Your search keyword '"F. Sidoti"' showing total 103 results

1. V348I mutation in UL23 gene of human herpesvirus 1 in a case of herpetic hepatitis and haemophagocytic lymphohistiocytosis

Author

S. Corcione, F. Sidoti, C. Costa, S. Mornese Pinna, C. Bonetto, R. Urbino, R. Cavallo, and F.G. De Rosa

Subjects

Infectious and parasitic diseases, RC109-216

Abstract

We herein report the case of a young immunocompetent adult patient with a rapidly fatal haemophagocytic lymphohistiocytosis syndrome related to human herpesvirus 1 (HHV-1) infection, with herpetic hepatitis and persistent high-level viraemia despite treatment with acyclovir. Haemophagocytic lymphohistiocytosis was confirmed in the patient's spleen and bone marrow. HHV-1 DNA was extracted from whole blood and liver biopsy and the UL23 gene was sequenced. A V348I natural polymorphism of the TK protein was found in blood and liver specimens. Further studies are needed to investigate the role of this polymorphism in the development of systemic immune dysregulation. Keywords: Acyclovir, haemophagocytic lymphohistiocytosis syndrome, UL23 gene, herpetic hepatitis, human herpesvirus-1

Published

2019

2. DEVELOPMENT OF A LUX-REAL TIME PCR FOR HUMAN HERPESVIRUS 7 (HHV7) IN PRIMARY CUTANEOUS T CELL LYMPHOMAS.

Author

F. Sidoti, M. Bergallo, C. Costa, R. Ponti, M.E. Terlizzi, S. Astegiano, C. Merlino, M. Novelli, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

3. HUMAN HERPES VIRUS 8 INFECTION IN KIDNEY TRANPLANT PATIENTS

Author

F. Sidoti, C. Costa, M. Bergallo, M.E. Terlizzi, S. Astegiano, D. Re, G.P. Segoloni, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

4. INCIDENCE OF HCMV INFECTION IN THE FIRST 3 MONTHS FOLLOWING RENAL TRANSPLANT

Author

M.E. Terlizzi, C. Costa, M. Bergallo, F. Sidoti, S. Astegiano, E. Piasentin, R. Vendrame, G.P. Segoloni, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

5. POLYOMAVIRUS BK IN KIDNEY BIOPSIES FROM TRANSPLANT RECIPIENTS

Author

S. Astegiano, M. Bergallo, C. Costa, F. Sidoti, M.E. Terlizzi, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

6. BK VIRUS AND JC VIRUS COINFECTION IN A RENAL TRANSPLANT RECIPIENT

Author

S. Astegiano, C. Costa, M. Bergallo, F. Sidoti, M.E. Terlizzi, G.P. Segoloni, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

7. LYTIC CYTOMEGALOVIRUS GENE EXPRESSION ANALYSIS USING RT-PCR

Author

M.E. Terlizzi, M. Bergallo, C. Costa, F. Sidoti, S. Astegiano, F. Sinesi, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2007

8. PREVALENZA DI INFEZIONE DA CMV, EBV E HHV8 NELLE MALATTIE INFIAMMATORIE INTESTINALI

Author

C. Costa, M. Bergallo, A. Lavagna, M. Daperno, F. Sidoti, A. Pera, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2006

9. NON-ORGAN-SPECIFIC AUTOANTIBODIES IN CMV PP65-ANTIGENAEMIA-POSITIVE AND - NEGATIVE RENAL TRANSPLANT RECIPIENTS

Author

C. Costa, M. Bergallo, G.A. Touscoz, F. Sidoti, C. Merlino, G.P. Segoloni, F. Giacchino, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2006

10. DIAGNOSI DELL’INFEZIONE DA CITOMEGALOVIRUS UMANO (HCMV) IN TRAPIANTATI RENALI

Author

M. Bergallo, C. Merlino, C. Costa, S. Mantovani, F. Sidoti, S. Baro, A. Negro Ponzi, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2005

11. SVILUPPO DI UNA PCR QUANTITATIVA COMPETITIVA PER LA VALUTAZIONE DELLA CARICA VIRALE DELL’EBV

Author

M. Bergallo, C. Merlino, R. Daniele, F. Sidoti, S. Mantovani, A. Negro Ponzi, and R. Cavallo

Subjects

Microbiology, QR1-502

Published

2004

12. TRANSPLANTATION CLINICAL 1

Author

T. Schachtner, P. Reinke, C. Dorje, G. Mjoen, K. Midtvedt, E. H. Strom, O. Oyen, T. Jenssen, A. V. Reisaeter, Y. V. Smedbraaten, S. Sagedal, M. W. Fagerland, A. Hartmann, S. Thiel, A. Zulkarnaev, A. Vatazin, F. Vincenti, E. Harel, A. Kantor, T. Thurison, G. Hoyer-Hansen, C. Craik, V. B. Kute, P. S. Shah, A. V. Vanikar, P. R. Modi, P. R. Shah, M. R. Gumber, H. V. Patel, D. P. Engineer, V. R. Shah, J. Rizvi, H. L. Trivedi, J. Malheiro, L. Dias, L. S. Martins, I. Fonseca, S. Pedroso, M. Almeida, A. Castro-Henriques, A. Cabrita, C. Costa, M. Ritta, F. Sinesi, F. Sidoti, S. Mantovani, A. Di Nauta, M. Messina, R. Cavallo, A. Verflova, E. Svobodova, J. Slatinska, A. Slavcev, E. Pokorna, O. Viklicky, J. Yagan, A. Chandraker, D. Diena, G. Tognarelli, A. Ranghino, S. Bussolino, F. Fop, G. P. Segoloni, L. Biancone, F. Leone, M. V. Mauro, P. Gigliotti, D. Lofaro, F. Greco, D. Perugini, T. Papalia, A. Perri, D. Vizza, C. Giraldi, R. Bonofilgio, S. Luis-Lima, D. Marrero, A. Gonzalez-Rinne, A. Torres, E. Salido, A. Jimenez-Sosa, A. Aldea-Perona, J. M. Gonzalez-Posada, L. Perez-Tamajon, A. Rodriguez-Hernandez, N. Negrin-Mena, E. Porrini, H. Pihlstrom, D. O. Dahle, H. Holdaas, N. Von Der Lippe, B. Waldum, F. Brekke, A. Amro, I. Os, P. Klin, H. Sanabria, P. Bridoux, J. De Francesco, R. M. Fortunato, P. Raffaele, J. Kong, S. H. Son, H. Y. Kwon, E. J. Whang, W. Y. Choi, C. S. Yoon, V. Thanaraj, A. Theakstone, K. Stopper, A. Ferraro, S. Bhattacharjya, M. Devonald, A. Williams, A. Mella, E. Gallo, M. C. Di Vico, F. Pagani, M. Gai, H. J. Cho, K. W. Nho, S.-K. Park, S. B. Kim, K. Yoshida, D. Ishii, T. Ohyama, D. Kohguchi, Y. Takeuchi, A. Varga, B. Sandor, K. Kalmar-Nagy, A. Toth, K. Toth, P. Szakaly, A. Kildushevsky, V. Fedulkina, R. Kantaria, O. Staeck, F. Halleck, O. Rissling, M. Naik, H.-H. Neumayer, K. Budde, D. Khadzhynov, D. Bhadauria, A. Kaul, N. Prasad, R. K. Sharma, S. Sezer, Z. Bal, M. Erkmen Uyar, O. Guliyev, B. Erdemir, T. Colak, N. Ozdemir, M. Haberal, Y. Caliskan, H. Yazici, A. S. Artan, O. A. Oto, N. Aysuna, S. Bozfakioglu, A. Turkmen, A. Yildiz, M. S. Sever, T. Yagisawa, A. Nukui, T. Kimura, K. Nannmoku, A. Kurosawa, Y. Sakuma, A. Miki, F. Damiano, G. Ligabue, S. De Biasi, M. Granito, A. Cossarizza, G. Cappelli, A. C. Henriques, J. Davide, M. E. Von During, T. G. Jenssen, J. Bollerslev, K. Godang, A. Asberg, T. Bachelet, C. Martinez, A. Bello, S. Kejji, L. Couzi, G. Guidicelli, S. Lepreux, J. Visentin, N. Congy-Jolivet, L. Rostaing, J.-L. Taupin, N. Kamar, P. Merville, H. Ozdemir, S. Yildirim, E. Tutal, B. Sayin, N. Ozdemir Acar, M. Banasik, M. Boratynska, K. Koscielska-Kasprzak, D. Kaminska, D. Bartoszek, O. Mazanowska, M. Krajewska, S. Zmonarski, P. Chudoba, T. Dawiskiba, M. Protasiewicz, A. Halon, A. Sas, M. Kaminska, M. Klinger, N. Stefanovic, T. Cvetkovic, R. Velickovic - Radovanovic, T. Jevtovic - Stoimenov, P. Vlahovic, R. Rungta, P. Das, D. S. Ray, S. Gupta, A. Kolonko, M. Szotowska, P. Kuczera, J. Chudek, A. Wiecek, E. Sikora-Grabka, M. Adamczak, P. Madej, A. Amanova, Z. Kendi Celebi, F. Bakar, M. G. Caglayan, K. Keven, C. Massimetti, G. Imperato, G. Zampi, A. De Vincenzi, G. D. D. Fabbri, F. Brescia, S. Feriozzi, J. J. Filipov, B. K. Zlatkov, E. P. Dimitrov, D. A. Svinarov, R. Poesen, K. De Vusser, P. Evenepoel, D. Kuypers, M. Naesens, B. Meijers, H. Kocak, V. T. Yilmaz, F. Yilmaz, H. B. Uslu, I. Aliosmanoglu, H. Ermis, A. Dinckan, R. Cetinkaya, F. F. Ersoy, G. Suleymanlar, J.-C. Oliveira, J. Santos, L. Lobato, D. Mendonca, Y. Watarai, T. Yamamoto, M. Tsujita, T. Hiramitsu, N. Goto, S. Narumi, T. Kobayashi, P.-D. Line, A. Housawi, A. House, C. Ng, K. Denesyk, F. Rehman, L. Moist, C. Musetti, M. Battista, C. Izzo, G. Guglielmetti, A. Airoldi, P. Stratta, T. Cena, M. Quaglia, R. Fenoglio, D. Cagna, A. Amoroso, A. Palmisano, A. M. Degli Antoni, A. Vaglio, G. Piotti, E. Cremaschi, C. Buzio, U. Maggiore, M.-C. Lee, B.-G. Hsu, F. Zalamea Jarrin, B. Sanchez Sobrino, O. Lafuente Covarrubias, S. Karsten Alvarez, P. Dominguez Apinaniz, R. Llopez Carratala, J. Portoles Perez, T. Yildirim, R. Yilmaz, E. Turkmen, M. Altindal, M. Arici, B. Altun, Y. Erdem, E. Dounousi, M. Mitsis, K. Naka, H. Pappas, L. Lakkas, H. Harisis, K. Pappas, V. Koutlas, I. Tzalavra, G. Spanos, L. Michalis, K. Siamopoulos, T. Iwabuchi, K. Nanmoku, S. Yasunaru, M. Yoshikawa, K. Kitamura, H. Fuji, M. Fujisawa, S. Nishi, P. Carta, M. Zanazzi, E. Buti, A. Larti, L. Caroti, L. Di Maria, E. E. Minetti, Y. Shi, L. Luo, B. Cai, T. Wang, Y. Zou, L. Wang, Y. Kim, H. S. Kim, B. S. Choi, C. W. Park, C. W. Yang, Y.-S. Kim, B. H. Chung, C. H. Baek, M. Kim, J.-S. Kim, W. S. Yang, D. J. Han, I. Mikolasevic, S. Racki, V. Lukenda, M. P. Persic, M. Colic, B. Devcic, L. Orlic, B. Gurlek Demirci, C. B. Say N, F. N. Ozdemir Acar, S. Vali, K. Ismal, M. Sahay, F. Civiletti, V. Cantaluppi, D. Medica, A. T. Mazzeo, B. Assenzio, I. Mastromauro, I. Deambrosis, F. Giaretta, V. Fanelli, L. Mascia, I. Gkirdis, A. Bechlioulis, D. Evangelou, F. Zarzoulas, A. Kotsia, O. Balafa, G. Tzeltzes, G. Nakas, R. Kalaitzidis, C. Katsouras, S. Uyanik, S. K. Toprak, O. Ilhan, M. Ekmen Uyar, H. Hernandez Vargas, M. Artamendi Larranaga, E. Ramalle Gomara, F. Gil Catalinas, A. Bello Ovalle, G. Pimentel Guzman, A. Coloma Lopez, M. Sierra Carpio, A. Gil Paraiso, C. Dall Anesse, I. Beired Val, E. Huarte Loza, B. Y. Choy, L. Kwan, M. Mok, T. M. Chan, T. Yamakawa, A. Kobayashi, I. Yamamoto, A. Mafune, Y. Nakada, Y. Tannno, N. Tsuboi, H. Yamamoto, K. Yokoyama, I. Ohkido, T. Yokoo, Y. Luque, D. Anglicheau, M. Rabant, R. Clement, H. Kreis, A. Sartorius, L.-H. Noel, M.-O. Timsit, C. Legendre, N. Rancic, N. Vavic, V. Dragojevic-Simic, J. Katic, N. Jacimovic, A. Kovacevic, M. Mikov, N. M. H. Veldhuijzen, M. B. Rookmaaker, A. D. Van Zuilen, T. Q. Nquyen, W. H. Boer, W. Sahtout, H. Ghezaiel, A. Azzebi, S. Ben Abdelkrim, Y. Guedri, S. Mrabet, S. Nouira, S. Ferdaws, S. Amor, A. Belarbia, D. Zellama, M. Mokni, A. Achour, A. Parikova, V. Hanzal, J. Fronek, B. J. Orandi, N. T. James, R. A. Montgomery, N. M. Desai, D. L. Segev, F. Fontana, M. Ballestri, and R. Magistroni

