V, Scognamiglio S, Deagostini MC, Randone O, Vigotti FN, and Calderale PM

Subjects
Costs and Cost Analysis, Humans, Hemodialysis, Home economics, Hemodialysis, Home mortality
Abstract

Background: Home hemodialysis (HHD) has met with alternating fortunes. The present revival of interest is due to lower costs and more frequent/efficient treatments. HHD is underdeveloped, and a marketing approach may help in defining development strategies. The aim of this study was to systematically review the recent literature (2000-2010) according to a marketing approach, defining the potential of HHD according to the classical marketing items: market size, growth rate, profitability, trends, keys for success, needs for structures and distribution channels., Methods: A Medline search was conducted for 2000-2010. The analysis took into account the recent trends in publication as a measure of interest, size and trends, while survival and costs were analyzed as keys for success. The issues of structures and distribution channels were arbitrarily considered as equivalent to the overall hemodialysis market., Results: Interest in HHD is growing, as shown by the increasing number of published papers (9 in 2000, 52 in 2010); yet, clinical studies accounted for less than half of the papers. In the 138 clinical studies, quality of life (33 papers) and metabolism (16 papers) were the most studied topics. Survival and cost analyses were highly heterogeneous (the broad inclusion of nocturnal or quotidian dialysis has to be mentioned). Overall, survival was equal to, or better than, that for other modalities, including transplantation and peritoneal dialysis; costs compared favorably with hospital dialysis and were equivalent to those of peritoneal dialysis., Conclusion: The small "market" of HHD is increasing, with potential for further growth, the keys for success being equivalence or superiority of survival at equivalent or lower costs.

Published
2012
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49. Protean presentation and multiple challenges of nephrocalcinosis in pregnancy (six pregnancies in four patients).

Author

Piccoli GB, Attini R, De Pascale A, Pagano A, Consiglio V, Scognamiglio S, Vigotti F, Bossotti C, Gollo E, Veltri A, and Todros T

Subjects
Adult, Cesarean Section, Female, Humans, Hypertension etiology, Hypertension pathology, Infant, Newborn, Infant, Premature, Nephrocalcinosis pathology, Pregnancy, Pregnancy, Twin, Prognosis, Prospective Studies, Water-Electrolyte Imbalance etiology, Water-Electrolyte Imbalance pathology, Calcium metabolism, Nephrocalcinosis etiology, Pregnancy Complications physiopathology
Abstract

Background: Nephrocalcinosis is an umbrella term covering increased content of calcium salts in the renal parenchyma, interstitial damage and potential evolution towards renal failure. Pregnancy is often the first occasion for biochemical or imaging tests in young women and may allow early diagnosis. Conversely, even mild kidney disease may represent a challenge in pregnancy., Aim: The aim of this study was to report on four patients in whom nephrocalcinosis was first diagnosed during pregnancy, exemplifying the protean presentation and multiple challenges of nephrocalcinosis in pregnancy., Methods: This is a case series study including data on all pregnancies prospectively gathered in the Nephrological-Obstetric Unit dedicated to pregnancy and kidney diseases (2000-11)., Results: Six pregnancies were observed in four patients (31-35 years; one twin pregnancy, one ongoing, one patient with three pregnancies). Symptoms were oedema in two (later developed in a further patient), renal functional impairment and electrolyte imbalance in two each. Two patients developed hypertension late in pregnancy. Electrolyte imbalance was life-threatening in one patient (severe acidosis, severe hyperkalaemia: 7.5 mEq/L). Delivery was by Caesarean section in three patients, preterm in one. Multiple or long hospitalizations for metabolic reasons were needed in three patients, the fourth was hospitalized for obstetric reasons. In all patients, diagnosis of nephrocalcinosis was made at ultrasounds during basic nephrological evaluation, confirmed at computerized tomography scan in three. The pathogenesis was linked to diuretic abuse in one case and to collagen disease, inborn errors and prematurity, possibly associated with diuretic misuse, in the others., Conclusion: Nephrocalcinosis may have protean presentations in pregnancy. The risk of severe electrolyte derangements, oedema and hypertension warrants strict clinical surveillance.

Published
2012
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50. [Studies of the action of Lipari pumice dust on experimental tuberculosis in guinea pigs and on cultures of Koch bacillus].

Author

Curci G, Ninni A, Sarappa A, D'Antonio G, and Scognamiglio S

Subjects
Aluminum Silicates pharmacology, Animals, Culture Media, Dust, Guinea Pigs, Mycobacterium tuberculosis growth & development, Mycobacterium tuberculosis pathogenicity, Mycobacterium tuberculosis drug effects, Silicic Acid pharmacology, Silicon Dioxide pharmacology, Silicotuberculosis
Published
1978

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