Subjects

Transplantation, Nephrology

Published

2014

13. Transplantation - clinical I

Author

M. Bonani, J. Brockmann, C. D. Cohen, T. Fehr, A. Nocito, M. Schiesser, A. L. Serra, M. Blum, M. Struker, D. F. Frey, R. P. Wuthrich, Y. W. Kim, S. J. Park, T. H. Kim, Y.-H. Kim, S. W. Kang, L. Webb, A. Casula, C. Tomson, Y. Ben-Shlomo, H. Mansour, A. Akl, E. Wafa, M. El Shahawy, R. Palma, S. Swaminathan, A. B. Irish, A. Kolonko, J. Chudek, A. Wiecek, Y. Vanrenterghem, D. Kuypers, D. V. Katrien, P. Evenepoel, K. Claes, B. Bammens, B. Meijers, M. Naesens, S. Lo, C.-K. Chan, D. Yong, P.-N. Wong, T.-H. Kwan, Y.-L. Cheng, K.-S. Fung, B.-Y. Choy, K.-F. Chau, C.-B. Leung, J. Ebben, J. Liu, S.-C. Chen, A. Collins, Y.-W. Ho, M. Abelli, A. Ferrario DI Torvajana, E. Ticozzelli, B. Maiga, A. Patane, P. Albrizio, M. Gregorini, C. Libetta, T. Rampino, P. Geraci, A. Dal Canton, M.-T. Rotter, J. Jacobi, K. Pressmar, K. Amann, K.-U. Eckardt, A. Weidemann, K. Muller, M. Stein, C. Diezemann, A. Sefrin, N. Babel, P. Reinke, T. Schachtner, C. Costa, G. A. Touscoz, F. Sidoti, F. Sinesi, S. Mantovani, S. Simeone, C. Balloco, E. Piasentin Alessio, M. Messina, G. Segoloni, R. Cavallo, R. .K. Sharma, D. A. Kaul, R. K. Gupta, A. Gupta, N. Prasad, D. Bhadhuria, K. J. Suresh, S. Benaboud, D. Prie, E. Thervet, S. Urien, C. Legendre, J.-C. Souberbielle, D. Hirt, G. Friedlander, J.-M. Treluyer, M. Courbebaisse, M. Arias, J. Campistol, J. Pascual, J. M. Grinyo, D. Hernandez, J. M. Morales, L. M. Pallardo, D. Seron, L. Senecal, A. Boucher, R. Dandavino, S. Colette, M. Vallee, J.-P. Lafrance, Y. Tung-Min, W. Min-Ju, C. Cheng-Hsu, C. Chi-Hung, S. Kuo-Hsiung, W. Mei-Chin, S. Direkze, M. Khorsavi, S. Stuart, A. Goode, G. Jones, C. Massimetti, I. Napoletano, G. Imperato, M. T. Muratore, S. Fazio, G. Pessina, F. Brescia, S. Feriozzi, K. Tanaka, K. Sakai, A. Futaki, Y. Hyoudo, M. Muramatsu, T. Kawamura, S. Shishido, S. Hara, A. Kushiyama, A. Aikawa, K. Jankowski, J. Gozdowska, D. Lewandowska, A. Kwiatkowski, M. Durlik, P. Pruszczyk, Y. Obi, N. Ichimaru, T. Kato, M. Okumi, J. Kaimori, K. Yazawa, N. Nonomura, Y. Isaka, S. Takahara, M. Aimele, R. Christophe, D. Geraldine, R. Eric, H. Alexandre, I. Masson, M. Nicolas, T. Ivan, J. Acil, T. Lise, H.-A. Aoumeur, D. Laurence, D. Pierre, C. Etienne, R. Lionel, K. Nassim, M. Emmanuel, A. Eric, M. Christophe, K. Alexandre, B. Pierre, H. Jean-Philippe, P. Dominique, L. Christophe, G. Alexei, D. Michel, P. Shah, V. B. Kute, A. Vanikar, M. Gumber, P. Modi, H. Trivedi, J. GoIebiewska, A. Debska-Slizien, B. Rutkowski, L. Domanski, G. Dutkiewicz, K. Kloda, A. Pawlik, A. Ciechanowicz, A. Binczak-Kuleta, J. Rozanski, M. Myslak, K. Safranow, K. Ciechanowski, C. S. Aline, T. Basset, X. Delavenne, E. Alamartine, C. Mariat, K. Bobrek-Lesiakowska, M. Wisniewska, M. Romanowski, M. Kurzawski, M. De Borst, L. Baia, G. Navis, S. Bakker, A. Ranghino, G. Tognarelli, E. Basso, A. M. Manzione, G. Daidola, G. P. Segoloni, T. Kimura, T. Yagisawa, N. Ishikawa, Y. Sakuma, T. Hujiwara, A. Nukui, M. Yashi, J. H. Kim, S.-S. Kim, D. J. Han, S.-K. Park, G. Randhawa, H. Patel, S. Taheri, O. Goker-Alpan, J. Ibrahim, K. Nedd, S. Shankar, H. Lein, B. Barshop, E. Boyd, M. Holida, R. Hillman, R. Mardach, N. Wienreb, B. Rever, R. Forte, A. Desai, A. Wijatyk, P. Chang, and R. Martin

Subjects

Transplantation, Nephrology

Published

2012

14. TRUST: Phase II trial of induction chemotherapy (CT) with FOLFOXIRI + bevacizumab (BV) followed by chemo-radiotherapy (CRT) + BV and surgery in locally advanced rectal carcinoma (LARC)

Author

C. Vivaldi, P. Buccianti, G. Musettini, F. Bergamo, M.D. Rizzato, A. Sainato, A. Martignetti, S. Lucchesi, M. Franceschi, C. Boso, F. Pasqualetti, L. Ginocchi, F. Di Clemente, A. Gonnelli, L. Urbani, S. Montrone, I. Maretto, F. Sidoti, A. Falcone, and G. Masi

Subjects

Oncology, Hematology

Published

2016

15. Theoretical and numerical treatment of surface integrals involving the free-space Green's function

Author

S. Caorsi, F. Sidoti, and D. Moreno

Subjects

Surface (mathematics), Computation, Surface integral, Mathematical analysis, Basis function, Geometry, Method of moments (statistics), Integral equation, symbols.namesake, Singularity, Green's function, symbols, Electrical and Electronic Engineering, Mathematics

Abstract

This paper deals with the problem of the calculation of surface integrals for electromagnetic scattering in the case of the widely popular double-triangular basis functions first introduced by Rao, Wilton, and Glisson (1982). An entire set of formulas is obtained which overrides the difficulties inherent to the singularity of the integrands, and results showing the stability, accuracy, and efficiency of the methods developed are reported in an application of the method of moments to the case of perfectly conducting surfaces and computation of near field in domains including the surface itself. Furthermore, the authors provide insight as regards the capability of triangular basis functions to model near field patterns. >

Published

1993

16. Joint optimisation of multimedia trasmission over an Ip wired/wireless link

Author

Lamy-Bergot, J. Huusko, M. G. Martini, P. Amon, C. Bergeron, P. Hammes, G. Jeney, S. X. Ng, G. Panza, J. Peltola, and F. Sidoti

Published

2006

17. Transplantation clinical

Author

M. Betjes, W. Weimar, N. Litjens, C. Costa, A. Saldan, F. Sinesi, F. Sidoti, S. Mantovani, S. Simeone, C. Balloco, E. Piasentin Alessio, A. Piceghello, A. DI Nauta, A. Ranghino, G. Segoloni, R. Cavallo, Y. V. Smedbraaten, A. Hartmann, H. Rollag, T. Leivestad, A. Foss, H. Viko, I. Os, S. Sagedal, J. Zuber, K. Saoussen, L. Q. Moglie, N. Laure-Helene, G. Victor, C. Valerie, S. Remi, L. Annie, D. Georges, H. Maryvonne, F.-B. Veronique, N. Patrick, R. Eric, L. Christophe, L. Chantal, R. Pruthi, R. Ravanan, A. Casula, and P. Roderick

Subjects

Transplantation, Nephrology

Published

2012

18. LAPARO-ENDOSCOPIC 'RENDEZ-VOUS': A NEW TECHNIQUE IN THE CHOLEDOCHOLITIASIS TREATMENT

Author

E, Cavina, M, Franceschi, F, Sidoti, O, Goletti, P, Buccianti, and M, Chiarugi

Subjects

Adult, Aged, 80 and over, Cholangiopancreatography, Endoscopic Retrograde, Male, Gallstones, Middle Aged, Intraoperative Period, Sphincterotomy, Endoscopic, Cholecystectomy, Laparoscopic, Cholelithiasis, Humans, Female, Cholangiography, Aged

Abstract

Endoscopic sphincterotomy for common bile duct stone clearance during laparoscopic cholecystectomy may fail due to difficulties in cannulating the papilla major. In this study we propose a new technique that facilitates the cannulation of the papilla and the common bile duct stone clearance during a standard laparoscopic cholecystectomy. Its clearance percentage, complication rate and post-operative stay have been evaluated and compared with standardized procedures such as open surgery and endoscopic sphincterotomy before laparoscopic cholecystectomy.In a group of 16 patients presenting with cholelithiasis and common bile duct stones or papillitis, the sphincterotome was driven across the papilla into the choledochus by a Dormia basket passed in the duodenum through the cystic duct during laparoscopic cholecystectomy. Measures of outcome were clearance rate, mortality, morbidity and hospital stay. Furthermore, data obtained from this sample of patients were compared with those from another two groups of 16 patients in which choledocholithiasis was managed either by endoscopic sphincterotomy performed before laparoscopic cholecystectomy or by open cholecystectomy and trans-duodenal sphincterotomy.The rate of cannulation of the papilla and of the common bile duct stone clearance was 100% when the combined endo-laparoscopic approach was used in 15 patients with endoscopic sphincterotomy (93,7%) and in 15 patients with open sphincterotomy (93,7%), cholecystectomy was successful in every case. The groups were statistically similar with regard to complications; none of the patients required blood transfusion. The mean post operative stay was 95.2 hours (range 48-240) for the first group, 350.1 hours (range 192-1680) for the second and 69.7 hours (range 24-132) for the third.The laparo-endoscopic rendezvous, though still in evolution, is an efficacious method which can be used during the laparoscopic strategy of common bile duct clearance.

Published

1998

19. [Prognostic risk factors in patients operated on for perforated peptic ulcer. A retrospective analysis of critical factors of mortality and morbidity in a series of 40 patients who underwent simple closure surgery]

Author

M, Chiarugi, P, Buccianti, O, Goletti, L, Decanini, F, Sidoti, and E, Cavina

Subjects

Adult, Aged, 80 and over, Male, Analysis of Variance, Laparotomy, Age Factors, Middle Aged, Prognosis, Severity of Illness Index, Postoperative Complications, Risk Factors, Duodenal Ulcer, Peptic Ulcer Perforation, Humans, Female, Laparoscopy, Stomach Ulcer, APACHE, Aged, Retrospective Studies

Abstract

To identify factors affecting mortality and morbidity in patients operated on for perforated peptic ulcer.Retrospective analysis.University Hospital, Italy.Forty patients consecutively operated on for perforated peptic ulcer by simple suture procedure performed either by laparotomy (n = 26) or laparoscopic (n = 14) approach.Mortality was 20% (n = 8) and morbidity in survivors was 25% (n = 8). Compared to survivors, non-survivors were older (mean age 79.3 yrs. vs 60.0 yrs., p0.01), had worse APACHE II and SAPS scores (mean 20.1 vs 8.5, p0.001; and 13.1 vs. 5.5, p0.0001 respectively), were treated later (mean interval from outbreak of symptoms to surgery 30.8 hrs. vs. 11.1 hrs., p0.01), and the size of their perforation was larger (mean 15.1 mm. vs. 8.6 mm, p0.05). The laparoscopic approach was the only factor that significantly was associated with morbidity in survivors (p0.01). The presence of at least two risk factors, enhanced the probability of death.Old age, great APACHE II and SAPS scores, delay in treatment and large size of the perforation were associated significantly to mortality in perforated peptic ulcer patients. Efforts should be made perioperatively for patients having these risk factors.

Published

1996

20. Omeprazole versus ranitidine plus somatostatin in the treatment of severe gastroduodenal bleeding: a prospective, randomized, controlled trial

Author

O, Goletti, F, Sidoti, P V, Lippolis, F, De Negri, and E, Cavina

Subjects

Male, Peptic Ulcer Hemorrhage, Acute Disease, Humans, Drug Therapy, Combination, Female, Prospective Studies, Middle Aged, Ranitidine, Somatostatin, Omeprazole

Abstract

In a randomized, controlled clinical trial omeprazole was compared with ranitidine plus somatostatin in the treatment of severe acute gastrointestinal bleeding due to peptic pathology. Intravenous infusion of the drugs was administered until clinical stabilization or surgical operation. The two regimens were equally effective in controlling bleeding. The need for blood transfusion and surgical operation together with the mortality rate did not differ significantly between groups. No toxic effects were observed as a result of the infusion of omeprazole. In this study the infusion of omeprazole alone showed an efficacy comparable to the association of ranitidine and somatostatin in the treatment of severe acute peptic bleeding.

Published

1994

21. [Ultrasonic diagnosis of gastroduodenal perforation]

Author

P V, Lippolis, G, Ghiselli, F, Sidoti, and O, Goletti

Subjects

Adult, Aged, 80 and over, Male, Radiography, Duodenal Ulcer, Peptic Ulcer Perforation, Humans, Female, Stomach Ulcer, Middle Aged, Aged, Ultrasonography

Abstract

Ultrasonography (US) is routinely used as a diagnostic approach in the surgical acute abdomen, even though its major limitation is the demonstration of the hollow viscus. In the present paper, the results obtained with US in 12 cases of gastric or duodenal perforations are reported. The diagnosis, of gastroduodenal perforation was correctly made in 58% of cases by means of US; in 91.7% of cases, at least one US finding correlable with gastroduodenal perforation was observed. Even though US exhibits poorer diagnostic sensitivity than conventional radiology, it can be considered a valuable diagnostic tool in the early diagnosis of gastroduodenal perforation especially when radiographic findings are negative.

Published

1992

22. Subcutaneous seeding after percutaneous ethanol injection of liver metastasis

Author

M Pucciarelli, Andrea Bertolucci, F Sidoti, Massimo Chiarugi, Massimo Seccia, F. De Negri, and Orlando Goletti

Subjects

medicine.medical_specialty, Skin Neoplasms, medicine.medical_treatment, Adenocarcinoma, Injections, Intralesional, Metastasis, Neoplasm Seeding, Biopsy, Humans, Medicine, Radiology, Nuclear Medicine and imaging, Subcutaneous metastasis, Aged, Chemotherapy, Ethanol, medicine.diagnostic_test, business.industry, Liver Neoplasms, Neoplasms, Second Primary, medicine.disease, Surgery, Needle track, Female, Radiology, Percutaneous ethanol injection, Complication, business

Abstract

A 72-year-old cirrhotic woman underwent percutaneous ethanol injection treatment of a liver metastasis of unknown origin. A subcutaneous metastasis developed at the site of the punctures. Needle track seeding is a rare complication of fine-needle biopsy but has never--to the authors' knowledge--been reported after percutaneous ethanol injection. The possible causes of this complication are discussed.

23. Maribavir treatment for resistant cytomegalovirus disseminated disease in kidney transplant recipients: A case-based scoping review of real life data in literature.

Author

Corcione S, Lupia T, Vita D, Sidoti F, Zanotto E, Solidoro P, Biancone L, Costa C, Balagna R, and De Rosa FG

Subjects

Humans, Female, Middle Aged, Drug Resistance, Viral, Cytomegalovirus, Dichlororibofuranosylbenzimidazole analogs & derivatives, Cytomegalovirus Infections drug therapy, Cytomegalovirus Infections virology, Kidney Transplantation, Antiviral Agents therapeutic use, Ribonucleosides therapeutic use, Benzimidazoles therapeutic use

Abstract

The treatment of refractory CMV is often associated with high toxicity. Maribavir (MBV) is a novel oral antiviral, known for its favourable safety profile in fragile patients. We describe a case of CMV disease with end organ damage following kidney transplantation at high risk, for recipient-donor serological mismatch. A 54-year-old female with history of obesity, hypertension, and chronic kidney disease, on prednisone and tacrolimus after kidney transplantation in November 2022, soon after developed primary CMV infection, treated with Valganciclovir and CMV Ig. In January 2023 the patient presented with fever and dyspnea. Pulmonary miliary opacities and right-upper lobe consolidation were found at CT-scan along with CMV-DNA positivity on BAL and serum. Lung biopsy confirmed CMV infection. Antiviral was switched to Ganciclovir. Despite initial benefit, fever and respiratory failure happened 8 days later, leading to intubation at day 15. Due to slow decrease serum CMV-DNA and detection of UL97 mutation, conferring resistance to valganciclovir and ganciclovir, the patient was started on foscarnet and letermovir. She was extubated after a gradual respiratory improvement and discharged from ICU to rehabilitation department with HFNC; reduction in serum CMV-DNA, but persistently elevated CMV-DNA on BAL were documented. At week 8, MBV was started and letermovir continued, for a 8 weeks course, without notable adverse effects. Respiratory function improved but soon after septic shock occurred. A bone marrow biopsy resulted in lymphoma, without indications for treatment: the patient developed coma and died 6 months after admission. MBV has recently been approved in Europe for treatment of R/R CMV in HSCT and SOT recipients. MBV showed superior rates of viraemia clearance after 8 weeks compared to SOC, demonstrating also a favourable safety profile with fewer patients discontinuing treatment and being affected by nephrotoxicity and neutropenia. Its main side effects are taste impairment, gastro-intestinal symptoms and asthenia. Based on actual promising perspectives regarding antiviral stewardship, more data are required to corroborate benefit of MBV in terms of toxicity and impact on mortality in highly fragile populations as SOT recipients. MBV received approval for the treatment of refractory or resistant CMV infections to other antiviral agents. Nevertheless, real-life data on efficacy and safety of MBV are still lacking. We conducted a narrative review of the current literature on MBV as treatment for CMV infection in kidney transplant recipients to understand clinical characteristics, safety and outcomes of MBV in this population. A search was run on the main scientific databases. 194 papers were identified, of which 188 were excluded by title and abstract evaluation. Subsequently, 6 papers were included. We performed descriptive statistics on the entire study population. The studies included in our analysis showed a higher prevalence of male subjects. The median age was 57 year. CKD was the most frequently reported comorbidity. Seven patients reported a donor/recipient mismatch (D+/R-). The case report and the cohort of patients collected from the literature show that MBV was used as an option in R/R CMV, notably for the presence or suspicion of CMV resistance to previous treatment. The clinical presentation of CMV in kidney SOT was heterogenous and varied from isolated reactivation of CMV-DNAemia, isolated fever or gastrointestinal involvement. For mild to moderate CMV disease, as with the cases reported in our review, or for proven ganciclovir, foscarnet or cidofovir resistance, MBV could be a valuable option. Outcomes of the patients treated with MBV were not reported in all the studies; however, where reported, 45.4% of the cases developed virological failure during MBV treatment with the development of specific resistance to MBV. MBV was generally well-tolerated, with low rates of toxicity, normally reversible. The introduction of new oral antivirals, such as MBV, could improve treatment, prophylaxis and preemptive treatment strategies, especially in anti-CMV treatment experienced patients., Competing Interests: Declaration of competing interest All the authors report no conflicts of interest., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

24. QuantiFERON CMV Test and CMV Serostatus in Lung Transplant: Stratification Risk for Infection, Chronic and Acute Allograft Rejection.

Author

Solidoro P, Sciarrone F, Sidoti F, Patrucco F, Zanotto E, Boffini M, Rinaldo RF, Bondi A, Albera C, Curtoni A, and Costa C

Subjects

Humans, Male, Female, Middle Aged, Adult, Aged, Interferon-gamma blood, CD8-Positive T-Lymphocytes immunology, Allografts, Interferon-gamma Release Tests methods, Chronic Disease, Lung Transplantation adverse effects, Cytomegalovirus Infections diagnosis, Cytomegalovirus Infections immunology, Graft Rejection diagnosis, Cytomegalovirus immunology

Abstract

The QuantiFERON CMV (QCMV) test evaluates specific adaptive immune system activity against CMV by measuring IFN-γ released by activated CD8+ T lymphocytes. We aimed to evaluate the QCMV test as a predictive tool for CMV manifestations and acute or chronic lung allograft rejection (AR and CLAD) in lung transplant (LTx) patients. A total of 73 patients were divided into four groups based on donor and recipient (D/R) serology for CMV and QCMV assay: group A low-risk for CMV infection and disease (D-/R-); group B and C at intermediate-risk (R+), group B with non-reactive QCMV and group C with reactive QCMV; group D at high-risk (D+/R-). Group D patients experienced higher viral replication; no differences were observed among R+ patients of groups B and C. D+/R- patients had a higher number of AR events and group C presented a lower incidence of AR. Prevalence of CLAD at 24 months was higher in group B with a higher risk of CLAD development (OR 6.33). The QCMV test allows us to identify R+ non-reactive QCMV population as the most exposed to onset of CLAD. This population had a higher, although non-significant, susceptibility to AR compared to the R+ population with reactive QCMV.

Published

2024

25. Molecular diagnosis of Cytomegalovirus infection: clinical performance of the Aptima transcription-mediated amplification assay toward conventional qPCR chemistry on whole blood samples.

Author

Bottino P, Pastrone L, Zanotto E, Sidoti F, Cavallo R, and Costa C

Subjects

Humans, Polymerase Chain Reaction methods, Cytomegalovirus genetics, Immunocompromised Host, DNA, Viral genetics, Viremia, Cytomegalovirus Infections

Abstract

Human Cytomegalovirus (HCMV) infection is life-threatening for immunocompromised patients. Quantitative molecular assays on whole blood or plasma are the gold standard for the diagnosis of invasive HCMV infection and for monitoring antiviral treatment in individuals at risk of HCMV disease. For these reasons, an accurate standardization toward the WHO 1st International Standard among different centers and diagnostic kits represents an effort for better clinical management of HCMV-positive patients. Herein, we evaluate, for the first time, the performance of a new transcription-mediated amplification (TMA) assay versus quantitative polymerase chain reaction (qPCR) chemistry, used as a routine method, on whole blood samples. A total of 755 clinical whole blood specimens were collected and tested simultaneously with TMA and qPCR assays. The data showed a qualitative agreement of 99.27% for positive quantified samples and 89.39% for those undetected between the two tested methods. Evaluation of viremia in positive samples highlighted a good correlation between TMA and qPCR chemistries in terms of International Units (ΔLog 10 IU/mL: -0.29 ± 0.40). The TMA assay showed a significant correlation with qPCR in patients monitored for up to 3 months, thus allowing an accurate assessment of viremia in transplant patients. Therefore, TMA chemistry showed good agreement with qPCR testing, used as a current diagnostic routine. It also offers important advantages, such as FDA approval on plasma and In Vitro Diagnostic (IVD) on both plasma and whole blood, automated workflow with minimal hands-on time, and random access loading, thus enabling a rapid and reliable diagnostic in HCMV-infected patients., Importance: In this paper, we describe the clinical performance of a novel transcription-mediated amplification (TMA) assay for the detection and quantification of human Cytomegalovirus (HCMV) DNA from whole blood samples. This is a pivotal analysis in immunocompromised patients [transplanted, HIV-positive, and Hematopoietic Stem Cell (HSC) recipients], and molecular tests with high sensitivity and specificity are necessary to evaluate the HCMV viral load in these patients. To our knowledge, this is the first in-depth evaluation of TMA chemistry for HCMV diagnosis on whole blood samples. Moreover, also technical aspects of this assay make it suitable for clinical diagnostics., Competing Interests: The authors declare no conflict of interest.

Published

2024

26. Automatic 3D Augmented-Reality Robot-Assisted Partial Nephrectomy Using Machine Learning: Our Pioneer Experience.

Author

Piana A, Amparore D, Sica M, Volpi G, Checcucci E, Piramide F, De Cillis S, Busacca G, Scarpelli G, Sidoti F, Alba S, Piazzolla P, Fiori C, Porpiglia F, and Di Dio M

Abstract

The aim of "Precision Surgery" is to reduce the impact of surgeries on patients' global health. In this context, over the last years, the use of three-dimensional virtual models (3DVMs) of organs has allowed for intraoperative guidance, showing hidden anatomical targets, thus limiting healthy-tissue dissections and subsequent damage during an operation. In order to provide an automatic 3DVM overlapping in the surgical field, we developed and tested a new software, called "ikidney", based on convolutional neural networks (CNNs). From January 2022 to April 2023, patients affected by organ-confined renal masses amenable to RAPN were enrolled. A bioengineer, a software developer, and a surgeon collaborated to create hyper-accurate 3D models for automatic 3D AR-guided RAPN, using CNNs. For each patient, demographic and clinical data were collected. A total of 13 patients were included in the present study. The average anchoring time was 11 (6-13) s. Unintended 3D-model automatic co-registration temporary failures happened in a static setting in one patient, while this happened in one patient in a dynamic setting. There was one failure; in this single case, an ultrasound drop-in probe was used to detect the neoplasm, and the surgery was performed under ultrasound guidance instead of AR guidance. No major intraoperative nor postoperative complications (i.e., Clavien Dindo > 2) were recorded. The employment of AI has unveiled several new scenarios in clinical practice, thanks to its ability to perform specific tasks autonomously. We employed CNNs for an automatic 3DVM overlapping during RAPN, thus improving the accuracy of the superimposition process.

Published

2024

27. Anti-CD38 targeted nanotrojan horses stimulated by acoustic waves as therapeutic nanotools selectively against Burkitt's lymphoma cells.

Author

Vighetto V, Conte M, Rosso G, Carofiglio M, Sidoti Abate F, Racca L, Mesiano G, and Cauda V

Abstract

The horizon of nanomedicine research is moving toward the design of therapeutic tools able to be completely safe per se, and simultaneously be capable of becoming toxic when externally activated by stimuli of different nature. Among all the stimuli, ultrasounds come to the fore as an innovative approach to produce cytotoxicity on demand in presence of NPs, without invasiveness, with high biosafety and low cost. In this context, zinc oxide nanoparticles (NPs) are among the most promising metal oxide materials for theranostic application due to their optical and semi-conductor properties, high surface reactivity, and their response to ultrasound irradiation. Here, ZnO nanocrystals constitute the stimuli-responsive core with a customized biomimicking lipidic shielding, resembling the composition of natural extracellular vesicles. This core-shell hybrid structure provides high bio- and hemocompatibility towards healthy cells and is here proofed for the treatment of Burkitt's Lymphoma. This is a very common haematological tumor, typically found in children, for which consolidated therapies are so far the combination of chemo-therapy drugs and targeted immunotherapy. In this work, the proposed safe-by-design antiCD38-targeted hybrid nanosystem exhibits an efficient selectivity toward cancerous cells, and an on-demand activation, leading to a significant killing efficacy due to the synergistic interaction between US and targeted hybrid NPs. Interestingly, this innovative treatment does not significantly affect healthy B lymphocytes nor a negative control cancer cell line, a CD38- acute myeloid leukemia, being thus highly specific and targeted. Different characterization and analyses confirmed indeed the effective formation of targeted hybrid ZnO NPs, their cellular internalization and the damages produced in Burkitt's Lymphoma cells only with respect to the other cell lines. The presented work holds promises for future clinical applications, as well as translation to other tumor types., (© 2024. The Author(s).)

Published

2024

28. Herpes Virus Infection in Lung Transplantation: Diagnosis, Treatment and Prevention Strategies.

Author

Patrucco F, Curtoni A, Sidoti F, Zanotto E, Bondi A, Albera C, Boffini M, Cavallo R, Costa C, and Solidoro P

Subjects

Humans, Herpesvirus 4, Human, Herpesvirus 3, Human, Simplexvirus, Epstein-Barr Virus Infections, Herpesviridae Infections diagnosis, Herpesviridae Infections epidemiology, Herpesviridae Infections prevention & control, Lung Transplantation adverse effects, Herpes Zoster complications

Abstract

Lung transplantation is an ultimate treatment option for some end-stage lung diseases; due to the intense immunosuppression needed to reduce the risk of developing acute and chronic allograft failure, infectious complications are highly incident. Viral infections represent nearly 30% of all infectious complications, with herpes viruses playing an important role in the development of acute and chronic diseases. Among them, cytomegalovirus (CMV) is a major cause of morbidity and mortality, being associated with an increased risk of chronic lung allograft failure. Epstein-Barr virus (EBV) is associated with transformation of infected B cells with the development of post-transplantation lymphoproliferative disorders (PTLDs). Similarly, herpes simplex virus (HSV), varicella zoster virus and human herpesviruses 6 and 7 can also be responsible for acute manifestations in lung transplant patients. During these last years, new, highly sensitive and specific diagnostic tests have been developed, and preventive and prophylactic strategies have been studied aiming to reduce and prevent the incidence of these viral infections. In this narrative review, we explore epidemiology, diagnosis and treatment options for more frequent herpes virus infections in lung transplant patients.

Published

2023

29. Robot-Assisted Radical Prostatectomy in Renal Transplant Recipients: A Systematic Review.

Author

Piana A, Pecoraro A, Sidoti F, Checcucci E, Dönmez Mİ, Prudhomme T, Bañuelos Marco B, López Abad A, Campi R, Boissier R, Di Dio M, Porpiglia F, Breda A, and Territo A

Abstract

Robot-assisted radical prostatectomy (RARP) has been shown to achieve excellent oncological outcomes with a low rate of complications in patients with prostate cancer. However, data on RARP in renal transplant recipients (RT) are dispersed. A literature search was conducted through April 2023 using PubMed/Medline, Embase and Web of Science databases. The primary aim was to evaluate the safety, oncologic and clinical outcomes of RARP in RT recipients. The secondary aim was to identify surgical technique modifications required to avoid iatrogenic damage to the transplanted kidney. A total of 18 studies comprising 186 patients met the inclusion criteria. Age at the time of treatment ranged 43-79 years. Biopsy results showed a high prevalence of low- and intermediate-risk disease. Operative time ranged between 108.3 and 400 mins, while estimated blood loss ranged from 30 to 630 mL. Length of hospital stay ranged from 3 to 6 days whereas duration of catheterization was between 5 and 18 days. Perioperative complication rate was 17.1%. Overall positive surgical margin rate was 24.19%, while biochemical recurrence was observed in 10.21% (19/186 patients). Modifications to the standard surgical technique were described in 13/18 studies. Modifications in port placement were described in 7/13 studies and performed in 19/88 (21.6%) patients. Surgical technique for the development of the Retzius space was reported in 13/18 studies. Data on lymphadenectomy were reported in 15/18 studies. Bilateral lymphadenectomy was described in 3/18 studies and performed in 4/89 (4.5%) patients; contralateral lymphadenectomy was reported in 7/18 studies and performed in 41/125 (32.8%) patients. RARP in RTRs can be considered relatively safe and feasible. Oncological results yielded significantly worse outcomes in terms of PSM and BCR rate compared to the data available in the published studies, with an overall complication rate highly variable among the studies included. On the other hand, low graft damage during the procedure was observed. Main criticisms came from different tumor screening protocols and scarce information about lymphadenectomy techniques and outcomes among the included studies.

Published

2023

30. Antiviral Approach to Cytomegalovirus Infection: An Overview of Conventional and Novel Strategies.

Author

Bottino P, Pastrone L, Curtoni A, Bondi A, Sidoti F, Zanotto E, Cavallo R, Solidoro P, and Costa C

Abstract

Human cytomegalovirus (HCMV) is a herpesvirus capable of establishing a lifelong persistence in the host through a chronic state of infection and remains an essential global concern due to its distinct life cycle, mutations, and latency. It represents a life-threatening pathogen for immunocompromised patients, such as solid organ transplanted patients, HIV-positive individuals, and hematopoietic stem cell recipients. Multiple antiviral approaches are currently available and administered in order to prevent or manage viral infections in the early stages. However, limitations due to side effects and the onset of antidrug resistance are a hurdle to their efficacy, especially for long-term therapies. Novel antiviral molecules, together with innovative approaches (e.g., genetic editing and RNA interference) are currently in study, with promising results performed in vitro and in vivo. Since HCMV is a virus able to establish latent infection, with a consequential risk of reactivation, infection management could benefit from preventive treatment for critical patients, such as immunocompromised individuals and seronegative pregnant women. This review will provide an overview of conventional antiviral clinical approaches and their mechanisms of action. Additionally, an overview of proposed and developing new molecules is provided, including nucleic-acid-based therapies and immune-mediated approaches.

Published

2023

31. Extraction Bottleneck in the Diagnosis of SARS-CoV-2: Evaluation of an Alternative Protocol Derived from Veterinary Use.

Author

Bottino P, Zanotto E, Sidoti F, Pastrone L, Piva R, Mereu E, Costa C, and Cavallo R

Abstract

The COVID-19 pandemic represented a challenge for health-care systems, and a major bottleneck in SARS-CoV-2 diagnosis was the unavailability of extraction reagents. To overcome this limitation, we performed a comparative analysis to evaluate the performance of an alternative extraction protocol derived from veterinary use adapted to an open robotic platform (Testing method). A total of 73 nasopharyngeal swabs collected for diagnosis of SARS-CoV-2 infection were simultaneously extracted with the Testing protocol and the laboratory Standard of Care in order to assess the performance of the first one. The Cohen's coefficient between both procedures was excellent (K Value = 0.955). Analysis of cycle threshold and linear regression showed a significant correlation between the two methods for each tested genetic target. Although validated for veterinary applications, the Testing method showed excellent performances in RNA extraction, with several advantages: lower sample input volume, the possibility to overcome the lack of deep-well plates and adaptability to robotic liquid handlers.

Published

2023

32. SARS-CoV-2 infection in a stem cell transplant recipient grafted from a SARS-CoV-2-positive donor.

Author

Busca A, Gabrielli G, Sidoti F, Costa C, Giaccone L, Dogliotti I, Dellacasa CM, Francisci T, Pecoraro C, Ruggeri M, Cavallo R, and De Rosa F

Subjects

Humans, SARS-CoV-2, Stem Cell Transplantation adverse effects, Tissue Donors, Transplant Recipients, COVID-19

Published

2022

33. Clinical features of respiratory syncytial virus bronchiolitis in an infant: rapid and fatal brain involvement.

Author

Bottino P, Miglino R, Pastrone L, Barbui AM, Botta G, Zanotto E, Sidoti F, Costa C, and Cavallo R

Subjects

Brain diagnostic imaging, Humans, Infant, Lung, Male, Respiratory Syncytial Viruses, Bronchiolitis diagnosis, Respiratory Syncytial Virus Infections complications, Respiratory Syncytial Virus Infections diagnosis

Abstract

Background: Respiratory Syncytial Virus (RSV) infection is a significant cause of bronchiolitis and pneumonia, mostly responsible for hospitalization and infant death worldwide. However, in recent years the importance of extrapulmonary RSV manifestations, especially at neurological level, have become evident. Seizures, lethargy, ataxia and status epilepticus are suggestive of brain involvement, but also in their absence a direct neurological damage RSV-related need to be evaluated., Case Presentation: A 40-day old male infant was admitted to the Emergency Department with severe bronchiolitis and dyspnea. The patient was reported to be coughing for a week with a vomiting episode in the previous two days. The nasopharyngeal swab confirmed the diagnosis of RSV infection and blood gas test showed hypoxemia and respiratory acidosis. For these reasons, the patient was provided with oxygen therapy. A few hours later, after an initial improvement in clinical parameters, a worsening of respiratory dynamics occurred and the patient was prepared for endotracheal intubation, but in the meantime death occurred. During all the observation period in the Emergency Room, no signs of neuropathological damage were evident. Post mortem examination showed lungs congestion with alveolar atelectasis and white matter degradation with severe edema at brain level. Microbiological analysis performed on autoptic samples confirmed the presence of RSV genome in tracheobronchial aspirate, meningeal swabs, pericardic and abdominal fluids, lung and brain biopsies., Conclusions: RSV is usually associated with respiratory diseases, however, as reported by an increasingly number of studies, the systemic dissemination of virus during severe disease can lead to a sudden infant death. The clinical picture herein reported showed a severe bronchiolitis resulting in a fatal and underestimated cerebral involvement due to RSV neurotropic behaviour and underline the need for clinicians to pay more attention to neurological involvement of RSV infection, even in absence of cerebral damage evidence., (© 2021. The Author(s).)

Published

2021

34. Detection of Carbapenemase and CTX-M Encoding Genes Directly from Bronchoalveolar Lavage Using the CRE and ESBL ELITe MGB Assays: Toward Early and Optimal Antibiotic Therapy Management of Critically Ill Patients with Pneumonia.

Author

Boattini M, Bianco G, Iannaccone M, Zanotto E, Sidoti F, Almeida A, De Rosa FG, Cavallo R, and Costa C

Subjects

Bronchoalveolar Lavage methods, Carbapenem-Resistant Enterobacteriaceae genetics, Critical Illness, Enterobacteriaceae Infections drug therapy, Enterobacteriaceae Infections microbiology, Genotype, Humans, Microbial Sensitivity Tests methods, Pneumonia microbiology, Retrospective Studies, Anti-Bacterial Agents pharmacology, Bacterial Proteins genetics, Pneumonia drug therapy, beta-Lactamases genetics

Abstract

The detection of carbapenemase extended-spectrum β-lactamase (ESBL)-producing Enterobacterales (EB) has become a major issue among critically ill patients, especially due to their impact on appropriate antimicrobial therapy. This study aimed at evaluating the potential contribution of molecular assays to early optimization of empirical antibiotic therapy among critically ill patients with carbapenemase- and/or CTX-M-producing EB pneumonia. The CRE and ESBL ELITe MGB ® assays were evaluated directly on 197 bronchoalveolar lavage (BAL) samples obtained from 120 patients. Molecular results were then compared to routine culture-based diagnostic results, and a retrospective analysis of the therapeutic antimicrobial management was performed. Among the 197 clinical specimens, bla KPC-like and bla CTX-M-like were detected in 20 (10.2%) and 12 (6.1%) specimens belonging to 15 and 11 patients, respectively. Positive predictive value (PPV) and negative predictive value (NPV) of the CRE ELITe MGB Kit were 85% [95% confidence interval [CI]: 64.9-94.6] and 100%, respectively. PPV and NPV of the ESBL ELITe MGB Kit were 75% [95% CI: 49.4-90.2] and 100%, respectively. Retrospective analysis of the therapeutic antimicrobial management at the time of BAL collection showed that in ∼50% of patients with carbapenemase- and CTX-M-producing EB pneumonia empirical antibiotic therapy could have been optimized at least 48-72 hr earlier if positive molecular data had been used. The CRE and ESBL ELITe MGB assays might be an interesting tool for expediting optimization of empirical antibiotic therapy in critically ill patients with pneumonia, depending on local epidemiology of antibiotic resistance, patient risk stratification for EB infection, and availability of an antimicrobial stewardship team.

Published

2021

35. Renal Allograft Biopsies with Polyomavirus BK Nephropathy: Turin Transplant Center, 2015-19.

Author

Zanotto E, Allesina A, Barreca A, Sidoti F, Gallo E, Bottino P, Iannaccone M, Bianco G, Biancone L, Cavallo R, and Costa C

Subjects

Adult, Aged, Aged, 80 and over, Allografts, BK Virus, Biopsy, Female, Humans, Immunosuppression Therapy, Immunosuppressive Agents therapeutic use, Kidney pathology, Kidney virology, Kidney Diseases drug therapy, Kidney Diseases pathology, Kidney Diseases virology, Male, Middle Aged, Polyomavirus Infections drug therapy, Polyomavirus Infections pathology, Polyomavirus Infections virology, Risk Factors, Transplantation, Homologous, Tumor Virus Infections complications, Viral Load, Young Adult, Kidney Diseases complications, Kidney Transplantation, Polyomavirus, Polyomavirus Infections complications

Abstract

Background: In kidney transplant patients, polyomavirus-associated nephropathy (PVAN) represents a serious complication; the key factor for the development of PVAN is immunosuppression level and modulation of anti-rejection treatment represents the first line of intervention. Allograft biopsy and histology remain the criterion standard for diagnosing PVAN., Methods: All consecutive renal biopsies with the diagnosis of PVAN carried out at the University Hospital City of Health and Science of Turin over a five-years period were studied. Renal allograft biopsy was performed due to renal function alterations associated to medium-high polyomavirus BK (BKV)-DNA levels on plasma specimen., Results: A total of 21 patients underwent a first biopsy to diagnose a possible BKV nephropathy, in 18, a second biopsy was made, in eight, a third biopsy, and finally, three underwent the fourth renal biopsy; following the results of each biopsies, immunosuppressant agents dosages were modified in order to reduce the effect of PVAN., Conclusions: In this study, the clinical and histological features of 21 kidney transplant recipients with BKV reactivation and development of PVAN are described. To date, the only treatment for PVAN consists in the reduction of immunosuppressive agents, constantly monitoring viral load.

Published

2020

36. Controlled ovarian stimulation and progesterone supplementation affect vaginal and endometrial microbiota in IVF cycles: a pilot study.

Author

Carosso A, Revelli A, Gennarelli G, Canosa S, Cosma S, Borella F, Tancredi A, Paschero C, Boatti L, Zanotto E, Sidoti F, Bottino P, Costa C, Cavallo R, and Benedetto C

Subjects

Adult, Embryo Transfer, Endometrium metabolism, Endometrium pathology, Female, Humans, Ovulation Induction adverse effects, Phylogeny, Pregnancy, Progesterone administration & dosage, RNA, Ribosomal, 16S genetics, Sperm Injections, Intracytoplasmic, Vagina metabolism, Vagina pathology, Endometrium microbiology, Fertilization in Vitro, Microbiota genetics, Vagina microbiology

Abstract

Purpose: Does controlled ovarian stimulation (COS) and progesterone (P) luteal supplementation modify the vaginal and endometrial microbiota of women undergoing in vitro fertilization?, Methods: Fifteen women underwent microbiota analysis at two time points: during a mock transfer performed in the luteal phase of the cycle preceding COS, and at the time of fresh embryo transfer (ET). A vaginal swab and the distal extremity of the ET catheter tip were analyzed using next-generation 16SrRNA gene sequencing. Heterogeneity of the bacterial microbiota was assessed according to both the Bray-Curtis similarity index and the Shannon diversity index., Results: Lactobacillus was the most prevalent genus in the vaginal samples, although its relative proportion was reduced by COS plus P supplementation (71.5 ± 40.6% vs. 61.1 ± 44.2%). In the vagina, an increase in pathogenic species was observed, involving Prevotella (3.5 ± 8.9% vs. 12.0 ± 19.4%), and Escherichia coli-Shigella spp. (1.4 ± 5.6% vs. 2.0 ± 7.8%). In the endometrium, the proportion of Lactobacilli slightly decreased (27.4 ± 34.5% vs. 25.0 ± 29.9%); differently, both Prevotella and Atopobium increased (3.4 ± 9.5% vs. 4.7 ± 7.4% and 0.7 ± 1.5% vs. 5.8 ± 12.0%). In both sites, biodiversity was greater after COS (p < 0.05), particularly in the endometrial microbiota, as confirmed by Bray-Curtis analysis of the phylogenetic distance among bacteria genera. Bray-Curtis analysis confirmed significant differences also for the paired endometrium-vagina samples at each time point., Conclusions: Our findings suggest that COS and P supplementation significantly change the composition of vaginal and endometrial microbiota. The greater instability could affect both endometrial receptivity and placentation. If our findings are confirmed, they may provide a further reason to encourage the freeze-all strategy.

Published

2020

37. Kinetics of cytomegalovirus and Epstein-Barr virus DNA in whole blood and plasma of kidney transplant recipients: Implications on management strategies.

Author

Lazzarotto T, Chiereghin A, Piralla A, Gibertoni D, Piccirilli G, Turello G, Campanini G, Gabrielli L, Costa C, Comai G, La Manna G, Biancone L, Rampino T, Gregorini M, Sidoti F, Bianco G, Mauro MV, Greco F, Cavallo R, and Baldanti F

Subjects

Adult, Antiviral Agents pharmacology, Cohort Studies, Cytomegalovirus drug effects, Cytomegalovirus physiology, Herpesvirus 4, Human drug effects, Herpesvirus 4, Human physiology, Humans, Immunosuppressive Agents pharmacology, Kinetics, Retrospective Studies, Cytomegalovirus genetics, DNA, Viral blood, Herpesvirus 4, Human genetics, Kidney Transplantation

Abstract

This retrospective multicenter cohort study investigated the kinetics (ascending and descending phases) of cytomegalovirus (CMV) and Epstein-Barr virus (EBV)-DNA in whole blood (WB) and plasma samples collected from adult kidney transplant (KT) recipients. CMV-DNA kinetics according to antiviral therapy were investigated. Three hundred twenty-eight paired samples from 42 episodes of CMV infection and 157 paired samples from 26 episodes of EBV infection were analyzed by a single commercial molecular method approved by regulatory agencies for both matrices. CMV-DNAemia followed different kinetics in WB and plasma. In the descending phase of infection, a slower decay of viral load and a higher percentage of CMV-DNA positive samples were observed in plasma versus WB. In the 72.4% of patients receiving antiviral therapy, monitoring with plasma CMV-DNAemia versus WB CMV-DNAemia could delay treatment interruption by 7-14 days. Discontinuation of therapy based on WB monitoring did not result in relapsed infection in any patients. Highly different EBV-DNA kinetics in WB and plasma were observed due to lower positivity in plasma; EBV positive samples with a quantitative result in both blood compartments were observed in only 11.5% of cases. Our results emphasize the potential role of WB as specimen type for post-KT surveillance of both infections for disease prevention and management., Competing Interests: The supporting source (i.e. Qiagen S.r.l., Italy) of the study is a commercial source. This does not alter our adherence to PLOS ONE policies on sharing data and materials.

Published

2020

38. Evaluation of CMV DNA in dried blood spot.

Author

Bottino P, Balloco C, Rittà M, Bianco G, Sidoti F, Cavallo R, and Costa C

Subjects

Humans, Sensitivity and Specificity, Serologic Tests, Viral Load, Cytomegalovirus genetics, Cytomegalovirus Infections diagnosis, Cytomegalovirus Infections virology, DNA, Viral chemistry, Dried Blood Spot Testing standards

Abstract

Cytomegalovirus is the primary viral cause of congenital infection. However, diagnosis may be difficult for clinical and technical reasons. Currently, evaluation of CMV DNA on dried blood spot (DBS) is an important instrument to define a congenital infection. The aim of this study was to identify a clinically and technically suitable diagnostic work-flow for CMV DNA evaluation on DBS. Sensitivity was not significantly influenced by storage time of up to 12 months and extraction technique; however, analysis in triplicate was crucial to obtain reliable results. Considering viral load in an infected foetus at risk of developing disease, a threshold value of approximately 104 copies/mL was characterized by high operating characteristics for detection of positivity at 12 months on DBS.

Published

2020

39. Collaborative national multicenter for the identification of conversion factors from copies/mL to international units/mL for the normalization of HCMV DNA load.

Author

Sidoti F, Piralla A, Costa C, Scarasciulli ML, Calvario A, Conaldi PG, Paba P, Perno CF, Gaeta A, Antonelli G, Sodano G, Santangelo R, Sanguinetti M, Vatteroni ML, Barzon L, Palù G, Abbate I, Capobianchi MR, Piccirilli G, Lazzarotto T, Baldanti F, and Cavallo R

Subjects

Cytomegalovirus genetics, Cytomegalovirus Infections blood, Cytomegalovirus Infections virology, DNA, Viral genetics, Humans, Nucleic Acid Amplification Techniques standards, Reference Standards, Reproducibility of Results, World Health Organization, Cytomegalovirus isolation & purification, Cytomegalovirus Infections diagnosis, DNA, Viral blood, Viral Load methods, Viral Load standards

Abstract

The present multicentric (n = 11 laboratories) study aimed to identify conversion factors from copies/mL to international units (IU)/mL for the normalization of HCMV DNA load using the first WHO International Standard for HCMV nucleic acid amplification techniques and to enhance interlaboratory agreement of HCMV DNA quantification methods. Study protocols for whole blood and plasma (extraction and amplification) were performed to calculate conversion factors from HCMV DNA copy number to IU. The greatest variability was observed in samples with lower HCMV concentrations (3.0 Log 10 ) in both biological matrices. Overall, 73.1% (206/282) of whole blood and 82.2% (324/394) of plasma samples analyzed fell within an acceptable variation range (±0.5 Log 10 difference). An average of 0.64 (range 0.21-1.17) was the conversion factor calculated for the HCMV whole blood panel and 0.82 (range 0.39-2.2) for the HCMV plasma panel., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

40. Recurrent herpes labialis and Herpes simplex virus-1 genitalis: what is the link?

Author

Delmonte S, Sidoti F, Ribero S, Dal Conte I, Curtoni A, Ciccarese G, Stroppiana E, Stella ML, Costa C, Cavallo R, Rebora A, and Drago F

Subjects

Adolescent, Adult, DNA, Viral analysis, Female, Herpes Genitalis epidemiology, Herpes Labialis epidemiology, Herpesvirus 1, Human isolation & purification, Herpesvirus 2, Human isolation & purification, Humans, Italy, Male, Recurrence, Risk Factors, Seroepidemiologic Studies, Sexual Partners, Sexually Transmitted Diseases epidemiology, Sexually Transmitted Diseases virology, Young Adult, Antibodies, Viral analysis, Herpes Genitalis diagnosis, Herpes Labialis diagnosis, Sexually Transmitted Diseases diagnosis

Abstract

Background: Recently, Herpes simplex virus (HSV)-1 seroprevalence declined among adolescents, rendering young people lacking HSV-1 antibodies more susceptible to genital HSV-1 acquisition, if sexually exposed. The aim of the present study was to identify the possible risk factors for the development of HSV-1 related Herpes genitalis (HG)., Methods: From January 2012 to December 2015, patients with HG attending three Sexually Transmitted Infections Units in Northern Italy were recruited. A genital swab on the lesions for the search of HSV-1/2 DNA through real time polymerase chain reaction (PCR) and a serum sample for HSV-1/2 specific serology were performed. Moreover, patients were asked whether they had personal history of herpes labialis (HL). Patients with PCR proved HSV-1 HG were included as cases; asymptomatic subjects attending STI Units for a blood check were recruited as controls and were checked for HSV-1/2 serology., Results: The study included 141 cases and 70 controls. Specific HSV-1 antibodies were found in 34.7% of the cases and 67% of the controls. History of recurrent herpes labialis (RHL) was found in 4% of the cases and 31% of the controls. The occurrence of RHL in HSV-1 seropositive patients resulted lower in the case group compared to the control group., Conclusions: We can speculate about a protective role for RHL against the clinical appearance of HSV-1 HG. The clinical usefulness of our study involved especially the counselling in serodiscordant couples. The presence of HSV-1 antibodies in asymptomatic sexual partners does appear protective for HG manifestation only in presence of RHL history.

Published

2019

41. Detection of antibiotic resistance genes from blood cultures: performance assessment and potential impact on antibiotic therapy management.

Author

Bianco G, Boattini M, Iannaccone M, Sidoti F, Cavallo R, and Costa C

Subjects

Bacteria genetics, Bacteria growth & development, Bacteria isolation & purification, Genotype, Humans, Phenotype, Retrospective Studies, Staphylococcal Infections diagnosis, beta-Lactamases genetics, Bacteria drug effects, Blood Culture methods, Drug Resistance, Bacterial, Enterobacteriaceae Infections microbiology, Genotyping Techniques methods, Microbial Sensitivity Tests methods, Staphylococcal Infections microbiology

Abstract

Molecular assays may constitute a valid method for timely prediction of antimicrobial resistance and optimization of empirical antibiotic therapies. This study assessed ELITe MGB assays of blood cultures to detect the main carbapenemase and extended-spectrum beta-lactamase (ESBL) genes, Staphylococcus aureus and mec genes in less than 3 h. Excellent agreement was found between the results of genotypic and conventional phenotypic approaches. Retrospective analysis of medical records revealed that approximately 50% of bloodstream infections caused by ESBL-producing Enterobacteriaceae, carbapenemase-producing Enterobacteriaceae or meticillin-resistant S. aureus were initially treated with inactive drugs. Overall, 36.3% of patients could have been treated with appropriate therapy at least 24 h earlier if molecular data had been used., (Copyright © 2019 The Healthcare Infection Society. Published by Elsevier Ltd. All rights reserved.)

Published

2019

42. V348I mutation in UL23 gene of human herpesvirus 1 in a case of herpetic hepatitis and haemophagocytic lymphohistiocytosis.

Author

Corcione S, Sidoti F, Costa C, Mornese Pinna S, Bonetto C, Urbino R, Cavallo R, and De Rosa FG

Abstract

We herein report the case of a young immunocompetent adult patient with a rapidly fatal haemophagocytic lymphohistiocytosis syndrome related to human herpesvirus 1 (HHV-1) infection, with herpetic hepatitis and persistent high-level viraemia despite treatment with acyclovir. Haemophagocytic lymphohistiocytosis was confirmed in the patient's spleen and bone marrow. HHV-1 DNA was extracted from whole blood and liver biopsy and the UL23 gene was sequenced. A V348I natural polymorphism of the TK protein was found in blood and liver specimens. Further studies are needed to investigate the role of this polymorphism in the development of systemic immune dysregulation.

Published

2019

43. Serological and molecular detection of Bartonella henselae in specimens from patients with suspected cat scratch disease in Italy: A comparative study.

Author

Allizond V, Costa C, Sidoti F, Scutera S, Bianco G, Sparti R, Banche G, Dalmasso P, Cuffini AM, Cavallo R, and Musso T

Subjects

Adolescent, Adult, Aged, Bartonella henselae genetics, Bartonella henselae immunology, Cat-Scratch Disease immunology, Child, Child, Preschool, Early Diagnosis, Female, Fluorescent Antibody Technique, Indirect, Humans, Infant, Italy, Male, Middle Aged, Real-Time Polymerase Chain Reaction, Sensitivity and Specificity, Young Adult, Antibodies, Bacterial metabolism, Bartonella henselae isolation & purification, Cat-Scratch Disease diagnosis, DNA, Bacterial genetics

Abstract

Cat scratch disease (CSD) is an infectious disease caused by Bartonella henselae, usually characterized by self-limiting regional lymphadenopathy and fever. Given the low clinical diagnostic sensitivity and specificity of conventional anti-B. henselae indirect immunofluorescence assays (IFAs), real-time polymerase chain reaction (PCR)-based detection of B. henselae is now being proposed as a more sensitive tool to diagnose CSD. Thus, here we have assessed the efficacy of real-time PCR in detecting B. henselae in different specimens from patients with suspected CSD and compared it to that of IFA. From March 2011 to May 2016, at the Microbiology and Virology Unit, Azienda Ospedaliera Universitaria Città della Salute e della Scienza di Torino, Turin, Italy, 115 clinical specimens (56 aspirated pus, 39 fresh lymph node biopsies, and 20 whole blood samples) and 99 sera from 115 patients with suspected CSD (62 females and 53 males between the ages of 3 months and 68 years) were analyzed by both real-time PCR, used in a qualitative way, and IFA (IgM and IgG) for the presence of B. henselae. For 16 patients, serological results were not available due to a clinical decision not to request the test. B. henselae DNA positivity was detected by real-time PCR in 37.39% of patients, while 62.61% of them were negative. Thus, patients were divided into two groups: real-time PCR+ (n = 43) and real-time PCR- (n = 72). Real-time PCR screening of whole blood, biopsies, and aspirated pus revealed B. henselae positivity in 40%, 38.46%, and 35.71% of patients, respectively. When we analyzed samples by IFA, we found the presence of B. henselae in 28 out of 99 (28.28%) patients, of which 11 (11.11%) belonged to the real-time PCR+ group and 17 (17.17%) to the real-time PCR- group. Among the 71 seronegative subjects, 16 (16.16%) were found positive for B. henselae by real-time PCR. Thus, by combining the results of both assays, we were able to increase the percentage of B. henselae positive specimens from 27.27% (real-time PCR) or 28.28% (IFA) to 44.44% (real-time PCR+IFA). Altogether, these findings indicate that the early detection of B. henselae in patients with suspicious CSD through combined real-time PCR and serological analyses can lead to a more accurate diagnosis of CSD, thereby allowing prompt and appropriate disease management., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

44. Tailored combined cytomegalovirus management in lung transplantation: a retrospective analysis.

Author

Solidoro P, Patrucco F, Libertucci D, Verri G, Sidoti F, Curtoni A, Boffini M, Simonato E, Rinaldi M, Cavallo R, and Costa C

Subjects

Adult, Antiviral Agents adverse effects, Cytomegalovirus growth & development, Cytomegalovirus immunology, Cytomegalovirus Infections diagnosis, Cytomegalovirus Infections immunology, Cytomegalovirus Infections virology, Drug Administration Schedule, Female, Humans, Immunocompromised Host, Immunoglobulin G adverse effects, Immunosuppressive Agents adverse effects, Male, Middle Aged, Opportunistic Infections diagnosis, Opportunistic Infections immunology, Opportunistic Infections virology, Pneumonia, Viral diagnosis, Pneumonia, Viral immunology, Pneumonia, Viral virology, Retrospective Studies, Risk Factors, Time Factors, Treatment Outcome, Viral Load, Virus Replication, Antiviral Agents administration & dosage, Cytomegalovirus drug effects, Cytomegalovirus Infections prevention & control, Immunoglobulin G administration & dosage, Lung Transplantation adverse effects, Opportunistic Infections prevention & control, Pneumonia, Viral prevention & control

Abstract

Background: There is no univocal prophylactic regimen to prevent cytomegalovirus (CMV) infection/disease in lung transplantation (LT) recipients. The aim of this study is to evaluate short-term clinical outcomes of a tailored combined CMV management approach., Methods: After 1-year follow up, 43 LT patients receiving combined CMV prophylaxis with antiviral agents and CMV-specific IgG were evaluated in a retrospective observational study. Systemic and lung viral infections were investigated by molecular methods on a total of 1134 whole blood and 167 bronchoalveolar lavage (BAL) and biopsy specimens. CMV immunity was assessed by ELISPOT assay. Clinical and therapeutic data were also evaluated., Results: We found 2/167 cases of CMV pneumonia (1.2%), both in the donor-positive/recipient-positive (D + /R + ) population, and 51/167 cases of CMV pulmonary infection (BAL positivity 30.5%). However, only 32/167 patients (19.1%) were treated due to their weak immunological response at CMV ELISPOT assay. Viremia ⩾100,000 copies/mL occurred in 33/1134 specimens (2.9%). Regarding CMV-serological matching (D/R), the D + /R - population had more CMV viremia episodes ( p  < 0.05) and fewer viremia-free days ( p  < 0.001)., Conclusions: Compared to previous findings, our study shows a lower incidence of CMV pneumonia and viremia despite the presence of a substantial CMV load. In addition, our findings further confirm the D + /R - group to be a high-risk population for CMV viremia. Overall, a good immunological response seems to protect patients from CMV viremia and pneumonia but not from CMV alveolar replication. The reviews of this paper are available via the supplemental material section.

Published

2019

45. Cytomegalovirus and Epstein-Barr Virus DNA Kinetics in Whole Blood and Plasma of Allogeneic Hematopoietic Stem Cell Transplantation Recipients.

Author

Lazzarotto T, Chiereghin A, Piralla A, Piccirilli G, Girello A, Campanini G, Gabrielli L, Costa C, Prete A, Bonifazi F, Busca A, Cairoli R, Colombo AA, Zecca M, Sidoti F, Bianco G, Paba P, Perno CF, Cavallo R, and Baldanti F

Subjects

Adult, Aged, Allografts, Female, Hematopoietic Stem Cell Transplantation, Humans, Kinetics, Male, Middle Aged, Retrospective Studies, Virus Replication, Blood virology, Cytomegalovirus genetics, DNA, Viral blood, Herpesvirus 4, Human genetics, Plasma virology, Transplant Recipients

Abstract

Currently, no consensus has been reached on the optimal blood compartment to be used for surveillance of cytomegalovirus (CMV) and Epstein-Barr virus (EBV) DNAemia. Although several comparative studies have been performed correlating CMV and EBV DNA loads in whole blood (WB) versus plasma, to our knowledge, no studies to date have analyzed the kinetics of both viruses in the 2 blood compartments. In this retrospective noninterventional multicenter cohort study, the kinetics of CMV and EBV DNA in 121 hematopoietic stem cell transplantation (HSCT) recipients were investigated by analyzing in parallel 569 and 351 paired samples from 80 and 58 sequential episodes of CMV and EBV DNAemia, respectively. Unlike previous studies, this study used a single automated molecular method that was CE-marked and Food and Drug Administration-approved for use in quantifying CMV and EBV DNA in both plasma and WB. Furthermore, the complete viral replication kinetics of all episodes (including both the ascending and the descending phases of the active infection) was examined in each patient. The previously observed overall correlation between CMV DNA levels in WB and plasma was confirmed (Spearman's ρ = .85; P < .001). However, although WB and plasma CMV DNAemia reached peak levels simultaneously, in the ascending phase, the median CMV DNA levels in plasma were approximately 1 log10 lower than WB. Furthermore, in patients who received preemptive therapy, CMV DNA showed a delayed decrease in plasma compared with WB. A lower correlation between EBV DNA levels in plasma versus WB was found (Spearman's ρ = .61; P < .001). EBV DNA kinetics was not consistent in the 2 blood compartments, mostly due to the lower positivity in plasma. Indeed, in 19% of episodes, EBV DNA was negative at the time of the EBV DNA peak in WB. Our results suggest a preferential use of WB for surveillance of CMV and EBV infection in HSCT recipients., (Copyright © 2018 The American Society for Blood and Marrow Transplantation. Published by Elsevier Inc. All rights reserved.)

Published

2018

46. Development of an EliSPOT assay for HSV-1 and clinical validation in lung transplant patients.

Author

Costa C, Di Nauta A, Rittà M, Sinesi F, Bianco G, Sidoti F, Solidoro P, and Cavallo R

Subjects

Adult, Female, Herpes Simplex virology, Herpesvirus 1, Human isolation & purification, Herpesvirus 1, Human physiology, Humans, Male, Middle Aged, T-Lymphocytes immunology, Transplant Recipients, Virus Activation, Young Adult, Enzyme-Linked Immunospot Assay methods, Herpes Simplex diagnosis, Herpesvirus 1, Human immunology, Immunity, Cellular, Lung Transplantation adverse effects

Abstract

Cellular immunity plays a major role in the control of HSV-1 infection/reactivation with a potential impact on the clinical-therapeutic management of immunocompromised patients, such as transplant recipients. Herein, we quantitatively evaluated T-cell response directed at HSV-1 by a newly developed IFN-γ EliSPOT assay in 53 patients (including 45 lung transplant recipients and eight subjects in waiting list). Overall, 62.2% of transplant patients and 62.5% of subjects on the waiting list showed a response to HSV-1 with no significant difference in the level of virus-specific cellular immunity. Response tended to be lower in the first three months posttransplantation with a progressive recovery of pretransplantation status by the second year and in the presence of HSV-1 DNA positivity in bronchoalveolar lavage. As expected, no response was found in seronegative patients. No significant difference in the level of response according to IgM and IgG status was found. Further studies are required to define the role of HSV-1 specific immune response for the clinical-therapeutic management of lung transplant patients and in other clinical settings and to define cut-off levels discriminating between absence/low and strong response to be related to the risk of viral infection/reactivation.

Published

2017

47. No evidence of association of human polyomaviruses V6, V7 and V12, and Saint Louis human polyomavirus with squamous cell carcinoma.

Author

Ribero S, Costa C, Sidoti F, Osella-Abate S, Senetta R, Cassoni P, Fierro MT, and Cavallo R

Subjects

Aged, Female, Humans, Male, Middle Aged, Polyomavirus, Retrospective Studies, Carcinoma, Squamous Cell virology, Polyomavirus Infections, Skin Neoplasms virology, Tumor Virus Infections virology

Published

2017

48. PTFE Graft as a "Bridge" to Communicating Veins Maturation in the Treatment of an Intrahepatic Cholangiocarcinoma Involving the 3 Hepatic Veins. The Minor-but-Complex Liver Resection.

Author

Urbani L, Balestri R, Sidoti F, Bernardini JR, Arces F, Licitra G, Leoni C, Forfori F, Colombatto P, Boraschi P, Castagna M, and Buccianti P

Subjects

Bile Ducts, Intrahepatic, Humans, Male, Middle Aged, Organ Sparing Treatments methods, Parenchymal Tissue surgery, Bile Duct Neoplasms surgery, Cholangiocarcinoma surgery, Hepatectomy methods, Hepatic Veins surgery, Polytetrafluoroethylene, Vascular Grafting instrumentation

Abstract

Background: Parenchyma-sparing liver surgery allows resecting hepatic veins (HV) at the hepatocaval confluence with minor (<3 adjacent segments) liver resections. PTFE graft can be used as a bridge to communicating-veins maturation to ensure the correct outflow of the spared liver. We present a video of an intrahepatic cholangiocarcinoma (IC) involving the three HV at the hepatocaval confluence treated with this approach., Methods: In a 50-year old obese (BMI 44.8) male a 6-cm IC involving the hepatocaval confluence was identified during the follow-up for a kidney malignancy. At the preoperative CT scan the left HV was not detectable, the middle HV was incorporated within the tumor, and right HV had a 3-cm contact with the tumor. No communicating veins were evident at preoperative imaging., Results: After a J-shape thoracophrenolaparotomy, the resection of segments II-III-IVa was partially extended to segment VIII-VII and I. The right HV was detached from the tumor, and the middle HV was reconstructed with a 7-mm ringed-armed PTFE graft anastomosed to V8. Surgery lasted 20 h and 55 min with an estimated blood loss of 3500 ml, but the postoperative course was uneventful and the patient was discharged on the 14th postoperative day. One month later the CT scan showed a patent PTFE graft with the maturation of communicating-veins. One year later a complete thrombosis of the PTFE graft was observed with normal liver perfusion and function, and the patient was disease-free., Conclusions: PTFE-based parenchyma-sparing liver resection is a new tool to treat tumors located at the hepatocaval confluence exploiting the maturation of intrahepatic communicating-veins between main HV.

Published

2016

49. Comparison of two molecular assays for detection of cytomegalovirus DNA in whole blood and plasma samples from transplant recipients.

Author

Costa C, Sidoti F, Mantovani S, Gregori G, Proietti A, Ghisetti V, and Cavallo R

Subjects

Cytomegalovirus genetics, Cytomegalovirus Infections blood, Cytomegalovirus Infections diagnosis, Cytomegalovirus Infections virology, DNA, Viral genetics, DNA, Viral isolation & purification, Humans, Viral Load, Bone Marrow Transplantation adverse effects, Cytomegalovirus isolation & purification, DNA, Viral blood, Kidney Transplantation adverse effects, Liver Transplantation adverse effects, Polymerase Chain Reaction methods

Abstract

In immunosuppressed patients, pre-emptive therapy and a strict follow-up of CMV infection are the standard of care for the prevention of CMV disease. Several real-time PCR assays for CMV DNA quantification on whole blood (WB) and plasma (PL) are commercially available. This study compared and correlated CMV viral loads obtained by the Cobas AmpliPrep/Cobas TaqMan (CAP/CTM) platform on plasma specimens with those obtained on corresponding whole blood specimens by the real-time PCR assay (ELITe MGB-CMV) in 185 sequential samples from 41 immunosuppressed patients. Correlation between the two assays was good. Kinetics of CMV DNA within the same patient was similar, but PL viral load was constantly 1 log lower than WB. In patients under antiviral therapy, low level of CMV DNA persisted in WB, while it was absent in PL. The good correlation between CMV DNA detected on both PL and WB supports the reliability of the two matrices for viral monitoring and the therapeutic management of CMV infection. Nevertheless, due to significant quantification differences between PL and WB CMV DNA, the same biological specimen should be used for a sequential and reliable follow-up of patients at high risk of CMV infection.

Published

2016

50. Diagnosis of viral gastroenteritis: limits and potential of currently available procedures.

Author

Sidoti F, Rittà M, Costa C, and Cavallo R

Subjects

Humans, Sensitivity and Specificity, Specimen Handling methods, Time Factors, Clinical Laboratory Techniques methods, Diagnostic Tests, Routine methods, Gastroenteritis diagnosis, Gastroenteritis virology, Virology methods, Virus Diseases diagnosis, Virus Diseases virology

Abstract

The diagnostic approaches to viral gastroenteritis have evolved substantially over the past decades because of the advances in detection methods, the emergence of new pathogens, and the increase in diarrhea hospitalizations attributed to viruses, especially in young children in non-industrialized countries. Overall, these factors have lead to a relevant improvement of types and operating characteristics of diagnostic methods (including sensitivity and specificity), as well as turnaround time. In this review, clinical and laboratory approaches to the diagnosis of viruses causing gastroenteritis are presented; in particular, specimen collection and detection methods are reviewed and discussed, taking into account performance and limitations.

Published

2015